Use and application of a pharmaceutical composition containing a mixture of natural-origin heterocyclical guanidine, for cosmetology, wound healing, focal dystonia and muscular spasm-related clinical pathologies

Information

  • Patent Grant
  • 8889681
  • Patent Number
    8,889,681
  • Date Filed
    Tuesday, October 1, 2013
    11 years ago
  • Date Issued
    Tuesday, November 18, 2014
    9 years ago
Abstract
Pharmaceutical compositions comprising tricyclic 3,4-propinoperhydropurines and uses thereof for the treatment of facial wrinkling are provided.
Description
STATEMENT REGARDING FEDERALLY SPONSORED RESEARCH OR DEVELOPMENT

Not applicable.


REFERENCE TO MICROFICHE APPENDIX

Not applicable.


FIELD OF THE INVENTION

This invention relates to pharmaceutical compositions containing heterocyclic guanidine-type compounds and uses thereof for blocking neuronal transmission. More specifically, this invention relates to tricyclic 3,4-propinoperhydropurines and uses thereof for blocking neuronal transmission.


BACKGROUND OF THE INVENTION

The presence of wrinkles in the neck and face of people are seen as negative aesthetic effects by social groups. These marks reflect face aging and increase the subjective awareness of the age of people. Since the beginning of civilization, natural or synthetic chemical compounds have been used and procedures have been developed (i.e. plastic surgery) to alleviate this problem. For example, plastic surgeons and cosmetic centers have been experimenting with and using Botulin A toxin as a pharmaceutical preparation that produces facial rejuvenation by removing face wrinkles Botulin A toxin is a neurotoxin that acts by chemiodenervation, or blocking the presynaptic release of the neurotransmitter acetylcholine in the neuromuscular plate, thus interfering with neuromuscular transmission, paralysing the muscle and preventing its contraction for a period of up to 4 months. Applied locally in the face of people, its effect is a facial rejuvenation that appears within 7-10 days after the toxin is applied, and has a duration of approximately 4 months. Botulin A toxin has been used for the treatment of diseases associated with muscular spasm, focal dystonia, sphincter relaxation (achalasia and anal fissure), hyperhydrosis and urinary bladder relaxation.


While Botulin A toxin is effective as a facial rejuvenate, it is an enzyme that is inherently unstable. This instability makes its use and handling complicated and less desirable. In fact, it requires freezing before using and must be used within four hours of opening the container. Because it is an enzyme, Botulin A toxin also generates antibodies that prevent its use in consecutive injections and can also induce an allergic response. In addition, its results are delayed 7-10 days, which is undesirable for patients wanting an immediate result. Accordingly, a need exists for a facial rejuvenate that is stable, fast-acting and that is not an enzyme.


SUMMARY OF THE INVENTION

In accordance with the objects of the invention, novel compositions and methods are provided. In one aspect of the invention, pharmaceutical compositions for interfering with neuronal transmission comprising an effective amount of at least one tricyclic 3,4-propinoperhydropurine are provided.


In a second aspect of the invention, preparations for facial rejuvenation are provided that comprise an effective amount of the composition of the invention and a facial cream.


In a third aspect of the invention, methods of interfering with neuronal transmission comprising contacting a neuron with an effective amount of the pharmaceutical compositions of the invention are provided.


In a fourth aspect of the invention, methods of interfering with muscle contracting comprising contacting a muscle with an effective amount of the composition of the invention are provided.





DETAILED DESCRIPTION OF THE DRAWINGS


FIG. 1 is an illustration of an application pattern for the treatment of a human face.





DETAILED DESCRIPTION OF THE INVENTION

In accordance with the present invention, it has been discovered that compositions comprising heterocyclic guanidine-type compounds, and more specifically tricyclic 3,4-propinoperhydropurines, can be used for many cosmetic or clinical applications, without any surgery, side effects, allergies, immune rejection or hematoma. The compositions of the invention may be used to treat conditions including, but not limited to blepharospasm, strabismus, focal dystonia, sphinceter relaxation (achalasia and anal fissure), hyperhydrosis, urinary bladder relaxation, muscular spasm-related pain management, muscular spasms, improved wound healing and facial wrinkling In accordance with the present invention, muscular relaxation is immediate, usually occurring in less than five minutes.


