COMPOSITIONS OF HERBAL FORMULATIONS AND USES THEREOF

Abstract
Disclosed herein are herbal formulations for relief from symptoms of skin disease. The formulations can also be combined with an active or inactive pharmaceutical ingredient, and/or a pharmaceutically acceptable excipient.
Description
BACKGROUND

Human bodies have evolved over millions of years in harmony with nature. Certain natural products induce the human body to function more efficiently at combating disease and adverse conditions. These products help the human body heal itself. Skin conditions, the most visible of human maladies, have historically received the most attention when it comes to the application of herbal remedies. Herbs have been used in the healing of adverse skin conditions for thousands of years. Aloe vera, for example, is an herbal extract that has been used throughout history as a skin soothant and healant. Even today, lotions containing aloe vera are used to help skin to heal after sunburn.


Despite advances in science, skin conditions remain prevalent and the alleviation of symptoms remains elusive. Humans must return to nature from whence they came to find suitable relief for these conditions.





BRIEF DESCRIPTION OF THE DRAWINGS


FIG. 1 is a graph showing the results of the application of the HAT-01 formulation to psoriasis patients.



FIG. 2 is an illustration of the pilot trial study design conducted to evaluate the safety, benefit & tolerability of HAT-01 in patients with atopic dermatitis



FIG. 3 demonstrates the benefit of HAT-01 in a study of patients with atopic dermatitis.



FIG. 4 illustrates the benefit of HAT-01 in a study in patients with atopic dermatitis.





DETAILED DESCRIPTION

Disclosed herein are herbal compositions, based on a proprietary preparation of traditional commonly used herbs. Our studies have demonstrated that these formulations are potent and safe agents with benefit in aiding the body to alleviate the symptoms of chronic skin conditions as described herein.


Disclosed herein are compositions comprising a mixture of plant extracts obtained from at least two plants selected from the group consisting of: Achillea millefolium; Aesuculus hippocastanum; Althaea officinalis; Avena sativa; Berberis vulgaris; Capsella Bursa Pastoris; Cochlearia officinalis; Conium maculatium; Ervum lens; Hamamelis virginiana; Hydrastis canadensis; Matricaria chamomilla; Nasturtium officinale; Phytolacca decendra; Pimpinella saxifraga; Populas alba; Populus tremuloides; Rhus toxicodendron; Sambucus nigra; Sanguinaria Canadensis; Scrophularia nodosa; Smilax medica; Tussilago farfara; Veronica officinalis; and Vincetoxicum officinale. Also disclosed are compositions comprising the above compositions and a pharmaceutically acceptable carrier, diluents, or excipient. In addition, disclosed herein are methods of treating skin conditions by using the above compositions.


Thus, in a first non-limiting aspect, disclosed herein are complex herbal preparations containing a unique mixture of traditional commonly used multiple herbs. In some embodiments, the mixture comprises four herbal extract components. In certain embodiments, the disclosed preparations comprise plant extracts.


The term “plant extract” or “plant extracts” as used herein refers to a composition of extracted plant substances, including but not limited to: juices; macerations; concentrates; syrups; cold, heated, fluid and/or fermented extracts; powders; tablets; tinctures; herbal teas in the form of infusions or decoctions; poultices; lotions; creams; gels; ointments; salves; liniments; balms; oils; essential oils; suspensions; emulsions; compresses; dressings; fomentations; eyebaths; gargles; enemas; boluses; and other forms of extracted plant substances such as are known to those of ordinary skill in the arts of pharmacognosy, herbalism, and medicinal formulation. As used herein the term “plant extract” or “plant extracts” further contemplates the use of a solvent known to practitioners in this art for the purpose of extraction and or formulation, including but not limited to the use of one or more solvents such as water, an alcohol, a polyhydric alcohol, an ether, an ester, a carboxylic acid, an amide, a carbonate, supercritical fluid carbon dioxide, an ionic liquid, an alkane, a petroleum-derived oil, a plant oil, or another solvent, wherein the solvent employed is optionally part of a pH-adjusted medium. The term “plant extract” or “plant extracts” as used herein further contemplates that the extract may have been obtained by the use of one or more methods such as expression, absorption by steeping or otherwise, maceration, distillation, evaporation optionally with vacuum enhancement, freeze drying, and other methods known in the arts of substance isolation from natural sources.


In some embodiments, the disclosed preparations comprise a mixture of plant extracts from at least two plants selected from the group consisting of: Achillea millefolium (Yarrow); Aesuculus hippocastanum (Horsechestnut); Althaea officinalis (Althea mallow, or Marsh Mallow); Avena sativa (Oat); Berberis vulgaris (Barberry shrub); Capsella Bursa Pastoris (Shepherd's Purse); Cochlearia officinalis (Spoon Wort); Conium maculatium (Hemlock); Ervum lens (Lentil); Hamamelis virginiana (Virginium Hamamelis); Hydrastis canadensis (Orange Root); Matricaria chamomilla (Chamomil); Nasturtium officinale (Watercress); Phytolacca decendra (Poke Root); Pimpinella saxifraga (Pimpernal); Populas alba (White poplar); Populus tremuloides (Trembling poplar; Quaking Aspen, Trembling Aspen, Quakies); Rhus toxicodendron (Ivy); Sambucus nigra (Elderberry); Sanguinaria Canadensis (Canadian Blood root); Scrophularia nodosa (Figwort); Smilax medica (Sarasaparrilla); Tussilago farfara (Coltsfoot); Veronica officinalis (Speedwell); and Vincetoxicum officinale (Swallow Wort).


In some embodiments the herbal preparations disclosed herein comprise at least one herbal extract in the following amount (w/w):

    • Achillea millefolium from about 0.01% to about 20%;
    • Aesuculus hippocastanum from about 0.01% to about 20%;
    • Althaea officinalis from about 0.01% to about 20%;
    • Avena sativa from about 0.01% to about 25%;
    • Berberis vulgaris from about 0.01% to about 20%;
    • Capsella Bursa Pastoris from about 0.01% to about 20%;
    • Cochlearia officinalis from about 0.01% to about 20%;
    • Conium maculatium from about 0.01% to about 35%;
    • Ervum lens from about 0.01% to about 20%;
    • Hamamelis virginiana from about 0.01% to about 25%;
    • Hydrastis canadensis from about 0.01% to about 20%;
    • Matricaria chamomilla from about 0.01% to about 20%;
    • Nasturtium officinale from about 0.01% to about 15%;
    • Phytolacca decendra from about 0.01% to about 20%;
    • Pimpinella saxifraga from about 0.01% to about 20%;
    • Populas alba from about 0.01% to about 20%;
    • Populus tremuloides from about 0.01% to about 20%;
    • Rhus toxicodendron from about 0.01% to about 25%;
    • Sambucus nigra from about 0.01% to about 20;
    • Sanguinaria Canadensis from about 0.01% to about 20%;
    • Scrophularia nodosa from about 0.01% to about 20%;
    • Smilax medica from about 0.01% to about 20%;
    • Tussilago farfara from about 0.01% to about 15%;
    • Veronica officinalis from about 0.010% to about 15%; and
    • Vincetoxicum officinale from about 0.01% to about 15%.


Throughout the present disclosure the term “about” a certain value means that a range of value±20%, such as (but not limited to) a range of value±10%, is contemplated. Thus, for example, having about 20% w/w of an ingredient includes the ingredient being present between 16% and 24%, such as (but not limited to) between 18% and 22%.


In some embodiments the herbal preparations disclosed herein comprise Achillea millefolium from about 1% to about 15%; or from about 1% to about 10%; or from about 1% to about 8%; or from about 1.5% to about 7%; or from about 2% to about 6%. In some embodiments the herbal preparations disclosed herein comprise Achillea millefolium in about 2.5%, while in other embodiments comprise about 5%.


In some embodiments the herbal preparations disclosed herein comprise Aesuculus hippocastanum from about 1% to about 15%; or from about 1% to about 10%; or from about 1% to about 8%; or from about 1.5% to about 7%; or from about 2% to about 6%. In some embodiments the herbal preparations disclosed herein comprise Aesuculus hippocastanum in about 2.4%, while in other embodiments comprise about 5%.


In some embodiments the herbal preparations disclosed herein comprise Althea officinalis from about 1% to about 15%; or from about 1% to about 10%; or from about 1% to about 8%; or from about 1.5% to about 7%; or from about 1.5% to about 5%. In some embodiments the herbal preparations disclosed herein comprise Althaea officinalis in about 2.0%, while in other embodiments comprise about 4%.


In some embodiments the herbal preparations disclosed herein comprise Avena sativa from about 1% to about 25%; or from about 3% to about 20%; or from about 5% to about 17%; or from about 5% to about 15%. In some embodiments the herbal preparations disclosed herein comprise Avena sativa in about 6.8%, while in other embodiments comprise about 14%.


In some embodiments the herbal preparations disclosed herein comprise Berberis vulgaris from about 1% to about 17%; or from about 1% to about 15%; or from about 3% to about 12%; or from about 3% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Berberis vulgaris in about 4.1%, while in other embodiments comprise about 8%.


In some embodiments the herbal preparations disclosed herein comprise Capsella Bursa Pastoris from about 1% to about 17%; or from about 1% to about 15%; or from about 1.5% to about 12%; or from about 1.5% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Capsella Bursa Pastoris in about 2.2%, while in other embodiments comprise about 8%.


In some embodiments the herbal preparations disclosed herein comprise Cochlearia officinalis from about 1% to about 17%; or from about 3% to about 15%; or from about 3% to about 12%; or from about 4% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Cochlearia officinalis in about 5.1%, while in other embodiments comprise about 10%.


In some embodiments the herbal preparations disclosed herein comprise Conium maculatium from about 1% to about 30%; or from about 1% to about 25%; or or from about 3.5% to about 23%. In some embodiments the herbal preparations disclosed herein comprise Conium maculatium in about 4%, in other embodiments comprise about 12.1%, while in yet other embodiments comprise about 21%.


In some embodiments the herbal preparations disclosed herein comprise Ervum lens from about 1% to about 17%; or from about 1% to about 15%; or from about 3% to about 12%; or from about 3% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Ervum lens in about 3.7%, while in other embodiments comprise about 8%.


In some embodiments the herbal preparations disclosed herein comprise Hamamelis virginiana from about 1% to about 25%; or from about 3% to about 20%; or from about 5% to about 17%; or from about 5% to about 15%. In some embodiments the herbal preparations disclosed herein comprise Hamamelis virginiana in about 8.9%, while in other embodiments comprise about 13%.


In some embodiments the herbal preparations disclosed herein comprise Hydrastis canadensis from about 1% to about 17%; or from about 3% to about 15%; or from about 3% to about 12%; or from about 3.5% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Hydrastis canadensis in about 5%, in other embodiments comprise about 6.0%, while in yet other embodiments comprise about 8%.


