Use of sulglicotide for the treatment of mucositis

Information

  • Patent Grant
  • 7662777
  • Patent Number
    7,662,777
  • Date Filed
    Thursday, May 12, 2005
    19 years ago
  • Date Issued
    Tuesday, February 16, 2010
    14 years ago
Abstract
A method for the treatment and/or prevention of mucositis due to an antitumour treatment which comprises the administration of a composition containing suiglicotide to a patient in needs of said antitumour treatment.
Description
RELATED APPLICATIONS

This application claims priority to International Application No. PCT/IT2005/000272, filed 12 May 2005 and to Italian Application No. MI2004A000989 filed 18 May 2004, the teachings of which are incorporated herein by reference.


BACKGROUND OF THE INVENTION

Mucositis is a common inflammatory condition affecting the mucous membranes, in particular following chemotherapy or radiotherapy in patients suffering from tumours.


These types of therapy, in addition to acting on neoplastic cells, in fact also act upon the cells of healthy tissue, especially those which replicate rapidly.


As a result, the oral cavity is one of the areas which is highly affected by the complications arising from such treatment; indeed, virtually all patients treated for tumours of the head and neck, and around 40% of those subjected to radio-chemotherapy for tumours in other locations (leukaemias or lymphomas) develop complications affecting the oral cavity (Minerva Stomatol. 2002:51:173-86).


In general, the term “mucositis” is understood to mean a clinical picture characterised by the presence of reduced epithelial thickness, intense erythema and ulcers, associated with a painful symptom complex and the possible occurrence of infection and haemorrhage (Oncologist 1998:3:446-52; Oncologist 1999:11:261-6).


The biological mechanism underlying the development of mucositis, in particular oral mucositis, is subdivided into four phases: an initial inflammatory/vascular phase during which, following radio- or chemotherapy, the epithelial tissues release a large quantity of cytokines such as, for example, interleukin 1 or TNF-α, which cause the first localised tissue damage; a second epithelial phase which affects the division of the epithelial basal cells, resulting in reduced renewal of said cells, atrophy and ulceration of the tissue; a third ulcerative/bacterial phase, which is when the symptoms are at their most intense, with bacterial colonisation of the lesion. This third phase also coincides with severe neutropaenia of the patient; the fourth and final characteristic phase of mucositis is considered to be the healing phase with recovery of proliferation and differentiation of epithelial cells, a progressive increase in white cells and normalisation of the local bacterial flora.


At present, both preventive and curative treatment is provided for mucositis. In the first case, agents are used which are capable of reducing mucous absorption of the chemotherapy drugs (for example cryotherapy, allopurinol or pilocarpine etc.), agents which reduce the changes in epithelial proliferation (for example beta-carotene, glutamine or silver nitrate etc.) or antiinflammatory and antimicrobial agents (for example, mesalazine and/or chlorhexidine).


In particular, with regard to mucositis of the oral cavity, cryotherapy is today the most widely recognised preventive treatment; this method is based on the administration of ice cubes to be kept in the mouth for a period of 30 minutes with the aim of bringing about vasoconstriction of the oral mucosa in order to reduce the temperature-dependent toxicity of some chemotherapeutics. Unfortunately, cryotherapy has proved to exhibit substantial preventive effectiveness only in patients treated with chemotherapeutics which can be administered as a bolus (fluorouracils) but has proved ineffective for continuously perfused chemotherapeutics because the drug is permanently present in the circulating blood and local vasoconstriction locale is of no benefit (Oral Oncology 1999; 35:453-70).


In the second case, use is made of agents which protect the mucosa (for example, sodium bicarbonate), anaesthetic or analgesic agents (for example, lidocaine, morphine and the derivatives thereof etc.), agents which accelerate the healing process (for example, vitamin E, tretinoin, laser therapy etc.) or special diets and/or specific oral hygiene regimens.


Other methods for treating mucositis are described in US patent applications US2003/0064913 and US2003/0236217, which are incorporated herein by reference.