The compositions of the invention comprise an effective amount of at least one tricyclic 3,4-propinoperhydropurine represented by the following structure:




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wherein R1 and R5 are independently H or OH; R2 and R3 are independently H or OSO3; and R4 is independently —OC(O)NH2, OH, H, —OC(O)NHSO3 or —OC(O)CH3; and a pharmacologically acceptable carrier. These tricyclic 3,4-propinoperhydropurines may be purified from dinoflagellates, cyanobacterias and also may be accumulated by highly contaminated mollusks, which are also temporary muscular relaxants when locally injected. Any pharmacologically acceptable carrier may be used, including but not limited to water. The compounds of the invention are generally diluted in a solution of acetic acid or 0.09% sodium chloride.


As used herein, “an effective amount” is that amount sufficient to interfere with neuronal transmission by blocking the presynaptic release of the neurotransmitter acetylcholine in the neuromuscular plate, thus interfering with transmission, paralysing the muscle and preventing it from contracting, or producing a relaxation of contracted muscles. For example, an effective amount of the compositions of the invention may be a 100 to 800 microliter dose of forty units per milliliter solution of tricyclic 3,4-propinoperhydropurines. The unit of activity is the amount of the composition of the invention necessary to block the muscular contractions of the crural biceps of a mouse leg for 1.5 to 2.0 hours. The compounds of the invention are generally diluted with a 10 mM (millimolar), pH 4 solution of acetic acid. In one specific embodiment of the invention, the compositions of the invention comprise 40 units per milliliter of a 10 mM, pH 4 solution of acetic acid.


In one embodiment of the invention, and with reference to Table 1 below, the pharmaceutical compositions of the invention comprise Saxitoxin. In a second embodiment of the invention, the pharmaceutical compositions of the invention comprise Gonyautoxin 2. In a third embodiment of the invention, the pharmaceutical compositions of the invention comprise Gonyautoxin 3. In a forth embodiment of the invention, the pharmaceutical compositions of the invention comprise Gonyautoxin 4. In a fifth embodiment of the invention, the pharmaceutical compositions of the invention comprise Gonyautoxin 5. In a sixth embodiment of the invention, the pharmaceutical compositions of the invention comprise neoSaxtoxin. In a seventh embodiment of the invention, the pharmaceutical compositions of the invention comprise Gonyautoxin 1. In an eighth embodiment of the invention, the pharmaceutical compositions of the invention comprise Decarbamoyl-Saxitoxin.









TABLE 1







Tricyclic 3,4-propinoperhydropurines












Compound
R1
R2
R3
R4
R5





Saxitoxin
H
H
H
—OC(O)NH2
OH


neoSaxitoxin
OH
H
H
—OC(O)NH2
OH


Decarbamoyl-
OH
H
H
OH
OH


Saxitoxin







Gonyautoxin 1
OH
H
OSO3
—OC(O)NH2
OH


Gonyautoxin 2
H
H
OSO3
—OC(O)NH2
OH


Gonyautoxin 3
H
OSO3
H
—OC(O)NH2
OH


Gonyautoxin 4
OH
OSO3
H
—OC(O)NH2
OH


Gonyautoxin 5
H
H
H
—OC(O)NHSO3
OH









In specific embodiments of the invention, the pharmaceutical compositions comprise a mixture of tricyclic 3,4-propinoperhydropurines. The compounds are purified and used individually and/or mixed together. In one preferred embodiment, the pharmaceutical compositions of the invention comprise a mixture of Gonyautoxin 2, Gonyautoxin 3, and Saxitoxin. In another preferred embodiment, the pharmaceutical compositions of the invention comprise a mixture of Gonyautoxin 4, Gonyautoxin 1, Gonyautoxin 5, Gonyautoxin 3 and Gonyautoxin 2. In yet another preferred embodiment, the pharmaceutical compositions of the invention comprise neoSaxitoxin and Gonyautoxin 2. In still another preferred embodiment, the pharmaceutical compositions of the invention comprise a mixture of Saxitoxin, neoSaxitoxin; Decarbamoyl-Saxitoxin, Gonyautoxin 3 and Gonyautoxin 2. It should be understood by those of skill in the art that other mixtures and combinations of tricyclic 3,4-propinoperhydropurines are within the scope of this invention.