In some embodiments the herbal preparations disclosed herein comprise Matricaria chamomilla from about 1% to about 17%; or from about 1% to about 15%; or from about 1.5% to about 12%; or from about 1.5% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Matricaria chamomilla in about 2.2%, while in other embodiments comprise about 8%.


In some embodiments the herbal preparations disclosed herein comprise Nasturtium officinale from about 0.01% to about 12%; or from about 0.01% to about 10%; or from about 0.1% to about 8%; or from about 0.1% to about 5%. In some embodiments the herbal preparations disclosed herein comprise Nasturtium officinale in about 0.9%, while in other embodiments comprise about 2%.


In some embodiments the herbal preparations disclosed herein comprise Phytolacca decendra from about 1% to about 17%; or from about 3% to about 15%; or from about 3% to about 12%; or from about 3.5% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Phytolacca decendra in about 4%, in other embodiments comprise about 5.8%, while in yet other embodiments comprise about 8%.


In some embodiments the herbal preparations disclosed herein comprise Pimpinella saxifraga from about 0.01% to about 12%; or from about 0.01% to about 10%; or from about 0.1% to about 8%; or from about 0.5% to about 5%. In some embodiments the herbal preparations disclosed herein comprise Pimpinella saxifraga in about 1.1%, while in other embodiments comprise about 2%.


In some embodiments the herbal preparations disclosed herein comprise Populas alba from about 1% to about 17%; or from about 3% to about 15%; or from about 3% to about 12%; or from about 4% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Populas alba in about 4.9%, while in other embodiments comprise about 10%.


In some embodiments the herbal preparations disclosed herein comprise Populus tremuloides from about 1% to about 17%; or from about 3% to about 15%; or from about 3% to about 12%; or from about 4% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Populus tremuloides in about 4.8%, while in other embodiments comprise about 10%.


In some embodiments the herbal preparations disclosed herein comprise Rhus toxicodendron from about 1% to about 25%; or from about 3% to about 20%; or from about 5% to about 20%; or from about 7% to about 20%. In some embodiments the herbal preparations disclosed herein comprise Rhus toxicodendron in about 8.3%, while in other embodiments comprise about 17%.


In some embodiments the herbal preparations disclosed herein comprise Sambucus nigra from about 1% to about 15%; or from about 1% to about 10%; or from about 1% to about 8%; or from about 1.5% to about 7%; or from about 1.5% to about 6%. In some embodiments the herbal preparations disclosed herein comprise Sambucus nigra in about 1.9%, while in other embodiments comprise about 4%.


In some embodiments the herbal preparations disclosed herein comprise Sanguinaria Canadensis from about 1% to about 17%; or from about 3% to about 15%; or from about 3% to about 12%; or from about 4% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Sanguinaria Canadensis in about 4.5%, while in other embodiments comprise about 9%.


In some embodiments the herbal preparations disclosed herein comprise Scrophularia nodosa from about 1% to about 17%; or from about 3% to about 15%; or from about 3% to about 12%; or from about 4% to about 10%. In some embodiments the herbal preparations disclosed herein comprise Scrophularia nodosa in about 4.0%, while in other embodiments comprise about 8%.


In some embodiments the herbal preparations disclosed herein comprise Smilax medica from about 1% to about 15%; or from about 1% to about 10%; or from about 1% to about 8%; or from about 1.5% to about 7%; or from about 2% to about 6.5%. In some embodiments the herbal preparations disclosed herein comprise Smilax medica in about 3.1%, while in other embodiments, comprise about 6%.


In some embodiments the herbal preparations disclosed herein comprise Tussilago farfara from about 0.01% to about 12%; or from about 0.01% to about 10%; or from about 0.1% to about 8%; or from about 0.1% to about 5%. In some embodiments the herbal preparations disclosed herein comprise Tussilago farfara in about 0.9%, while in other embodiments comprise about 2%.


In some embodiments the herbal preparations disclosed herein comprise Veronica officinalis from about 0.01% to about 12%; or from about 0.01% to about 10%; or from about 0.1% to about 8%; or from about 0.1% to about 5%. In some embodiments the herbal preparations disclosed herein comprise Veronica officinalis in about 0.8%, while in other embodiments comprise about 2%.


In some embodiments the herbal preparations disclosed herein comprise Vincetoxicum officinale from about 0.01% to about 12%; or from about 0.01% to about 10%; or from about 0.1% to about 8%; or from about 0.1% to about 5%. In some embodiments the herbal preparations disclosed herein comprise Vincetoxicum officinale in about 0.9%, while in other embodiments comprise about 2%.


In one embodiment, the herbal preparation disclosed herein comprises Mixture I. Mixture I comprises plant extracts obtained from the following plants: Althaea officinalis; Ervum lens; Populas alba; Populus tremuloides; Conium maculatium; Sambucus nigra; Hamamelis virginiana; and Phytolacca decendra.


In another embodiment, the herbal preparation disclosed herein comprises Mixture II. Mixture II comprises plant extracts obtained from the following plants: Conium maculatium; Phytolacca decendra; Pimpinella saxifraga; Rhus toxicodendron; and Vincetoxicum officinale.


In yet another embodiment, the herbal preparation disclosed herein comprises Mixture III. Mixture Ill comprises plant extracts obtained from the following plants: Avena sativa; Aesuculus hippocastanum; Capsella Bursa Pastoris; Hamamelis virginiana; Hydrastis canadensis; Achillea millefolium; and Sanguinaria Canadensis.


In still another embodiment, the herbal preparation disclosed herein comprises Mixture IV. Mixture IV comprises plant extracts obtained from the following plants: Berberis vulgaris; Matricaria chamomilla; Cochlearia officinalis; Hydrastis canadensis; Nasturtium officinale; Scrophularia nodosa; Smilax medica; Tussilago farfara; and Veronica officinalis.


In one embodiment, the herbal preparation disclosed herein comprises Mixture V. Mixture V comprises plant extracts obtained from the following plants: Berberis vulgaris; Cochlearia officinalis; Conium maculatium; Hydrastis canadensis; Matricaria chamomilla; Nasturtium officinale; Phytolacca decendra; Pimpinella saxifraga; Rhus toxicodendron; Scrophularia nodosa; Smilax medica; Tussilago farfara; Veronica officinalis; and Vincetoxicum officinale.


In one embodiment, the herbal preparation disclosed herein comprises Mixture VI. Mixture VI comprises plant extracts obtained from the following plants: Achillea millefolium; Aesuculus hippocastanum; Althaea officinalis; Avena sativa; Conium maculatium; Ervum lens; Hamamelis virginiana; Hydrastis canadensis; Phytolacca decendra; Populas alba; Populus tremuloides; Sambucus nigra; and Sanguinaria Canadensis.


In some embodiments, the herbal preparation disclosed herein comprises a combination of Mixture I and Mixture II. In another embodiment, the herbal preparation disclosed herein comprises a combination of Mixture I and Mixture III. In another embodiment, the herbal preparation disclosed herein comprises a combination of Mixture I and Mixture IV.


In some embodiments, the herbal preparation disclosed herein comprises a combination of Mixture II and Mixture III. In another embodiment, the herbal preparation disclosed herein comprises a combination of Mixture II and Mixture IV.


In some embodiments, the herbal preparation disclosed herein comprises a combination of Mixture III and Mixture IV.


In some embodiments, the herbal preparation disclosed herein comprises a combination of Mixture I, Mixture II and Mixture III. In another embodiment, the herbal preparation disclosed herein comprises a combination of Mixture I, Mixture II and Mixture IV. In another embodiment, the herbal preparation disclosed herein comprises a combination of Mixture I, Mixture III and Mixture IV. In another embodiment, the herbal preparation disclosed herein comprises a combination of Mixture II, Mixture III and Mixture IV.


In another embodiment, the herbal preparation disclosed herein comprises a combination of Mixture I, Mixture II, Mixture Ill and Mixture IV.


In some embodiments, the herbal preparation disclosed herein comprises a combination of Mixture V and Mixture VI.


In some embodiments the herbal preparations disclosed herein comprise at least two herbal extracts each of which is selected from the following list and each is present in the following amount (w/w): Achillea millefolium from about 0.01% to about 20%; Aesuculus hippocastanum from about 0.01% to about 20%; Althaea officinalis from about 0.01% to about 20%; Avena sativa from about 0.01% to about 25%; Berberis vulgaris from about 0.01% to about 20%; Capsella Bursa Pastoris from about 0.01% to about 20%; Cochlearia officinalis from about 0.01% to about 20%; Conium maculatium from about 0.01% to about 35%; Ervum lens from about 0.01% to about 20%; Hamamelis virginiana from about 0.01% to about 25%; Hydrastis canadensis from about 0.01% to about 20%; Matricaria chamomilla from about 0.01% to about 20%; Nasturtium officinale from about 0.01% to about 15%; Phytolacca decendra from about 0.01% to about 20%; Pimpinella saxifraga from about 0.01% to about 20%; Populas alba from about 0.01% to about 20%; Populus tremuloides from about 0.01% to about 20%; Rhus toxicodendron from about 0.01% to about 25%; Sambucus nigra from about 0.01% to about 20;Sanguinaria Canadensis from about 0.01% to about 20%; Scrophularia nodosa from about 0.01% to about 20%; Smilax medica from about 0.01% to about 20%; Tussilago farfara from about 0.01% to about 15%; Veronica officinalis from about 0.01% to about 15%; and Vincetoxicum officinale from about 0.01% to about 15%.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group I plant extracts and at least one plant extract from the Group II plant extracts, where the at least one Group I plant extract and the at least one Group II plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group I plant extracts and at least one plant extract from the Group III plant extracts, where the at least one Group I plant extract and the at least one Group Ill plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group I plant extracts and at least one plant extract from the Group IV plant extracts, where the at least one Group I plant extract and the at least one Group IV plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group II plant extracts and at least one plant extract from the Group III plant extracts, where the at least one Group II plant extract and the at least one Group III plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group II plant extracts and at least one plant extract from the Group IV plant extracts, where the at least one Group II plant extract and the at least one Group IV plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group III plant extracts and at least one plant extract from the Group IV plant extracts, where the at least one Group III plant extract and the at least one Group IV plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group I plant extracts, at least one plant extract from the Group II plant extracts, and at least one plant extract from the Group Ill plant extracts, where the at least one Group I plant extract, the at least one Group II plant extract, and the at least one Group Ill plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group I plant extracts, at least one plant extract from the Group II plant extracts, and at least one plant extract from the Group IV plant extracts, where the at least one Group I plant extract, the at least one Group II plant extract, and the at least one Group IV plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group I plant extracts, at least one plant extract from the Group III plant extracts, and at least one plant extract from the Group IV plant extracts, where the at least one Group I plant extract, the at least one Group Ill plant extract, and the at least one Group IV plant extract are different.