However, none of these preventive strategies or therapeutic approaches has proved entirely effective in the prevention or treatment of mucositis, in particular due to chemotherapy and/or radiotherapy, which remains a cause of suffering in patients suffering from tumours, such as in mucositis of the oral cavity in patients with head and/or neck tumours.


Sulglicotide is a sulfuric polyester of a glycopeptide obtained by extraction from pig duodenum. Sulglicotide is obtained by enzymatic proteolysis, repeated purification and subsequent sulfation steps; the final product is identified by electrophoresis on cellulose acetate.


Sulglicotide is a gastroprotective and antiulcer drug; it is not absorbed intestinally and is known to produce its effects only within the gastric lumen.


Indeed, sulglicotide is usually administered as a gastroprotective to individuals whose stomach wall has been attacked by drugs such as, for example, aspirin and taurocholic acid or by generic nonsteroidal antiinflammatory drugs. Clinical studies have demonstrated the effectiveness of administering sulglicotide to patients suffering from rheumatoid arthritis and receiving treatment with indomethacin and diclofenac, so preventing the occurrence of gastric or duodenal ulceration associated with the use of such nonsteroidal antiinflammatories (Scand. J. Gastroenterol. 1993; October; 28(10):875-8).


The mechanism of action, apart from being linked to pepsin inactivation, is due to the stimulation of the secretion of mucous and bicarbonate by the cells of the gastric mucosa.


In particular, sulglicotide is known to be the drug of choice for the treatment of gastric conditions associated with Helicobacter pylori inflammation.



Helicobacter pylori is a spiral-shaped, gram-negative bacterium which, thanks to its various characteristics, survives in the acidic environment of the gastric mucosa and proliferates under the mucous which coats the internal wall of the stomach, adhering to the cells of the mucosa itself. It is the cause of duodenal ulcers as well as being one of the main causes of chronic gastritis. Current treatments are based on antibiotics and, in the ever more frequent event of antibiotic-resistant strains and relapse, on specific antiulcer drugs.


Indeed, both in animal models and in various clinical studies, the administration of sulglicotide has brought about a considerable antiulcer action in the stomach, with a substantial improvement in the inflammation due to H. pylori (J. Physiol. Pharmacol. 1999 June; 50(2):197-210). Sulglicotide principally acts by inhibiting the effect of the LPS (lipopolysaccharide) produced by the bacterium which prevents somatostatin-receptor binding, causing overproduction of gastrin and acidic secretions which are responsible for the subsequent formation of the ulcer.


SUMMARY OF THE INVENTION

It has now surprisingly been found that using suiglicotide in the treatment of mucositis brings about a considerable improvement with regard to the inflammatory symptom complex and to mucosal damage, with functioning of epithelial cells being significantly restored.


In particular, sulglicotide exhibits its effectiveness in the treatment of mucositis of the oral cavity. More particularly, sulglicotide is active in the treatment of mucositis due to chemotherapy and/or radiotherapy.


Sulglicotide, by increasing levels of both type PGE2 and type PGI2 prostaglandins, brings about increased secretion of mucous and normalised renewal of the epithelial cells of the mucosa. Furthermore, sulglicotide is capable of increasing the secretion of EGF (Epidermal Growth Factor) and so ensuring both the onset of much less severe conditions of the mucosa, and the acceleration of the healing process of such conditions.


The increase in the quantity of EGF, or of the receptor thereof, in fact brings about increased proliferation of the epithelial cells with the formation of a superstratum of said cells and consequent thickening of the mucosa, in particular the oral and/or gastrointestinal mucosa, which is so able to act as a barrier to attack from cytotoxic agents (for example radiation) and significantly reduce any damage.


Growth factors, EGF in particular, are factors which essentially determine the sensitivity of the epithelial cells towards cytotoxic agents.


Thus, the use of sulglicotide in mucositis, in particular mucositis of the oral cavity and used before and/or during chemotherapy and/or radiotherapy in patients suffering from tumours, such as tumours of the head and neck (for example laryngeal, pharyngeal or oesophageal carcinoma), results in a reduction in the damage to the mucosa and lower toxicity of said antitumour treatments, with subsequent resolution of the mucositis associated therewith.