In one embodiment of the invention, the compounds of the invention are used in combination with an effective amount of Botulin A toxin. In this embodiment, the pharmaceutical compositions of the invention comprise an effective amount of Botulin A toxin and an effective amount of at least one tricyclic 3,4-propinoperhydropurine. The combination may be used in any cosmetic or clinical application in which the compounds of the invention, or Botulin A toxin are used, for example, blepharospasm, strabismus, focal dystonia, sphincter relaxation (achalasia and anal fissure), hyperhydrosis, urinary bladder relaxation, muscular spasm-related pain management, muscular spasms, improved wound healing, and facial wrinkle removal.


These pharmaceutical compositions of the invention may be used for many cosmetic and clinical applications including, but not limited to blepharospasm, strabismus, focal dystonia, sphincter relaxation (achalasia and anal fissure), hyperhydrosis, urinary bladder relaxation, muscular spasm-related pain management, muscular spasms, improved wound healing, and facial wrinkle removal. Generally, the pharmaceutical compositions of the invention are applied locally in the form of preparations. To form preparations, an effective amount of the pharmaceutical compositions of the invention are added to a facial cream complete with its coadjuvants. Unlike Botulin A toxin, these preparations are stable at room temperature, do not require refrigeration, are sterilizable, do not generate antibodies, are not peptide in nature, act immediately, and may be injected repeatedly without any side effects.


Without being bound by theory, when applied locally, these compounds carry out their antispasmodic action by blocking the spreading of nervous impulse, or neuronal transmission, by reversibly binding to the sole biological molecular receptor, i.e. the voltage gated sodium channel, present in all neurons and excitable cells. By binding to this channel, there is no entry of sodium to the neuronal cell; depolarization does not occur and, therefore, propagation of the impulse is stopped. This action mechanism blocks the presynaptic release of the neurotransmitter acetylcholine in the neuromuscular plate, thus interfering with neuromuscular transmission, paralysing the muscle and preventing it from contracting, or producing a relaxation of muscles contracted by pathological problems. This mechanism is particularly efficient for cosmetic purposes, as it does not let some facial muscles contract, all of them associated with and responsible for the formation of wrinkles, thus producing the sought-after effect of facial rejuvenation.


The pharmaceutical preparations of the invention are applied locally around the muscle that is to be paralysed or prevented from contracting. The application should be in amounts of no more than one milliliter in different places around the muscle, particularly around the areas of greatest innervations. The unit of activity is the amount of the compositions of the invention necessary to block the contractions of the crural biceps of a mouse leg for 1.5 to 2 hours. The preferred dosage rate is 100 to 800 microliters per injected point, depending on the size, irrigation and anatomical location of the muscle, while maintaining a concentration of 20-40 units/milliliter. The effect is immediately apparent, generally occuring a maximum of thirty seconds after injection. The maximum effect may be seen within 15 minutes. Its effective duration depends on the dose administered, the muscle in question, as well as the volume and specific composition administered. This is the pattern for all clinical applications and pathologies. The injection may be accomplished by using a 1 milliliter, tuberculin-type disposable syringe with a twenty-seven to thirty gauge needle. In the case of strabismus, a dose of twenty to forty units in a volume of 50-100 microliters may be injected in the orbicular muscle. Use of the pharmaceutical preparations of the invention is limited to individuals over twelve years old. There is no contraindication for pregnant women.


The advantageous properties of this invention can be observed by reference to the following example, which is meant to illustrate, and not limit, the invention in any way.