In one embodiment, the herbal preparation disclosed herein comprises at least one plant extract from the Group II plant extracts, at least one plant extract from the Group Ill plant extracts, and at least one plant extract from the Group IV plant extracts, where the at least one Group II plant extract, the at least one Group Ill plant extract, and the at least one Group IV plant extract are different.


Group I comprises a plant extract obtained from a plant selected from the group consisting of: Althaea officinalis; Ervum lens; Populas alba; Populus tremuloides; Conium maculatium; Sambucus nigra; Hamamelis virginiana; and Phytolacca decendra.


Group II comprises a plant extract obtained from a plant selected from the group consisting of: Conium maculatium; Phytolacca decendra; Pimpinella saxifraga; Rhus toxicodendron; and Vincetoxicum officinale.


Group Ill comprises a plant extract obtained from a plant selected from the group consisting of: Avena sativa; Aesuculus hippocastanum; Capsella Bursa Pastoris; Hamamelis virginiana; Hydrastis canadensis; Achillea millefolium; and Sanguinaria Canadensis.


Group IV comprises a plant extract obtained from a plant selected from the group consisting of: Berberis vulgaris; Matricaria chamomilla; Cochlearia officinalis; Hydrastis canadensis; Nasturtium officinale; Scrophularia nodosa; Smilax medica; Tussilago farfara; and Veronica officinalis.


Thus, embodiments of the herbal extracts disclosed herein include the mixtures numbered below in Table 1, comprising at least two components, where the components are listed in Table 1.











TABLE 1





No.
Component 1
Component 2

















1

Achillea millefolium from about 0.01% to


Aesuculus hippocastanum from about




about 20%
0.01% to about 20%


2

Achillea millefolium from about 0.01% to


Althaea officinalis from about 0.01% to




about 20%
about 20%


3

Achillea millefolium from about 0.01% to


Avena sativa from about 0.01% to about




about 20%
25%


4

Achillea millefolium from about 0.01% to


Berberis vulgaris from about 0.01% to




about 20%
about 20%


5

Achillea millefolium from about 0.01% to


Cochlearia officinalis from about 0.01% to




about 20%
about 20%


6

Achillea millefolium from about 0.01% to


Conium maculatium from about 0.01% to




about 20%
about 35%


7

Achillea millefolium from about 0.01% to


Ervum lens from about 0.01% to about




about 20%
20%


8

Achillea millefolium from about 0.01% to


Hamamelis virginiana from about 0.01%




about 20%
to about 25%


9

Achillea millefolium from about 0.01% to


Hydrastis canadensis from about 0.01% to




about 20%
about 20%


10

Achillea millefolium from about 0.01% to


Copsella Bursa Pastoris from about 0.01%




about 20%
to about 20%


11

Achillea millefolium from about 0.01% to


Matricaria chamomilla from about 0.01%




about 20%
to about 20%


12

Achillea millefolium from about 0.01% to


Nasturtium officinale from about 0.01% to




about 20%
about 15%


13

Achillea millefolium from about 0.01% to


Phytolacca decendra from about 0.01% to




about 20%
about 20%


14

Achillea millefolium from about 0.01% to


Pimpinella saxifraga from about 0.01% to




about 20%
about 20%


15

Achillea millefolium from about 0.01% to


Populas alba from about 0.01% to about




about 20%
20%


16

Achillea millefolium from about 0.01% to


Populus tremuloides from about 0.01% to




about 20%
about 20%


17

Achillea millefolium from about 0.01% to


Rhus toxicodendron from about 0.01% to




about 20%
about 25%


18

Achillea millefolium from about 0.01% to


Sambucus nigra from about 0.01% to




about 20%
about 20%


19

Achillea millefolium from about 0.01% to


Sanguinaria Canadensis from about 0.01%




about 20%
to about 20%


20

Achillea millefolium from about 0.01% to


Scrophularia nodosa from about 0.01% to




about 20%
about 20%


21

Achillea millefolium from about 0.01% to


Smilax medica from about 0.01% to about




about 20%
20%


22

Achillea millefolium from about 0.01% to


Tussilago farfara from about 0.01% to




about 20%
about 15%


23

Achillea millefolium from about 0.01% to


Veronica officinalis from about 0.01% to




about 20%
about 15%


24

Achillea millefolium from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 20%
to about 15%


25

Aesuculus hippocastanum from about


Althaea officinalis from about 0.01% to




0.01% to about 20%
about 20%


26

Aesuculus hippocastanum from about


Avena sativa from about 0.01% to about




0.01% to about 20%
25%


27

Aesuculus hippocastanum from about


Berberis vulgaris from about 0.01% to




0.01% to about 20%
about 20%


28

Aesuculus hippocastanum from about


Cochlearia officinalis from about 0.01% to




0.01% to about 20%
about 20%


29

Aesuculus hippocastanum from about


Conium maculatium from about 0.01% to




0.01% to about 20%
about 35%


30

Aesuculus hippocastanum from about


Ervum lens from about 0.01% to about




0.01% to about 20%
20%


31

Aesuculus hippocastanum from about


Hamamelis virginiana from about 0.01%




0.01% to about 20%
to about 25%


32

Aesuculus hippocastanum from about


Hydrastis canadensis from about 0.01% to




0.01% to about 20%
about 20%


33

Aesuculus hippocastanum from about


Capsella Bursa Pastoris from about 0.01%




0.01% to about 20%
to about 20%


34

Aesuculus hippocastanum from about


Matricaria chamomilla from about 0.01%




0.01% to about 20%
to about 20%


35

Aesuculus hippocastanum from about


Nasturtium officinale from about 0.01% to




0.01% to about 20%
about 15%


36

Aesuculus hippocastanum from about


Phytolacca decendra from about 0.01% to




0.01% to about 20%
about 20%


37

Aesuculus hippocastanum from about


Pimpinella saxifraga from about 0.01% to




0.01% to about 20%
about 20%


38

Aesuculus hippocastanum from about


Populas alba from about 0.01% to about




0.01% to about 20%
20%


39

Aesuculus hippocastanum from about


Populus tremuloides from about 0.01% to




0.01% to about 20%
about 20%


40

Aesuculus hippocastanum from about


Rhus toxicodendron from about 0.01% to




0.01% to about 20%
about 25%


41

Aesuculus hippocastanum from about


Sambucus nigra from about 0.01% to




0.01% to about 20%
about 20%


42

Aesuculus hippocastanum from about


Sanguinaria Canadensis from about 0.01%




0.01% to about 20%
to about 20%


43

Aesuculus hippocastanum from about


Scrophularia nodosa from about 0.01% to




0.01% to about 20%
about 20%


44

Aesuculus hippocastanum from about


Smilax medica from about 0.01% to about




0.01% to about 20%
20%


45

Aesuculus hippocastanum from about


Tussilago farfara from about 0.01% to




0.01% to about 20%
about 15%


46
Aesuculus hippocastanum from about

Veronica officinalis from about 0.01% to




0.01% to about 20%
about 15%


47
Aesuculus hippocastanum from about

Vincetoxicum officinale from about 0.01%




0.01% to about 20%
to about 15%


48

Althaea officinalis from about 0.01% to


Avena sativa from about 0.01% to about




about 20%
25%


49

Althaea officinalis from about 0.01% to


Berberis vulgaris from about 0.01% to




about 20%
about 20%


50

Althaea officinalis from about 0.01% to


Cochlearia officinalis from about 0.01% to




about 20%
about 20%


51

Althaea officinalis from about 0.01% to


Conium maculatium from about 0.01% to




about 20%
about 35%


52

Althaea officinalis from about 0.01% to


Ervum lens from about 0.01% to about




about 20%
20%


53

Althaea officinalis from about 0.01% to


Hamamelis virginiana from about 0.01%




about 20%
to about 25%


54

Althaea officinalis from about 0.01% to


Hydrastis canadensis from about 0.01% to




about 20%
about 20%


55

Althaea officinalis from about 0.01% to


Capsella Bursa Pastoris from about 0.01%




about 20%
to about 20%


56

Althaea officinalis from about 0.01% to


Matricaria chamomilla from about 0.01%




about 20%
to about 20%


57

Althaea officinalis from about 0.01% to


Nasturtium officinale from about 0.01% to




about 20%
about 15%


58

Althaea officinalis from about 0.01% to


Phytolacca decendra from about 0.01% to




about 20%
about 20%


59

Althaea officinalis from about 0.01% to


Pimpinella saxifraga from about 0.01% to




about 20%
about 20%


60

Althaea officinalis from about 0.01% to


Populas alba from about 0.01% to about




about 20%
20%


61

Althaea officinalis from about 0.01% to


Populus tremuloides from about 0.01% to




about 20%
about 20%


62

Althaea officinalis from about 0.01% to


Rhus toxicodendron from about 0.01% to




about 20%
about 25%


63

Althaea officinalis from about 0.01% to


Sambucus nigra from about 0.01% to




about 20%
about 20%


64

Althaea officinalis from about 0.01% to


Sanguinaria Canadensis from about 0.01%




about 20%
to about 20%


65

Althaea officinalis from about 0.01% to


Scrophularia nodosa from about 0.01% to




about 20%
about 20%


66

Althaea officinalis from about 0.01% to


Smilax medica from about 0.01% to about




about 20%
20%


67

Althaea officinalis from about 0.01% to


Tussilago farfara from about 0.01% to




about 20%
about 15%


68

Althaea officinalis from about 0.01% to


Veronica officinalis from about 0.01% to




about 20%
about 15%


69

Althaea officinalis from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 20%
to about 15%