Consequently, according to the present invention, sulglicotide is active in the prevention and treatment of mucositis, in particular oral mucositis due to antitumour treatments such as chemotherapy and/or radiotherapy.





BRIEF DESCRIPTION OF THE DRAWING

FIG. A is an illustration of the morphology of a normal intestinal crypt.


FIG. B is an illustration of the morphology of an intestinal crypt after irradiation with centers of regeneration.


FIG. C is an illustration of the morphology of an intestinal crypt containing fewer than 10 cells.





DETAILED DESCRIPTION OF ONE EMBODIMENT

Animal testing was carried out with the aim of assessing the efficacy of suiglicotide in protecting the clonogenic cells of the intestinal mucosa from radiation-induced damage. Protection of the clonogenic cells ensures the survival of the intestinal crypt which promotes the restoration of the normal epithelium.


The animals treated in the present test are free from H. pylori, or their gastrointestinal mucosa does not exhibit the characteristic signs of inflammation brought about by this bacterium.


In the present test, the inflammatory damage was caused by a 13 Gy X-ray dose. 60 male BDF1 mice, divided into 10 groups each of 6 animals, were treated.


Sulglicotide was administered daily as a preventive measure to 4 groups (plus one control/saline solution group) via a gastric tube and at various doses, namely respectively 12 mg/kg, 50 mg/kg, 200 mg/kg and 800 mg/kg three days before irradiation with a final dose 30 minutes before irradiation.


The other 4 groups (plus one control/saline solution group) received sulglicotide as a treatment, again via a gastric tube and at various doses, namely respectively 12.5 mg/kg, 50 mg/kg, 200 mg/kg and 800 mg/kg immediately after irradiation and thereafter daily for 3 days before sacrifice on the 4th day.


All the animals survived the treatment and no adverse affects were observed. The animals were collected 4 days after irradiation and sacrificed. 10 intestinal circumferences were measured for each animal (60 per group) and the number of surviving crypts and their width was assessed, a mean being calculated for each group. Only intact circumferences and crypts containing 10 or more clonogenic cells were included.


The data obtained are summarised in Table 1 below. The attached Figures show the normal intestinal morphology (Fig. A) or after irradiation with centres of regeneration in which surviving crypts can be seen with only one or more clonogenic cells and the remaining mesenchyme completely lacking (Fig. B). These individuals develop diarrhoea and die from mucositis. Figure C shows an intestinal morphology with phantom crypts or crypts containing fewer than 10 cells.