EXAMPLE

Before the application, a photographic record is made of the person to be treated, first with her face resting and relaxed, and then, frowning and producing a maximum facial contraction. The person then places ice on their forehead and on the two lateral zones where the preparation is to be injected. With reference to FIG. 1, the application should follow a specific pattern. A volume is injected alongside each black-dot injection point shown in FIG. 1. A pharmaceutical composition comprising a (2:1:1 volume/volume) mixture of Gonyautoxin 2, Gonyautoxin 3 and Saxitoxin mixture is applied at a dose of 40 units/milliliter. Each injection is made with a 1 milliliter, tuberculin-type disposable syringe with a 27-30 gauge needle. After injecting, the point of injection is disinfected with a gauze soaked in bi-alcohol or in any other disinfectant. The total amount required to complete the face treatment is 1.7 milliliters.


The expected result is an immediate inability to frown and to show lines when the face is resting. The person experiences a feeling of facial stretching similar to that felt when applying a facial cream mask. After that, ice is applied on the injected zones for five minutes. Thirty minutes after the application, the patient gets used to the feeling of facial stretching. At that time, the person walks out with no discernible wrinkles, a rejuvenated facial look, no face marks or hematoma, and completely normal. The face recovers its normal color within twenty minutes, depending on how relaxed the injected patient has become. The whole application procedure takes ten minutes at the most, and produces a very slight pain from the needle and the injected solution. The pain disappears as soon as the syringe is withdrawn. There are no traumas of any kind, nor any sequelae. The patient may be checked the next day and every fifteen days thereafter. At this dose, the effect lasts for one month. After the first month, the treatment may be repeated as often as necessary.


In view of the above, it will be seen that all the objects and features of the present invention are achieved, and other advantageous results obtained. The examples and description of the invention contained herein is illustrative only, and is not intended in a limiting sense.

Claims
  • 1. A method of treating anal fissure in a human subject in need thereof comprising administering a therapeutically effective amount of a pharmaceutical composition comprising at least one compound selected from the group consisting of Gonyautoxin 1, Gonyautoxin 2, Gonyautoxin 3, Gonyautoxin 4, Gonyautoxin 5, and combinations thereof, and a pharmacologically acceptable carrier.
  • 2. The method of claim 1, wherein the composition comprises at least two compounds selected from the group consisting of Gonyautoxin 1, Gonyautoxin 2, Gonyautoxin 3, Gonyautoxin 4 and Gonyautoxin 5.
  • 3. The method of claim 1, wherein the carrier comprises acetic acid, water, or 0.09% sodium chloride.
  • 4. The method of claim 1, wherein the composition consists of a mixture of Gonyautoxin 2 and Gonyautoxin 3.
  • 5. The method of claim 1, wherein the composition is administered via injection at the site of the anal fissure.
  • 6. The method of claim 5, wherein the amount of the composition has a concentration of 20-40 units per milliliter.
  • 7. The method of claim 1, wherein the composition is applied topically.
  • 8. The method of claim 7, wherein the composition is a cream.
Priority Claims (1)
Number Date Country Kind
2764-2001 Nov 2001 CL national
CROSS REFERENCE TO RELATED APPLICATIONS

This application is a continuation of U.S. application Ser. No. 11/338,156, filed Jan. 24, 2006, which is a divisional of U.S. application Ser. No. 10/294,388 filed on Nov. 14, 2002. This application also claims priority under the Paris Convention for the Protection of Industrial Property to Chilean Patent Application Number 2764-2001, filed on Nov. 15, 2001 in the Department of Industrial Property in the Republic of Chile.