70

Avena sativa from about 0.01% to about


Berberis vulgaris from about 0.01% to




25%
about 20%


71

Avena sativa from about 0.01% to about


Cochlearia officinalis from about 0.01% to




25%
about 20%


72

Avena sativa from about 0.01% to about


Conium maculatium from about 0.01% to




25%
about 35%


73

Avena sativa from about 0.01% to about


Ervum lens from about 0.01% to about




25%
20%


74

Avena sativa from about 0.01% to about


Hamamelis virginiana from about 0.01%




25%
to about 25%


75

Avena sativa from about 0.01% to about


Hydrastis canadensis from about 0.01% to




25%
about 20%


76

Avena sativa from about 0.01% to about


Capsella Bursa Pastoris from about 0.01%




25%
to about 20%


77

Avena sativa from about 0.01% to about


Matricaria chamomilla from about 0.01%




25%
to about 20%


78

Avena sativa from about 0.01% to about


Nasturtium officinale from about 0.01% to




25%
about 15%


79

Avena sativa from about 0.01% to about


Phytolacca decendra from about 0.01% to




25%
about 20%


80

Avena sativa from about 0.01% to about


Pimpinella saxifraga from about 0.01% to




25%
about 20%


81

Avena sativa from about 0.01% to about


Populas alba from about 0.01% to about




25%
20%


82

Avena sativa from about 0.01% to about


Populus tremuloides from about 0.01% to




25%
about 20%


83

Avena sativa from about 0.01% to about


Rhus toxicodendron from about 0.01% to




25%
about 25%


84

Avena sativa from about 0.01% to about


Sambucus nigra from about 0.01% to




25%
about 20%


85

Avena sativa from about 0.01% to about


Sanguinaria Canadensis from about 0.01%




25%
to about 20%


86

Avena sativa from about 0.01% to about


Scrophularia nodosa from about 0.01% to




25%
about 20%


87

Avena sativa from about 0.01% to about


Smilax medica from about 0.01% to about




25%
20%


88

Avena sativa from about 0.01% to about


Tussilago farfara from about 0.01% to




25%
about 15%


89

Avena sativa from about 0.01% to about


Veronica officinalis from about 0.01% to




25%
about 15%


90

Avena sativa from about 0.01% to about


Vincetoxicum officinale from about 0.01%




25%
to about 15%


91

Berberis vulgaris from about 0.01% to


Cochlearia officinalis from about 0.01% to




about 20%
about 20%


92

Berberis vulgaris from about 0.01% to


Conium maculatium from about 0.01% to




about 20%
about 35%


93

Berberis vulgaris from about 0.01% to


Ervum lens from about 0.01% to about




about 20%
20%


94

Berberis vulgaris from about 0.01% to


Hamamelis virginiana from about 0.01%




about 20%
to about 25%


95

Berberis vulgaris from about 0.01% to


Hydrastis canadensis from about 0.01% to




about 20%
about 20%


96

Berberis vulgaris from about 0.01% to


Copsella Bursa Pastoris from about 0.01%




about 20%
to about 20%


97

Berberis vulgaris from about 0.01% to


Matricaria chamomilla from about 0.01%




about 20%
to about 20%


98

Berberis vulgaris from about 0.01% to


Nasturtium officinale from about 0.01% to




about 20%
about 15%


99

Berberis vulgaris from about 0.01% to


Phytolacca decendra from about 0.01% to




about 20%
about 20%


100

Berberis vulgaris from about 0.01% to


Pimpinella saxifraga from about 0.01% to




about 20%
about 20%


101

Berberis vulgaris from about 0.01% to


Populas alba from about 0.01% to about




about 20%
20%


102

Berberis vulgaris from about 0.01% to


Populus tremuloides from about 0.01% to




about 20%
about 20%


103

Berberis vulgaris from about 0.01% to


Rhus toxicodendron from about 0.01% to




about 20%
about 25%


104

Berberis vulgaris from about 0.01% to


Sambucus nigra from about 0.01% to




about 20%
about 20%


105

Berberis vulgaris from about 0.01% to


Sanguinaria Canadensis from about 0.01%




about 20%
to about 20%


106

Berberis vulgaris from about 0.01% to


Scrophularia nodosa from about 0.01% to




about 20%
about 20%


107

Berberis vulgaris from about 0.01% to


Smilax medica from about 0.01% to about




about 20%
20%


108

Berberis vulgaris from about 0.01% to


Tussilago farfara from about 0.01% to




about 20%
about 15%


109
Berberis vulgaris from about 0.01% to

Veronica officinalis from about 0.01% to




about 20%
about 15%


110

Berberis vulgaris from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 20%
to about 15%


111

Cochlearia officinalis from about 0.01%


Conium maculatium from about 0.01% to




to about 20%
about 35%


112

Cochlearia officinalis from about 0.01%


Ervum lens from about 0.01% to about




to about 20%
20%


113

Cochlearia officinalis from about 0.01%


Hamamelis virginiana from about 0.01%




to about 20%
to about 25%


114

Cochlearia officinalis from about 0.01%


Hydrastis canadensis from about 0.01% to




to about 20%
about 20%


115

Cochlearia officinalis from about 0.01%


Capsella Bursa Pastoris from about 0.01%




to about 20%
to about 20%


116

Cochlearia officinalis from about 0.01%


Matricaria chamomilla from about 0.01%




to about 20%
to about 20%


117

Cochlearia officinalis from about 0.01%


Nasturtium officinale from about 0.01% to




to about 20%
about 15%


118

Cochlearia officinalis from about 0.01%


Phytolacca decendra from about 0.01% to




to about 20%
about 20%


119

Cochlearia officinalis from about 0.01%


Pimpinella saxifraga from about 0.01% to




to about 20%
about 20%


120

Cochlearia officinalis from about 0.01%


Populas alba from about 0.01% to about




to about 20%
20%


121

Cochlearia officinalis from about 0.01%


Populus tremuloides from about 0.01% to




to about 20%
about 20%


122

Cochlearia officinalis from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 20%
about 25%


123

Cochlearia officinalis from about 0.01%


Sambucus nigra from about 0.01% to




to about 20%
about 20%


124

Cochlearia officinalis from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 20%
to about 20%


125

Cochlearia officinalis from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 20%
about 20%


126

Cochlearia officinalis from about 0.01%


Smilax medica from about 0.01% to about




to about 20%
20%


127

Cochlearia officinalis from about 0.01%


Tussilago farfara from about 0.01% to




to about 20%
about 15%


128

Cochlearia officinalis from about 0.01%


Veronica officinalis from about 0.01% to




to about 20%
about 15%


129

Cochlearia officinalis from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 20%
to about 15%


130

Conium maculatium from about 0.01%


Ervum lens from about 0.01% to about




to about 35%
20%


131

Conium maculatium from about 0.01%


Hamamelis virginiana from about 0.01%




to about 35%
to about 25%


132

Conium maculatium from about 0.01%


Hydrastis canadensis from about 0.01% to




to about 35%
about 20%


133

Conium maculatium from about 0.01%


Capsella Bursa Pastoris from about 0.01%




to about 35%
to about 20%


134

Conium maculatium from about 0.01%


Matricaria chamomilla from about 0.01%




to about 35%
to about 20%


135

Conium maculatium from about 0.01%


Nasturtium officinale from about 0.01% to




to about 35%
about 15%


136

Conium maculatium from about 0.01%


Phytolacca decendra from about 0.01% to




to about 35%
about 20%


137

Conium maculatium from about 0.01%


Pimpinella saxifraga from about 0.01% to




to about 35%
about 20%


138

Conium maculatium from about 0.01%


Populas alba from about 0.01% to about




to about 35%
20%


139

Conium maculatium from about 0.01%


Populus tremuloides from about 0.01% to




to about 35%
about 20%


140

Conium maculatium from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 35%
about 25%


141

Conium maculatium from about 0.01%


Sambucus nigra from about 0.01% to




to about 35%
about 20%


142

Conium maculatium from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 35%
to about 20%


143

Conium maculatium from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 35%
about 20%


144

Conium maculatium from about 0.01%


Smilax medica from about 0.01% to about




to about 35%
20%


145

Conium maculatium from about 0.01%


Tussilago farfara from about 0.01% to




to about 35%
about 15%


146

Conium maculatium from about 0.01%


Veronica officinalis from about 0.01% to




to about 35%
about 15%


147

Conium maculatium from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 35%
to about 15%


148

Ervum lens from about 0.01% to about


Hamamelis virginiana from about 0.01%




20%
to about 25%


149

Ervum lens from about 0.01% to about


Hydrastis canadensis from about 0.01% to




20%
about 20%


150

Ervum lens from about 0.01% to about


Capsella Bursa Pastoris from about 0.01%




20%
to about 20%


151

Ervum lens from about 0.01% to about


Matricaria chamomilla from about 0.01%




20%
to about 20%


152

Ervum lens from about 0.01% to about


Nasturtium officinale from about 0.01% to




20%
about 15%


153

Ervum lens from about 0.01% to about


Phytolacca decendra from about 0.01% to




20%
about 20%


154

Ervum lens from about 0.01% to about


Pimpinella saxifraga from about 0.01% to




20%
about 20%


155

Ervum lens from about 0.01% to about


Populas alba from about 0.01% to about




20%
20%


156

Ervum lens from about 0.01% to about


Populus tremuloides from about 0.01% to




20%
about 20%


157

Ervum lens from about 0.01% to about


Rhus toxicodendron from about 0.01% to




20%
about 25%


158

Ervum lens from about 0.01% to about


Sambucus nigra from about 0.01% to




20%
about 20%


159

Ervum lens from about 0.01% to about


Sanguinaria Canadensis from about 0.01%




20%
to about 20%


160

Ervum lens from about 0.01% to about


Scrophularia nodosa from about 0.01% to




20%
about 20%


161

Ervum lens from about 0.01% to about


Smilax medica from about 0.01% to about




20%
20%


162

Ervum lens from about 0.01% to about


Tussilago farfara from about 0.01% to




20%
about 15%


163

Ervum lens from about 0.01% to about


Veronica officinalis from about 0.01% to




20%
about 15%


164

Ervum lens from about 0.01% to about


Vincetoxicum officinale from about 0.01%




20%
to about 15%


165

Hamamelis virginiana from about 0.01%


Hydrastis canadensis from about 0.01% to




to about 25%
about 20%


166

Hamamelis virginiana from about 0.01%


Capsella Bursa Pastoris from about 0.01%




to about 25%
to about 20%


167

Hamamelis virginiana from about 0.01%


Matricaria chamomilla from about 0.01%




to about 25%
to about 20%


168

Hamamelis virginiana from about 0.01%


Nasturtium officinale from about 0.01% to




to about 25%
about 15%


169

Hamamelis virginiana from about 0.01%


Phytolacca decendra from about 0.01% to




to about 25%
about 20%


170

Hamamelis virginiana from about 0.01%


Pimpinella saxifraga from about 0.01% to




to about 25%
about 20%


171

Hamamelis virginiana from about 0.01%


Populas alba from about 0.01% to about




to about 25%
20%


172

Hamamelis virginiana from about 0.01%


Populus tremuloides from about 0.01% to




to about 25%
about 20%


173

Hamamelis virginiana from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 25%
about 25%


174

Hamamelis virginiana from about 0.01%


Sambucus nigra from about 0.01% to




to about 25%
about 20%


175

Hamamelis virginiana from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 25%
to about 20%


176

Hamamelis virginiana from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 25%
about 20%


177

Hamamelis virginiana from about 0.01%


Smilax medica from about 0.01% to about




to about 25%
20%


178

Hamamelis virginiana from about 0.01%


Tussilago farfara from about 0.01% to




to about 25%
about 15%


179

Hamamelis virginiana from about 0.01%


Veronica officinalis from about 0.01% to




to about 25%
about 15%


180

Hamamelis virginiana from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 25%
to about 15%