TABLE 1









Corrected



Mouse
No. crypts/
Crypt
crypts/


Treatment
no.
circumference
length/μm
circumference



















12.5 mg/kg
1
6.8
46.61
4.6


sulglicotide
2
5.4
52.09
3.3


pretreatment
3
14.5
50.40
9.1



4
7.8
47.22
5.2



5
6.7
45.33
4.7



6
5.8
52.08
3.5



Mean
7.8
48.95
5.1


50 mg/kg
1
1.6
45.17
1.1


sulglicotide
2
2.5
54.43
1.5


pretreatment
3
2.5
40.12
2.0



4
6.9
48.67
4.5



5
12
45.76
8.3



6
5.6
51.80
3.4



Mean
5.2
47.68
3.5


200 mg/kg
1
11.3
40.44
8.9


sulglicotide
2
10.5
47.86
7.0


pretreatment
3
11.0
50.46
6.9



4
7.0
49.07
4.5



5
9.0
49.44
5.8



6
9.8
46.99
6.6



Mean
9.8
47.38
6.6


800 mg/kg
1
8.6
44.77
6.1


sulglicotide
2
7.4
47.92
4.9


pretreatment
3
7.3
51.44
4.5



4
10.2
49.36
6.6



5
8.2
51.09
5.1



6
3.1
42.28
2.3



Mean
7.5
47.81
4.9


Control saline
1
10.3
51.12
6.4


pretreatment
2
8.3
46.17
5.7



3
2.8
51.84
1.7



4
4.2
52.28
2.6



5
4.5
45.01
3.2



6
13.1
43.01
9.7



Mean
7.2
48.24
4.9


12.5 mg/kg
1
8.1
43.35
5.9


sulglicotide
2
1.8
49.16
1.2


posttreatment
3
5.5
44.09
4.0



4
2.9
41.04
2.2



5
7.7
51.00
4.8



6
1.5
46.65
1.0



Mean
4.6
45.88
3.2


50 mg/kg
1
9.8
49.70
6.3


sulglicotide
2
7.6
49.32
4.9


posttreatment
3
4.4
53.89
2.6



4
3.7
48.85
2.4



5
5.8
45.86
4.0



6
13.8
48.53
9.0



Mean
7.5
49.36
4.9


200 mg/kg
1
10.4
46.25
7.1


sulglicotide
2
7.3
46.29
5.0


posttreatment
3
8.1
52.88
4.9



4
5.9
45.86
4.1



5
5.7
58.58
3.1



6
4.0
51.00
2.5



Mean
6.9
50.14
4.5


800 mg/kg
1
16.7
42.06
12.6


sulglicotide
2
12.2
48.03
8.1


posttreatment
3
6.6
42.40
4.9



4
5.6
43.95
4.0



5
3.8
45.00
2.7



6
8.3
42.33
6.2



Mean
8.9
43.96
6.4


Control saline
1
8.8
53.52
5.2


posttreatment
2
10.2
49.95
6.5



3
3.4
53.08
2.0



4
11.1
47.30
7.5



5
4.6
49.92
2.9



6
5.3
49.58
3.4



Mean
7.2
50.56
4.6


Control
1
101
34.99



2
97.7
32.15



3
91.4
31.73



4
93.4
28.89



5
96.3
31.78



6
95.4
30.9



Mean
95.7
31.74









Results:


The data collected emphasise the efficacy of sulglicotide on irradiation damage and the association between efficacy and the different dose administered. At the lowest doses (12.5 mg/kg and 50 mg/kg), sulglicotide does not exhibit any preventive effect on the damage to clonogenic cells and the intestinal crypts; evidence of increased survival of the crypts and thus of protection from irradiation damage is found at a dose of 200 mg/kg (35%). A dose of greater than 200 mg/kg also exhibits no protective efficacy. However, while it is effective in preventive terms, the dose of 200 mg/kg exhibits no activity in the post-irradiation treatment groups.


In these cases, only the higher dose of 800 mg/kg has any significant therapeutic effect on the damage caused by the X-rays.


In conclusion, sulglicotide, administered to mice free from Helicobacter pylori via a gastric tube at various doses, proves to be effective in the prevention or treatment of radiation damage.

Claims
  • 1. A method for the treatment and/or reduction of oral mucositis due to an antitumor treatment which comprises the administration of a composition consisting essentially of sulglicotide to a patient receiving said antitumour treatment.
  • 2. A method according to claim 1 in which the antitumour treatment is chemotherapy and/or radiotherapy.
  • 3. A method according to claim 1 in which the sulglicotide is administered in a quantity of from 12.5 mg/kg to 800 mg/kg.
  • 4. A method according to claim 1 in which said compositions are topical dosage forms.
  • 5. A method according to claim 1 in which said pharmaceutical compositions are oral dosage forms.
  • 6. A method according to claim 1 in which said compositions are parenteral dosage forms.
Priority Claims (1)
Number Date Country Kind
MI2004A0989 May 2004 IT national
PCT Information
Filing Document Filing Date Country Kind 371c Date
PCT/IT2005/000272 5/12/2005 WO 00 11/14/2006
Publishing Document Publishing Date Country Kind
WO2005/110458 11/24/2005 WO A
US Referenced Citations (5)
Number Name Date Kind
5085867 Farolfi et al. Feb 1992 A
5496828 Cullinan et al. Mar 1996 A
6274601 Cullinan Aug 2001 B1
20030064913 Sonis Apr 2003 A1
20030236217 Shalwitz et al. Dec 2003 A1
Foreign Referenced Citations (2)
Number Date Country
0 274 745 Jul 1988 EP
WO 9218153 Oct 1992 WO
Related Publications (1)
Number Date Country
20080234180 A1 Sep 2008 US