US Referenced Citations (44)
Number Name Date Kind
3957966 Valan May 1976 A
4001413 Adams et al. Jan 1977 A
4029794 Adams et al. Jun 1977 A
5183462 Borodic Feb 1993 A
5298019 Borodic Mar 1994 A
5437291 Pasricha et al. Aug 1995 A
5504117 Gorfine Apr 1996 A
5562907 Arnon Oct 1996 A
5674205 Pasricha et al. Oct 1997 A
5714468 Binder Feb 1998 A
5721215 Aoki et al. Feb 1998 A
5837265 Montal et al. Nov 1998 A
5908746 Suzuki et al. Jun 1999 A
6030974 Schwartz et al. Feb 2000 A
6117877 Fogel Sep 2000 A
6143306 Donovan Nov 2000 A
6187756 Lee et al. Feb 2001 B1
6261572 Donovan Jul 2001 B1
6299893 Schwartz et al. Oct 2001 B1
6306423 Donovan et al. Oct 2001 B1
6326020 Kohane et al. Dec 2001 B1
6358926 Donovan Mar 2002 B2
6407088 Dong et al. Jun 2002 B1
6416765 Donovan Jul 2002 B1
6432986 Levin Aug 2002 B2
6447787 Gassner et al. Sep 2002 B1
6552191 Zhou et al. Apr 2003 B1
6559154 Kang et al. May 2003 B2
6599906 Ku et al. Jul 2003 B1
6780866 Ku et al. Aug 2004 B2
20010046962 Graham Nov 2001 A1
20010053369 Donovan Dec 2001 A1
20010053370 Donovan Dec 2001 A1
20020025327 Schmidt Feb 2002 A1
20020086036 Walker Jul 2002 A1
20020142010 Graham Oct 2002 A1
20020161013 Liu et al. Oct 2002 A1
20020176872 Aoki et al. Nov 2002 A1
20020192240 Brooks et al. Dec 2002 A1
20020198226 Ku et al. Dec 2002 A1
20030036502 Gassner et al. Feb 2003 A1
20040009180 Donovan Jan 2004 A1
20040018213 Aoki et al. Jan 2004 A1
20040028706 Aoki et al. Feb 2004 A1
Foreign Referenced Citations (6)
Number Date Country
1192903 Sep 1998 CN
1363275 Aug 2002 CN
WO 9843619 Oct 1998 WO
WO 9851290 Nov 1998 WO
WO 0024419 May 2000 WO
WO 0136588 May 2001 WO
Non-Patent Literature Citations (44)
Entry
Abedrapo, et al., Dis. Colon Rectum, vol. 47, No. 4, Apr. 2004, p. 598.
Andrinolo, D., Gomes, P., Fraga, S., Soares de Silva, P., Lagos, N. “Transport of the organic cations gonyautoxin 2/3 epimers, a paralytic shellfish poision toxic, through the human and rat intestinal epitheliums” Toxicon, 40:(2002) 1389-1397.
Andrinolo, D., Iglesias, Y., Garcia, C., Lagos, N. “Toxicokinetics and toxicodynamics of gonyautoxins alter an oral toxin dose in cats” Toxicon, 40:(2002) 699-709.
Andrinolo, D., Lagos, N. “Paralytic shellfish poisioning (PSP). Toxicology and kinetcis” Seafood and freswater toxins , 10 (2000):203-215.
Andrinolo, D., Michael, L., Lagos, N. “Toxic effects, pharmacokinetics and clearance of saxitoxin, a component of paralytic shellfish poison (PSP), in cats” Toxicon, 37:(1999) 447-464.
Andrinolo, D., Santinelli, N., Otaño, S., Sastre, V. and Lagos, N. “Paralytic shellfish toxins in musels and Alexandrium tamarense at Valdes peninsula, Chubut, Patagonia, Argentina: kinetics of a natural depuration” Journal of Shellfish Research, 18 (1999): 203-209.
Andrinolo, et al., “Toxicokinetics and Toxicodynamics of Gonyautoxins after an Oral Toxin dose in Cats”, Toxicon, vol. 40, 2001, pp. 699-709.
Ates, O., Cayli, S.R., Article Neurological Res. 2007 Apr. 29(3): 317-23.
Barbier, Julian. Conotoxins targeting voltage-sensitive Na+ channels, Bacterial, Plant & Animal Toxins, 2003:127-145.
Borodic, G.E. And Pearce, L.B. “New Concepts in Botulinum Toxin Therapy.” Drug Safety. 1994, 11(3): pp. 145-152.