181

Hydrastis canadensis from about 0.01%


Capsella Bursa Pastoris from about 0.01%




to about 20%
to about 20%


182

Hydrastis canadensis from about 0.01%


Matricaria chamomilla from about 0.01%




to about 20%
to about 20%


183

Hydrastis canadensis from about 0.01%


Nasturtium officinale from about 0.01% to




to about 20%
about 15%


184

Hydrastis canadensis from about 0.01%


Phytolacca decendra from about 0.01% to




to about 20%
about 20%


185

Hydrastis canadensis from about 0.01%


Pimpinella saxifraga from about 0.01% to




to about 20%
about 20%


186

Hydrastis canadensis from about 0.01%


Populas alba from about 0.01% to about




to about 20%
20%


187

Hydrastis canadensis from about 0.01%


Populus tremuloides from about 0.01% to




to about 20%
about 20%


188

Hydrastis canadensis from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 20%
about 25%


189

Hydrastis canadensis from about 0.01%


Sambucus nigra from about 0.01% to




to about 20%
about 20%


190

Hydrastis canadensis from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 20%
to about 20%


191

Hydrastis canadensis from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 20%
about 20%


192

Hydrastis canadensis from about 0.01%


Smilax medica from about 0.01% to about




to about 20%
20%


193

Hydrastis canadensis from about 0.01%


Tussilago farfara from about 0.01% to




to about 20%
about 15%


194

Hydrastis canadensis from about 0.01%


Veronica officinalis from about 0.01% to




to about 20%
about 15%


195

Hydrastis canadensis from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 20%
to about 15%


196

Capsella Bursa Pastoris from about


Matricaria chamomilla from about 0.01%




0.01% to about 20%
to about 20%


197

Capsella Bursa Pastoris from about


Nasturtium officinale from about 0.01% to




0.01% to about 20%
about 15%


198

Capsella Bursa Pastoris from about


Phytolacca decendra from about 0.01% to




0.01% to about 20%
about 20%


199

Capsella Bursa Pastoris from about


Pimpinella saxifraga from about 0.01% to




0.01% to about 20%
about 20%


200

Capsella Bursa Pastoris from about


Populas alba from about 0.01% to about




0.01% to about 20%
20%


201

Capsella Bursa Pastoris from about


Populus tremuloides from about 0.01% to




0.01% to about 20%
about 20%


202

Capsella Bursa Pastoris from about


Rhus toxicodendron from about 0.01% to




0.01% to about 20%
about 25%


203

Capsella Bursa Pastoris from about


Sambucus nigra from about 0.01% to




0.01% to about 20%
about 20%


204

Capsella Bursa Pastoris from about


Sanguinaria Canadensis from about 0.01%




0.01% to about 20%
to about 20%


205

Capsella Bursa Pastoris from about


Scrophularia nodosa from about 0.01% to




0.01% to about 20%
about 20%


206

Capsella Bursa Pastoris from about


Smilax medica from about 0.01% to about




0.01% to about 20%
20%


207

Capsella Bursa Pastoris from about


Tussilago farfara from about 0.01% to




0.01% to about 20%
about 15%


208

Capsella Bursa Pastoris from about


Veronica officinalis from about 0.01% to




0.01% to about 20%
about 15%


209

Capsella Bursa Pastoris from about


Vincetoxicum officinale from about 0.01%




0.01% to about 20%
to about 15%


210

Matricaria chamomilla from about


Nasturtium officinale from about 0.01% to




0.01% to about 20%
about 15%


211

Matricaria chamomilla from about


Phytolacca decendra from about 0.01% to




0.01% to about 20%
about 20%


212

Matricaria chamomilla from about


Pimpinella saxifraga from about 0.01% to




0.01% to about 20%
about 20%


213

Matricaria chamomilla from about


Populas alba from about 0.01% to about




0.01% to about 20%
20%


214

Matricaria chamomilla from about


Populus tremuloides from about 0.01% to




0.01% to about 20%
about 20%


215

Matricaria chamomilla from about


Rhus toxicodendron from about 0.01% to




0.01% to about 20%
about 25%


216

Matricaria chamomilla from about


Sambucus nigra from about 0.01% to




0.01% to about 20%
about 20%


217

Matricaria chamomilla from about


Sanguinaria Canadensis from about 0.01%




0.01% to about 20%
to about 20%


218

Matricaria chamomilla from about


Scrophularia nodosa from about 0.01% to




0.01% to about 20%
about 20%


219

Matricaria chamomilla from about


Smilax medica from about 0.01% to about




0.01% to about 20%
20%


220

Matricaria chamomilla from about


Tussilago farfara from about 0.01% to




0.01% to about 20%
about 15%


221

Matricaria chamomilla from about


Veronica officinalis from about 0.01% to




0.01% to about 20%
about 15%


222

Matricaria chamomilla from about


Vincetoxicum officinale from about 0.01%




0.01% to about 20%
to about 15%


223

Nasturtium officinale from about 0.01%


Phytolacca decendra from about 0.01% to




to about 15%
about 20%


224

Nasturtium officinale from about 0.01%


Pimpinella saxifraga from about 0.01% to




to about 15%
about 20%


225

Nasturtium officinale from about 0.01%


Populas alba from about 0.01% to about




to about 15%
20%


226

Nasturtium officinale from about 0.01%


Populus tremuloides from about 0.01% to




to about 15%
about 20%


227

Nasturtium officinale from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 15%
about 25%


228

Nasturtium officinale from about 0.01%


Sambucus nigra from about 0.01% to




to about 15%
about 20%


229

Nasturtium officinale from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 15%
to about 20%


230

Nasturtium officinale from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 15%
about 20%


231

Nasturtium officinale from about 0.01%


Smilax medica from about 0.01% to about




to about 15%
20%


232

Nasturtium officinale from about 0.01%


Tussilago farfara from about 0.01% to




to about 15%
about 15%


233

Nasturtium officinale from about 0.01%


Veronica officinalis from about 0.01% to




to about 15%
about 15%


234

Nasturtium officinale from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 15%
to about 15%


235

Phytolacca decendra from about 0.01%


Pimpinella saxifraga from about 0.01% to




to about 20%
about 20%


236

Phytolacca decendra from about 0.01%


Populas alba from about 0.01% to about




to about 20%
20%


237

Phytolacca decendra from about 0.01%


Populus tremuloides from about 0.01% to




to about 20%
about 20%


238

Phytolacca decendra from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 20%
about 25%


239

Phytolacca decendra from about 0.01%


Sambucus nigra from about 0.01% to




to about 20%
about 20%


240

Phytolacca decendra from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 20%
to about 20%


241

Phytolacca decendra from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 20%
about 20%


242

Phytolacca decendra from about 0.01%


Smilax medica from about 0.01% to about




to about 20%
20%


243

Phytolacca decendra from about 0.01%


Tussilago farfara from about 0.01% to




to about 20%
about 15%


244

Phytolacca decendra from about 0.01%


Veronica officinalis from about 0.01% to




to about 20%
about 15%


245

Phytolacca decendra from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 20%
to about 15%


246

Pimpinella saxifraga from about 0.01%


Populas alba from about 0.01% to about




to about 20%
20%


247

Pimpinella saxifraga from about 0.01%


Populus tremuloides from about 0.01% to




to about 20%
about 20%


248

Pimpinella saxifraga from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 20%
about 25%


249

Pimpinella saxifraga from about 0.01%


Sambucus nigra from about 0.01% to




to about 20%
about 20%


250

Pimpinella saxifraga from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 20%
to about 20%


251

Pimpinella saxifraga from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 20%
about 20%


252

Pimpinella saxifraga from about 0.01%


Smilax medica from about 0.01% to about




to about 20%
20%


253

Pimpinella saxifraga from about 0.01%


Tussilago farfara from about 0.01% to




to about 20%
about 15%


254

Pimpinella saxifraga from about 0.01%


Veronica officinalis from about 0.01% to




to about 20%
about 15%


255

Pimpinella saxifraga from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 20%
to about 15%


256

Populas alba from about 0.01% to about


Populus tremuloides from about 0.01% to




20%
about 20%


257

Populas alba from about 0.01% to about


Rhus toxicodendron from about 0.01% to




20%
about 25%


258

Populas alba from about 0.01% to about


Sambucus nigra from about 0.01% to




20%
about 20%


259

Populas alba from about 0.01% to about


Sanguinaria Canadensis from about 0.01%




20%
to about 20%


260

Populas alba from about 0.01% to about


Scrophularia nodosa from about 0.01% to




20%
about 20%


261

Populas alba from about 0.01% to about


Smilax medica from about 0.01% to about




20%
20%


262

Populas alba from about 0.01% to about


Tussilago farfara from about 0.01% to




20%
about 15%


263

Populas alba from about 0.01% to about


Veronica officinalis from about 0.01% to




20%
about 15%


264

Populas alba from about 0.01% to about


Vincetoxicum officinale from about 0.01%




20%
to about 15%


265

Populus tremuloides from about 0.01%


Rhus toxicodendron from about 0.01% to




to about 20%
about 25%


266

Populus tremuloides from about 0.01%


Sambucus nigra from about 0.01% to




to about 20%
about 20%


267

Populus tremuloides from about 0.01%


Sanguinaria Canadensis from about 0.01%




to about 20%
to about 20%


268

Populus tremuloides from about 0.01%


Scrophularia nodosa from about 0.01% to




to about 20%
about 20%


269

Populus tremuloides from about 0.01%


Smilax medica from about 0.01% to about




to about 20%
20%


270

Populus tremuloides from about 0.01%


Tussilago farfara from about 0.01% to




to about 20%
about 15%


271

Populus tremuloides from about 0.01%


Veronica officinalis from about 0.01% to




to about 20%
about 15%


272

Populus tremuloides from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 20%
to about 15%


273

Rhus toxicodendron from about 0.01% to


Sambucus nigra from about 0.01% to




about 25%
about 20%


274

Rhus toxicodendron from about 0.01% to


Sanguinaria Canadensis from about 0.01%




about 25%
to about 20%


275

Rhus toxicodendron from about 0.01% to


Scrophularia nodosa from about 0.01% to




about 25%
about 20%


276

Rhus toxicodendron from about 0.01% to


Smilax medica from about 0.01% to about




about 25%
20%


277

Rhus toxicodendron from about 0.01% to


Tussilago farfara from about 0.01% to




about 25%
about 15%


278

Rhus toxicodendron from about 0.01% to


Veronica officinalis from about 0.01% to




about 25%
about 15%


279

Rhus toxicodendron from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 25%
to about 15%


280

Sambucus nigra from about 0.01% to


Sanguinaria Canadensis from about 0.01%




about 20%
to about 20%


281

Sambucus nigra from about 0.01% to


Scrophularia nodosa from about 0.01% to




about 20%
about 20%


282

Sambucus nigra from about 0.01% to


Smilax medica from about 0.01% to about




about 20%
20%


283

Sambucus nigra from about 0.01% to


Tussilago farfara from about 0.01% to




about 20%
about 15%


284

Sambucus nigra from about 0.01% to


Veronica officinalis from about 0.01% to




about 20%
about 15%


285

Sambucus nigra from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 20%
to about 15%