Botana, L. Seafood and Freshwater Toxins Pharmacology, Physiology, and Detection. (2000) Marcel Dekker, Inc., 203-215.
Bower, et al., “Nonprotein Neurotoxins”, Clinical Toxicology, 1981, vol. 18, No. 7, pp. 813-863.
Carruthers, A. Update on Botulinum Toxin. Skin Therapy Letter. (1999) 4: 1-2.
Carruthers, A., Kiene, K., and Carruthers, J. (1996) Botulinum A exotoxin use in clinical dermatology. 1 Am. Acad Dermatology. 34: 788-797.
Carruthers, J. and Carruthers, A. (2001) Botulinum Toxin (Botox) Chemodenervation for Facial Rejuvenation. Facial Plastic Surgery Clinics of North America. 9: 197-204.
Choudhary, G., Shang, L., Li, Xiufeng., and Dudley, Jr., Samuel C. “Energetic Localization of Saxitoxin in its Channel Binding Site” Biophysical Journal Aug. 2002: 912-919, vol. 83.
Compagnon, D., Garcia, C., Andrinolo, D., Salas, K., Ruiz-Tagle, N., Lagos, N. “Toxinas Paralizantes en microalgas. Un ejemplo de biodiversidad. Sustentabilidad de la Bioversidad” Universidad de Concepción, Chile , 2001:253-264.
Compagnon, D., Lembeye, G., Marcos, N., Ruiz-Tagle, N., Lagos, N. “Accumulation of Paralytic shellfish poisioning toxins in the bivalve Aulacomya ater and two carnivorous gastropods Concholepas, Concholepas and Agrobuccinum ranelliformes during an Alexandrium catenella bloom in Southern Chile” Journal of Shellfish Research, 17 (1998): 67-73.
Gennenah, A. A., Shimizu, Y., Specific Toxicity of Paralyric Shellfish Poisons, Journal of Agriculture Chemistry, 1981, 29, 1289-1291.
Hall, S., Strichartz, G., Moczydlowski, E., Ravindran, A., and Reichardt, P. B. The Saxitoxins; Sources, Chemistry, and Pharmacology. In: Marine Toxins: Origin, Structure and Molecular Pharmacology Eds., Hall, A., and Strichartz G American Chemical Society Symposium series 418. Washington, DC: American Chemical Society, (1990) pp. 29-65.
Heckmann, M., et al., “Botulinum Toxin A in dermatology”, Hautarzt, 1998, vol. 49, No. 2, pp. 87-90.
Ho, Philip T., MD, Gorup, Alexander M., MD, and Keen, Monte S., MD. “The Role of Botulinum Toxin A in the Long-term Prevention of Facial Wrinkles: A Preliminary Observational Report”, Otolaryngology—Head and Neck Surgery, Aug. 1997, vol. 117, No. 2, p. 161.
Ikawa et al., “Toxin Profiles of the blue-green alga aphanizomen flos-aquae” 1985, Toxic Dinoflagellates, Proc. Int. Conf. 3rd, 299-304.
Jankovic, J., and Brin, M.F. (1991) Therapeutic Uses of Botulinum Toxin. New England Journal of Medicine. 324: 1186-1194.
Ken, C Y. (1966) Tetrodotoxin, Saxitoxin and Their Significance in the Study of Excitation Phenomena Pharmacological Reviews 18: 997-1049.
Lagos, N. “Microalgal blooms: A global issue with negative impact in Chile” Biol. Res. 31 (1998): 375-386.
Lagos, N. “Principales Toxinas de origen Fitoplanctonico: Identificacion y cuantificacion mediante Cromatografia Liquida de Alta Resolucion (HPLC). Floraciones Algales Nocivas en el Cono sur Americana” Institute Espanol de Oceanografia, 2002.
Lagos, N., Garcia, C., Ruiz-Tagle, N., Andrinolo, D., Compagnon, D. & Sales, K. Toxinas paralizantes en microalgas Un ejemplo de biodiversidad. Universidad de Concepcion-Chile, 2001: 253-264.