286

Sanguinaria Canadensis from about


Scrophularia nodosa from about 0.01% to




0.01% to about 20%
about 20%


287

Sanguinaria Canadensis from about


Smilax medica from about 0.01% to about




0.01% to about 20%
20%


288

Sanguinaria Canadensis from about


Tussilago farfara from about 0.01% to




0.01% to about 20%
about 15%


289

Sanguinaria Canadensis from about


Veronica officinalis from about 0.01% to




0.01% to about 20%
about 15%


290

Sanguinaria Canadensis from about


Vincetoxicum officinale from about 0.01%




0.01% to about 20%
to about 15%


291

Scrophularia nodosa from about 0.01%


Smilax medica from about 0.01% to about




to about 20%
20%


292

Scrophularia nodosa from about 0.01%


Tussilago farfara from about 0.01% to




to about 20%
about 15%


293

Scrophularia nodosa from about 0.01%


Veronica officinalis from about 0.01% to




to about 20%
about 15%


294

Scrophularia nodosa from about 0.01%


Vincetoxicum officinale from about 0.01%




to about 20%
to about 15%


295

Smilax medica from about 0.01% to


Tussilago farfara from about 0.01% to




about 20%
about 15%


296

Smilax medica from about 0.01% to


Veronica officinalis from about 0.01% to




about 20%
about 15%


297

Smilax medica from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 20%
to about 15%


298

Tussilago farfara from about 0.01% to


Veronica officinalis from about 0.01% to




about 15%
about 15%


299

Tussilago farfara from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 15%
to about 15%


300

Veronica officinalis from about 0.01% to


Vincetoxicum officinale from about 0.01%




about 15%
to about 15%









In another non-limiting aspect, disclosed herein are process for obtaining a plant extract, the process comprising the step of a) mixing the plant with water and/or another solvent, b) distilling the mixture, and c) collecting the distillate.


In some embodiments, the process further comprises the step of d) separating the aqueous phase from the oil phase and collecting the aqueous phase, after step c).


In some embodiments, the process further comprises the step of e) adding more of the plant to the aqueous phase and fermenting the mixture, after step c) or after step d).


In some embodiments, the process further comprises the step of f) distilling the fermented mixture and collecting the distillate, after step e).


In some embodiments, the process further comprises the steps of g) heating the remaining plant material until most of the moisture has evaporated, after step f), and h) extracting the water soluble salts or hygroscopic salts from the dried plant material. In some embodiments, the remaining plant material is not completely dry. In other embodiments, the remaining plant material is completely dry. In further embodiments, the remaining plant material begins to char. In yet other embodiments, the remaining plant material begins to incinerate.


In some embodiments, the process further comprises the step of i) adding the distillate of step e) to the extracted salts of step h).


In another non-limiting aspect, disclosed herein are herbal extractions obtained by the above process.


When afflicted with an epidermal condition, the human skin naturally works to alleviate the symptoms of the condition. For example, in most cases, redness, itching, or scaling due to some disorders improve over time, or until the next episode of a flare up. The herbal preparations disclosed herein help the skin in its natural course to reduce the adverse symptoms. Without being bound to a particular theory, the present inventors believe that the present herbal preparations provide the skin with the nutrients and building blocks necessary to efficiently and effectively work to reduce the symptoms.


Thus, in another non-limiting aspect, disclosed herein are methods of reducing symptoms associated with a skin condition in a subject, comprising identifying the subject in need thereof and administering to the subject an effective amount of an herbal preparation as disclosed herein.


In some embodiments, the symptoms associated with a skin condition include, but are not limited to, redness, itching, scaling, flaking, dry skin, acne, and the like associated with disorders such as acne vulgaris, psoriasis, eczema, or atopic dermatitis. In certain embodiments, the skin symptom is pruritis (itching), erythema (redness), or excoriations (flaking).


The term “subject” refers to an animal, such as (but not limited to) a mammal, and more particularly (but not by way of limitation) a human, who is the object of treatment, observation or experiment. The mammal may be selected from the group consisting of mice, rats, rabbits, guinea pigs, dogs, cats, sheep, goats, cows, primates, such as monkeys, chimpanzees, and apes, and humans.


The term “effective amount” or “therapeutically effective amount” is used to indicate an amount of an herbal preparation that elicits the biological response indicated. This response may occur in a tissue, system, animal or human and includes alleviation of the symptoms being treated.


In another non-limiting aspect, disclosed herein are compositions comprising the herbal preparations disclosed herein and at least one physiologically acceptable excipient, diluent, or carrier.


The term “excipient” refers to a substance added to the compositions disclosed herein. In some cases, the herbal preparations disclosed herein may not by itself be easily administered and/or absorbed by the subject. In these cases the herbal preparations may be dissolved into or mixed with an excipient. Excipients are also sometimes used to bulk up formulations that contain the herbal preparations, to allow for convenient and accurate application. In addition to their use in the single application quantity, excipients can be used in the manufacturing process to aid in the handling of the herbal preparations concerned. Excipients also aid in stabilizing the formulations of the herbal preparations, for example by keeping the various ingredients in solution or in suspension, preventing precipitation or crystallization, or adherence to container walls.


The term “carrier” defines a chemical compound that facilitates the incorporation of a compound into cells or tissues. For example, dimethyl sulfoxide (DMSO) is a commonly utilized carrier as it facilitates the uptake of many organic compounds into the cells or tissues of a subject.


The term “diluent” defines chemical compounds diluted in water that will dissolve the herbal extracts of interest and/or stabilize the formulation of the herbal preparations, including shelf life. Salts dissolved in buffered solutions are utilized as diluents in the art. One commonly used buffered solution is phosphate buffered saline because it mimics the salt conditions of human blood. Since buffer salts can control the pH of a solution at low concentrations, a buffered diluent rarely modifies the benefit of the herbal preparation.


Accordingly, disclosed herein are compositions and methods for the alleviation of the symptoms of skin conditions. The herbal preparations of the present disclosure can be delivered or administered to a mammal, (e.g., human subject), alone, or in the form of a formulated composition wherein the herbal preparation is mixed with suitable carriers or excipient(s) in an effective amount.


The herbal preparations that are used in the methods disclosed herein can be administered as formulated compositions comprising the herbal preparation together with one or more other physiologically acceptable component. Compositions can be in the form of solids (i.e., powders, granules, dragees, tablets, or pills), semi-solids (i.e., gels, slurries, or ointments), or liquids.


Suitable routes of administration may, for example, include oral, topical, rectal, transmucosal, epidural, vaginal, transdermal, or buccal administration.


Suitable formulations for use in the present disclosure are found in, for example, Remington's Pharmaceutical Sciences, Mack Publishing Company, Philadelphia, PA, 17th ed. (1985) and Langer, Science, 249:1527-1533 (1990). The compositions described herein can be manufactured in a conventional manner, e.g., mixing, dissolving, granulating, dragee-making, levigating, emulsifying, encapsulating, entrapping, or lyophilizing processes.


The herbal preparations can be formulated with common excipients, diluents or carriers, and compressed into tablets, or formulated as elixirs or solutions for convenient oral administration. The agents can also be formulated as sustained release dosage forms and the like.


The compositions disclosed herein may be manufactured in a manner that is itself known, e.g., by means of conventional mixing, dissolving, granulating, dragee-making, levigating, emulsifying, encapsulating, entrapping or tabletting processes.


Compositions for use in accordance with the present disclosure thus may be formulated in a conventional manner using one or more physiologically acceptable carriers comprising excipients and auxiliaries, which facilitate processing of the herbal extracts into herbal preparations. Proper formulation is dependent upon the route of administration chosen. Any of the well-known techniques, carriers, and excipients may be used as suitable and as understood in the art; e.g., in Remington's Pharmaceutical Sciences, above.


For transmucosal administration, penetrants appropriate to the barrier to be permeated are used in the formulation. Such penetrants are generally known in the art.


Compositions suitable for use in accordance with the present disclosure include compositions wherein the herbal preparations are contained in an effective amount. The effective amounts for the methods of the present disclosure can depend on a variety of factors, including, e.g., age, body weight, general health, sex, diet, time and manner of administration, and the severity of the particular affliction being treated.


EXAMPLES
Example 1: Herb Extraction
Procedure A

Herb extraction was achieved by steam distillation. Optionally, one or more of the steps of oil separation, fermentation, hygroscopic salt extraction, and cohobation was added to the steam distillation step. The procedures were as follows.


Steam Distillation

Three liters of deionized water was poured into a 5 L distillation apparatus flask, which was then placed on a sand bath. Herb was added to the distillation apparatus flask until the flask was about half full. A filter paper was placed at the joint of the distillation apparatus before hooking up the reaction head adaptor. A 2 L receiving flask was used. Low heat was provided, sufficient for steam to cloud the distillation apparatus and adapter. After 1.5 L of distillate was collected, the heat was turned off and the apparatus was allowed to cool. The distillate was removed. One liter of deionized water was added to the distillation apparatus flask and the distillation was repeated. The distillation was repeated three times.


Oil Separation

The distillate, containing an aqueous phase and an oil phase, was transferred into a foil drain tube. The stopcock at the end of the drain tube was opened and the water was drained off into a 5 L flask.


Fermentation

Herb was placed into the 5 L flask containing the water after oil separation. The flask was sealed using a secure fermentation lock, and was incubated at 27° C. for two weeks. Subsequently, the water was distilled 5 times and the distillate was saved in a separate container.


Hygroscopic Salt Extraction

The remaining plant material was boiled until the moisture was evaporated and the plant material began to incinerate. Once the incinerated plant material became grey, it was removed from heat and allowed to cool. A Soxhlet extractor was used to extract the water soluble salts from the incinerated plant material. The salts were isolated by rotary evaporation. The extracted salts were placed in a calcining kiln at 600° C. for 1 week. The process was repeated for a total of 3 times.


Cohobation

The solution obtained after fermentation and the volatile oils were added to the isolated salts. The mixture was incubated at 30° C. for 1 week. The herbal-medicinal concentrate was separated without disturbing the sediment. The concentrate can be diluted as needed.


Procedure B

Each individual plant raw material was subjected to steam distillation. After distillation the leftover material was in the form of wet mass. Additional water was added and the mixture was allowed to ferment in a glass container covered with a cloth lid. Fermentation was continued for 7 days at room temperature. During the fermentation the pH was monitored. Fermentation was allowed to continue until the mixtures began to putrefy. After the fermentation was over the biomass was filtered through a cloth filter and was subjected to distillation at 80-90° C. to get 30-40% of distillate of filtrate.