Lagos, N., Onodera, H., Zagatto, P.A., Andrinolo, D., Azevedo, S., Oshima, Y. The first evidence of paralytic shellfish toxins in the freshwater cyanobacterium Cylindrospermopsis raciborskii, isolated from Brazil. Toxicon(1999) 37: 1359-1373.
Letienne, R., et al., Pharmacological characterisation of sodium channels in sinoatrial node pacemaking in the rat heart, Eur J. Pharmacol, Jan. 20, 2006:530(3):243-9.
Llewellyn, Lyndon E., Saxitoxin, a toxic marine natural product that targets a multitude of receptors, Nat. Prod. Rep., 2006, 23, pp. 200-222.
Long, R.R., Sargent, J.C., and Hammer, K. (1990) Paralytic shellfish poisoning: A case report and serial electrophysiologic observations. Neurology 40: 1310-1311.
Maria, Giorgio, MD, Cassetta, Emanuele, MD, Gui, Daniele, MD, Brisinda, Guiseppe, MD, Bentivoglio, Annarita, MD and Albanese, Alberto, MD “A Comparison of Botulinum Toxin and Saline for the Treatment of Chronic Anal Fissure” The New England Journal of Medicine, Jan. 1998, pp. 217-220, vol. 338, No. 4.
Munchau, et al., “Uses of Botulinum Toxin Injection in Medicine Today”, BMJ, vol. 320, pp. 161-165, Jan. 2000.
Nelson, Richard, M.D., A Systematic Review of Medical Therapy for Anal Fissure. Diseases of the Colon and Rectum. 2004, 47, pp. 422-431.
Oshima, Y. Post-Column derivatization HPLC methods for Paralytic Shellfish Poisons. Manual on Harmful Marine Microalgae, IOC of UNESCO Manuals and Guides No. 33. 1995, p. 81-94.
Penzotti, Jennifer L., et al, Neosaxitoxin Interactions with the Na+Channel Outer Vestibule Determined by Mutant Cycle Analysis, Biophysical Journal, vol. 80 Feb. 2001, 698-706.
Pereira, P., Onodera, H., Andrinolo, D., Franca, S., Araujo, F., Lagos, N., Oshima, Y. Paralytic shellfish toxins in the freshwater cyanobacterium Aphanizomenon flosaquae, isolated from Montargil reservoir, Portugal. Toxicom 38: (2000) 1689-1702.
Rataud, Jean, et al, Comparative study of voltage-sensitive sodium channel blockers in focal ischaemia and electric convulsions in rodents, Neuroscience Letters, vol. 172,Issues 1-2, May 19, 1994, pp. 19-23.
Rivas, M., Garcia, C., Liberona, J., Lagos, N. Biochemical characterization and inhibitory effects of dinophysistoxin-1, okadaic acid and microcystine 1-r on protein phosphatase 2a purified from the mussel Myfilus chilensis. Bio Res (2000) 33: 197-206.
Schantz, E.J., et al. Properties and Use of Botulinum Toxin and Other Microbial Neurotoxins in Medicine, Microbiological Review. Mar. 1992, p. 80-99.
Strichartz, O. Structural Determinants of the Affinity of Saxitoxin for Neuronal Sodium Channels. 1984, J Gen. Physiol 84:281-305.
Uribe, J.C., Garcia, C., Rivas, M., & Lagos, N. First Report of Diarrhetic Shellfish Toxins in Magellanic Fjords, Southern Chile. Journal of Shellfish Research. (2001) vol. 20, No. 1, 69-74.
Wheeler, Anthony H., “Therapeutic Uses of Botulinum Toxin”, American Family Physician, vol. 55, No. 2, pp. 541-545, Feb. 1997.
Related Publications (1)
Number Date Country
20140163051 A1 Jun 2014 US
Divisions (1)
Number Date Country
Parent 10294288 Nov 2002 US
Child 11338156 US
Continuations (1)
Number Date Country
Parent 11338156 Jan 2006 US
Child 14043634 US