The leftover biomass was transferred to trays made from GI/MS and covered with cloth and was kept for drying in the shade. The drying was continued until the biomass became crisp dry, i.e., for about 15-20 days. During this time the material was turned around once in a day. After drying the material was subjected to ashing by either 1) burning the dry mass and collecting the cooled ash, which was then transferred to a crucible and heated further in an oven, or 2) incinerating the biomass by heating in a crucible at 600° C. The ash obtained is dissolved in distilled water and subjected to further distillation. All distillates were combined together and subjected to cohobation, where the combined product is heated under reflux for some time.


Example 2: Herbal Preparations

For the experiments detailed below, a unique herbal preparation (HAT-01) was used. Table 2 shows the herbs and their weight percentages within this formulation.









TABLE 2







Composition of HAT-01













Percentage


Genus
Species
Common Name
Composition














Conium


maculatum

Hemlock
12.1



Hamamelis


virginiana

Witch hazel
8.9



Rhus


toxicodendron

Ivy
8.3


Avena

sativa

Oat
6.8



Hydrastis


canadensis

Orange root
6.0



Phytolacca


decandra

Poke root
5.8



Cochlearia


officinalis

Scurvy grass
5.1



Populus


alba

White Poplar
4.9



Populus


tremuloides

Quaking Aspen
4.8



Sanguinaria


canadensis

Blood root
4.5



Berberis


vulgaris

Barberry
4.1



Scrophularia


nodosa

Figwort
4.0



Ervum


lens

Lentil
3.7



Smilax


medica

Sarsaparilla
3.1



Achillea


millefolium

Yarrow
2.5



Aesculus


hippocastanum

Horsechestnut
2.4



Capsella


Bursa Pastoris

Shepherd's Purse
2.3



Matricaria


chamomilla

Chamomile
2.2



Althaea


officinalis

Mallow
2.0



Sambucus


nigra

Elderberry
1.9



Pimpinella


saxifraga

Burnet
1.1



Vincetoxicum


officinale

Swallow wort
0.9



Nasturtium


officinale

Watercress
0.9



Tussilago


farfara

Colts foot
0.9



Veronica


officinalis

Speedwell
0.8




Total
100









Furthermore, to compare constituent efficacy and synergism, HAT-01 was also partially formulated into two: HAT-01:P1 and HAT-01:P2 as described in Tables 3 and 4, respectively. These herbs have established clinical benefit, and are considered safe for clinical use in chronic inflammatory conditions.









TABLE 3







Composition of HAT-01:P1













Percentage



Genus
Species
Composition
















Conium


maculatum

21




Rhus


toxicodendron

17




Cochlearia


officinalis

10




Hydrastis


canadensis

8




Phytolacca


decandra

8




Berberis


vulgaris

8




Scrophularia


nodosa

8




Smilax


medica

6




Matricaria


chamomilla

4




Pimpinella


saxifraga

2




Vincetoxicum


officinale

2




Nasturtium


officinale

2




Tussilago


farfara

2




Veronica


officinalis

2




Total
100

















TABLE 4







Composition of HAT-01:P2













Percentage



Genus
Species
Composition
















Hamamelis


virginiana

13




Avena


sativa

14




Populus


alba

10




Populus


tremuloides

10




Sanguinaria


canadensis

9




Ervum


lens

8




Achillea


millefolium

5




Aesculus


hippocastanum

5




Hydrastis


canadensis

5




Capsella


Bursa Pastoris

5




Althaea


officinalis

4




Conium


maculatum

4




Phytolacca


decandra

4




Sambucus


nigra

4




Total
100










Our NMR analyses of the ingredients in HAT-01 have confirmed the relative concentrations of components, and absolute concentrations of known substances. Of note, results from 1H-NMR spectroscopic analyses of HAT-01 showed no evidence of a corticosteroid moiety, which correlates well with our findings that no changes were observed in serum cortisol levels in mice before and after treatment with 10% oral HAT-01, and demonstrating that HAT-01 effects are nonsteroidal.


Example 3: Benefits of HAT-01 in Patients with Psoriasis: Pilot Trial

To assess the benefits of HAT-01 in psoriasis, we performed an 8-week, open-label, two armed study (HAT-01 and OTC medication arm) in patients with mild to moderate chronic plaque psoriasis. Patients (aged 18 to 70 years) with stable chronic plaque psoriasis of at least 6 months duration with a psoriasis body surface area (BSA)≤10% were included. All areas with the exception of the face, groin and axillae were treated. Patients with current or recent malignancies, severe asthma, infections, uncontrolled hypertension, and/or those treated with systemic or topical corticosteroid or immunosuppressant agents were excluded from the study. Patients with abnormal screening laboratory values, as well as pregnant women, were also excluded from the study. Patients were not allowed to use any medicated cosmetics that might influence the outcome of the study. A total of 16 patients fulfilling psoriasis inclusion criteria were enrolled into an exploratory 8 week, open-label study designed to investigate the safety, utility and tolerability of HAT-01. Patients were enrolled into one of two arms: (a) twice-daily application of HAT-01 (n=9 patients) or (b) twice-daily application of over-the-counter topical medications which are first-line therapy for patients with psoriasis and included topical vitamin D3 analog calcipotriene or topical retinoids (n=7 patients). Approximately 300 μl of HAT-01 was applied per lesion, prepared as a 10% dilution of the concentrated herbal extracts in 4.9% EtOH. The primary outcome was defined as the percentage change from baseline in the body surface area affected by psoriasis at weeks 2, 4, and 8 following treatment. Safety evaluations included tolerability assessments and incidence of adverse events.


Patients were evaluated for changes in total body surface area, erythema, scaling, and plaque resolution. Patients with moderate disease activity who received HAT-01 demonstrated an average 42% reduction in the percentage in body surface area affected by psoriasis at 8 weeks, whereas those treated with a control OTC topical vitamin D3 analog calcipotriene and topical retinoids exhibited a reduction in the percentage in body surface area affected by psoriasis by only 12% (FIG. 1). Significant resolution in erythema and scaling with changes in plaque elevation (from that of marked to slight) was observed in 8 of 9 patients after 8 weeks of HAT-01 treatment.


HAT-01 was well tolerated, with no treatment-related adverse events observed throughout the 8-week trial. At week 8, all patients treated with HAT-01 had no reports of skin atrophy, pruritus, or burning/stinging. In contrast at 8 weeks of treatment, 4 of 7 patients that were treated with control OTC topical vitamin D3 analog calcipotriene exhibited local treatment-site irritation, burning sensation, and pain.


Example 4: Therapeutic Effects of HAT-01 in Patients with Acne Vulgaris: Clinical Vignettes

To assess the effects of HAT-01 in acne vulgaris, an open-label study of HAT-01 in subjects with mild to moderate (grade I and II) acne vulgaris was undertaken at an outpatient setting of a private practice clinic. Subjects aged 18 to 50 years of age with ≥three inflammatory or non-inflammatory lesions of papules or pustules in the face were included. Exclusion criteria included: severe acne, the use of any anti-acne medications within the preceding four weeks, or subjects with cystic lesions or any acne requiring systemic treatment. Subjects were not allowed to use any medicated cosmetics that might influence the outcome of the study. A total of 4 patients fulfilling criteria were enrolled. The primary efficacy outcome was defined as the change from baseline of the total lesion count. Subjects were asked to follow a 4 week regimen of twice daily applications of HAT-01 (300 μl applied per lesion, prepared as a 10% dilution of the concentrated herbal extracts in 4.9% EtOH). An analysis of the post-treatment inflammatory and non-inflammatory lesion counts demonstrated a highly significant reduction of scores from baseline to 4 week time points, indicative of the therapeutic potential of HAT-01 in acne vulgaris. HAT-01 was well tolerated, with no treatment-related adverse events observed throughout the 4-week trial including no reports of skin atrophy, pruritus, or burning/stinging at the local treatment-site.


Example 5: Clinical Studies
Methodology

The clinical trial was conducted in a contract research organization setting with three investigators (dermatologists) in a multi-center site. Patients were block randomized from a central location into each study arm. Patients were assessed both before and throughout the course of treatment at each visit using by SCORAD and a Patient Benefit Index (which assesses AD patient-relevant treatment benefit). SCORAD values, ranging from 0 to 103, are classified as mild (<15), moderate (16-40) and severe (>41), and are calculated as (0.2×Area)+(3.5×Erythema+Edema+Crust+Excoriation+Lichenification+Dryness)+(pruritis+sleep loss). All three investigators were given prior training and testing for standardized scoring of SCORAD in AD, an approach that has been found to be significantly beneficial for minimizing observer variability.


Our primary objective was the efficacy of HAT-01, HAT-01P1, and/or HAT-01P2 in the reduction of pruritus in atopic dermatitis patients.


Our secondary objective(s) were to evaluate the therapeutic benefit of HAT-01, HAT-01P1, and/or HAT-01P2 in atopic dermatitis as measured by the SCORAD (SCORing Atopic Dermatitis),


evaluate the therapeutic benefit of HAT-01, HAT-01P1, and/or HAT-01P2 to reduce pruritus from patient's perspective as assessed by the Patient Benefit Index, and


safety and tolerability of HAT-01, HAT-01P1, and/or HAT-01P2 in atopic dermatitis patients.


Double Blinded Randomization: A double blind approach where both investigators and patients are blinded was used. Investigators performed enrollment and blinded assignment using blinded labels. Assignments were rotated through enrollment by investigators to enable random continuous enrollment and avoid selection bias.


Treatment: Atopic dermatitis patients fulfilling eligibility (inclusion and exclusion criteria) were provided with an informed consent. A topical formulation of HAT-01, HAT-01P1, and/or HAT-01P2 was randomly and blindly provided (without patient knowledge) and followed through 2, 4, 8, and 12 weeks after treatment. Patients were assessed both before and throughout the course of treatment (each visit) for the following indices: SCORAD (SCORing Atopic Dermatitis), Patient Benefit Index. Each patient also had up to 10 mls of blood drawn prior to (0) and at 4, and 12, weeks post-therapy to distinguish laboratorial and cytokine changes over time. Serum from 64 patients with AD on an approved randomized single blind placebo-controlled clinical trial of HAT-01, placebo and partial formulations of HAT-01 were obtained for all groups at 3 time points (0, 4, 12 weeks).


Therapeutic Effects of HAT-01 in Patients with Atopic Dermatitis: Pilot Trial


To correlate our findings in human patients with AD, we performed an exploratory 10-week, open-label study to evaluate the utility of HAT-01 in atopic dermatitis. Significant resolution of symptoms and signs of AD was observed through a Three Item Severity score in 15 of 18 patients after 4 weeks of topical HAT-01 treatment, with no relapses at 10-weeks of follow up. We then performed pilot clinical studies to evaluate the utility of HAT-01 in atopic dermatitis. Patients with severe asthma and/or those treated with systemic or topical (greater than medium strength) corticosteroids or immunosuppressant agents were excluded from the study. An exploratory 10-week, open-label study was designed to investigate the safety, efficacy and tolerability of a twice-daily application of a topical formulation of HAT-01 in AD. A total of 18 patients fulfilling diagnostic criteria for AD were enrolled and placed on a regimen of twice daily application of a topical formulation of HAT-01 (300 μl of 1:10). FIG. 2 portrays the design outline of this pilot trial. The primary efficacy outcome was defined as the change in the Three Item Severity score (TIS score) of AD based on the evaluation of erythema, oedema/papulation and excoriation in each representative lesion. Significant resolution of symptoms and signs of AD was observed in 83% of patients (15 of 18) after 4 weeks of HAT-01 treatment, with no relapses at 8-week or 10-week follow up (FIG. 3). Patients with severe disease activity pretreatment (TIS score>6) demonstrated an average 54.6% reduction in disease activity at 4-weeks, and an average of 77.1% reduction in disease activity by 10-weeks (FIG. 3). Of note, a significant reduction in edema and erythema was observed within 2-weeks, which was followed by improvements in oozing and excoriations within 4 weeks following treatment with HAT-01. Significant improvement in xerosis (dryness) was also immediately observed, while improvement in lichenification (thickening) took up to 10 weeks for effective resolution.


AD: Therapeutic effects of HAT-01 in patients with atopic dermatitis: Randomized placebo-controlled trial. To further investigate the safety, efficacy and tolerability of a twice-daily application of a topical formulation of HAT-01 in atopic dermatitis (AD), a total of 64 patients fulfilling inclusion criteria for AD were enrolled into a randomized placebo-controlled single (patient) blind clinical trial with a regimen of twice daily application of a topical formulation of HAT-01 (300 μl of 1:10). The primary efficacy outcome was defined as the change in the Severity Scoring of Atopic Dermatitis (SCORAD) values. SCORAD values, ranging from 0 to 103, are classified as mild (<15), moderate (16-40) and severe (>41), and are calculated as (0.2×Area)+(3.5×Erythema+Edema+Crust+Excoriation+Lichenification+Dryness)+(pruritis+sleep loss). As shown in FIG. 4, significant resolution of symptoms and signs of AD was observed in 84% of patients after 4 weeks of HAT-01 treatment, with sustained effects and no relapses at 8-week or 12-weeks of follow up (FIG. 4). Placebo (vehicle) treatment had no significant effect on SCORAD values, and treatment with partial formulations HAT-01:P1 and HAT-01:P2 had only minimal effects relative to treatment with whole HAT-01 (FIG. 4). Significant reduction in edema and erythema was observed within 4-weeks, which was followed by improvements in oozing and excoriations within 8 weeks following treatment with HAT-01. Significant improvement in xerosis was also observed at 4 weeks, while improvement in lichenification took up to 12 weeks for effective resolution. Importantly, HAT-01 was well tolerated and no treatment-related adverse events were observed throughout the 12-week pilot trial, indicating the safe and potent therapeutic benefit of HAT-01 in a majority of the patients studied with AD.

Claims
  • 1. A topical composition formulated for application to a skin of a subject, the topical composition comprising: a mixture of at least seven different plant extracts, wherein each of the at least seven plant extracts is selected from the group consisting of Achillea millefolium; Aesculus hippocastanum; Althaea officinalis; Avena sativa; Berberis vulgaris; Capsella bursa-pastoris; Cochlearia officinalis; Conium maculatum; Ervum lens; Hamamelis virginiana; Hydrastis canadensis; Malva sylvestris; Matricaria chamomilla; Nasturtium officinale; Phytolacca decandra; Pimpinella saxifraga; Populus alba; Populus tremuloides; Rhus toxicodendron; Sambucus nigra; Sanguinaria canadensis; Scrophularia nodosa; Smilax medica; Tussilago farfara; Veronica officinalis; Vincetoxicum officinale; and combinations thereof; and wherein each of the at least seven different plant extracts is extracted in an extraction composition that comprises at least one solvent other than water, and wherein each of the at least seven different plant extracts is extracted by a process selected from the group consisting of steam distillation, oil separation, fermentation, hygroscopic salt extraction, and cohobation; andat least one pharmaceutically acceptable carrier, diluent, or excipient; andwherein the topical composition is in the form of a cream, gel, lotion, ointment, or salve for application to the skin of the subject.
  • 2. The topical composition of claim 1, wherein the mixture comprises at least eight different plant extracts.
  • 3. The topical composition of claim 1, wherein the mixture comprises at least ten different plant extracts.
  • 4. The topical composition of claim 1, wherein the mixture comprises at least twelve different plant extracts.
  • 5. The topical composition of claim 1, wherein the mixture comprises at least fourteen different plant extracts.
  • 6. The topical composition of claim 1, wherein the mixture comprises at least sixteen different plant extracts.
  • 7. The topical composition of claim 1, wherein the mixture comprises at least eighteen different plant extracts.
  • 8. The topical composition of claim 1, wherein the mixture comprises plant extracts obtained from Achillea millefolium; Aesculus hippocastanum; Althaea officinalis; Avena sativa; Berberis vulgaris; Capsella Bursa Pastoris; Cochlearia officinalis; Ervum lens; Hamamelis virginiana; Malva sylvestris; Matricaria chamomilla; Nasturtium officinale; Phytolacca decandra; Pimpinella saxifraga; Populas alba; Populus tremuloides; Sambucus nigra; Sanguinaria Canadensis; Scrophularia nodosa; Smilax medica; Tussilago farfara; Veronica officinalis; and Vincetoxicum officinale.
  • 9. The topical composition of claim 1, wherein the at least one solvent present in the extraction composition utilized with at least one of the plant extracts is selected from the group consisting of an alcohol, a polyhydric alcohol, an ether, an ester, a carboxylic acid, an amide, a carbonate, supercritical fluid carbon dioxide, an ionic liquid, an alkane, a petroleum-derived oil, a plant oil, and combinations thereof.
  • 10. The topical composition of claim 9, wherein the at least one solvent comprises ethanol.
  • 11. The topical composition of claim 1, wherein the extraction composition further comprises water.
  • 12. The topical composition of claim 1, wherein the topical composition is formulated as a sustained release dosage form.
  • 13. A method of reducing symptoms associated with a skin condition in a subject, wherein the skin condition is associated with acne vulgaris, psoriasis, eczema, atopic dermatitis, pruritis, erythema, or excoriations, the method comprising the steps of: identifying the subject in need thereof; andapplying an effective amount of the topical composition of claim 1 to a skin of the subject.
  • 14. A composition formulated for oral administration to a subject, the composition comprising: a mixture of at least seven different plant extracts, wherein each of the at least seven plant extracts is selected from the group consisting of Achillea millefolium; Aesculus hippocastanum; Althaea officinalis; Avena sativa; Berberis vulgaris; Capsella bursa-pastoris; Cochlearia officinalis; Conium maculatum; Ervum lens; Hamamelis virginiana; Hydrastis canadensis; Malva sylvestris; Matricaria chamomilla; Nasturtium officinale; Phytolacca decandra; Pimpinella saxifraga; Populus alba; Populus tremuloides; Rhus toxicodendron; Sambucus nigra; Sanguinaria canadensis; Scrophularia nodosa; Smilax medica; Tussilago farfara; Veronica officinalis; Vincetoxicum officinale; and combinations thereof; and wherein each of the at least seven different plant extracts is extracted in an extraction composition that comprises at least one solvent other than water, and wherein each of the at least seven different plant extracts is extracted by a process selected from the group consisting of steam distillation, oil separation, fermentation, hygroscopic salt extraction, and cohobation; andat least one pharmaceutically acceptable carrier, diluent, or excipient acceptable for oral administration to the subject.
  • 15. The oral composition of claim 14, wherein the mixture comprises at least ten different plant extracts.
  • 16. The oral composition of claim 14, wherein the mixture comprises at least sixteen different plant extracts.
  • 17. The oral composition of claim 14, wherein the mixture comprises plant extracts obtained from Achillea millefolium; Aesculus hippocastanum; Althaea officinalis; Avena sativa; Berberis vulgaris; Capsella Bursa Pastoris; Cochlearia officinalis; Ervum lens; Hamamelis virginiana; Malva sylvestris; Matricaria chamomilla; Nasturtium officinale; Phytolacca decandra; Pimpinella saxifraga; Populas alba; Populus tremuloides; Sambucus nigra; Sanguinaria Canadensis; Scrophularia nodosa; Smilax medica; Tussilago farfara; Veronica officinalis; and Vincetoxicum officinale.
  • 18. The oral composition of claim 14, wherein the at least one solvent present in the extraction composition utilized with at least one of the plant extracts is selected from the group consisting of an alcohol, a polyhydric alcohol, an ether, an ester, a carboxylic acid, an amide, a carbonate, supercritical fluid carbon dioxide, an ionic liquid, an alkane, a petroleum-derived oil, a plant oil, and combinations thereof.
  • 19. The oral composition of claim 18, wherein the extraction composition further comprises water.
  • 20. A method of reducing symptoms associated with a skin condition in a subject, wherein the skin condition is associated with acne vulgaris, psoriasis, eczema, atopic dermatitis, pruritis, erythema, or excoriations, the method comprising the steps of: identifying the subject in need thereof; andadministering an effective amount of the oral composition of claim 14 to the subject.
CROSS REFERENCE TO RELATED APPLICATIONS/INCORPORATION BY REFERENCE

This application is a continuation of U.S. patent application Ser. No. 17/684,811, filed Mar. 2, 2022, now abandoned; which is a continuation of U.S. patent application Ser. No. 16/842,528, filed Apr. 7, 2020, now abandoned; which is a continuation of U.S. patent application Ser. No. 15/889,921, filed Feb. 6, 2018, now abandoned; which is a continuation of U.S. patent application Ser. No. 14/733,771, filed Jun. 8, 2015, now U.S. Pat. No. 9,889,174, issued Feb. 13, 2018; which is a continuation of U.S. patent application Ser. No. 13/471,913, filed May 15, 2012, now U.S. Pat. No. 9,050,359, issued Jun. 9, 2015; which claims priority under 35 USC § 119(e) to U.S. Provisional Application No. 61/486,724, filed May 16, 2011. The entire contents of each of the above-referenced patent applications are hereby expressly incorporated herein by reference.

Provisional Applications (1)
Number Date Country
61486724 May 2011 US
Continuations (5)
Number Date Country
Parent 17684811 Mar 2022 US
Child 18659701 US
Parent 16842528 Apr 2020 US
Child 17684811 US
Parent 15889921 Feb 2018 US
Child 16842528 US
Parent 14733771 Jun 2015 US
Child 15889921 US
Parent 13471913 May 2012 US
Child 14733771 US