[go: up one dir, main page]

HK1085931A - Use of acetyl-d-aminoglycosamine in treatment of local lesions and systematic symptoms related to infections of virus or bacteria - Google Patents

Use of acetyl-d-aminoglycosamine in treatment of local lesions and systematic symptoms related to infections of virus or bacteria Download PDF

Info

Publication number
HK1085931A
HK1085931A HK06106070.4A HK06106070A HK1085931A HK 1085931 A HK1085931 A HK 1085931A HK 06106070 A HK06106070 A HK 06106070A HK 1085931 A HK1085931 A HK 1085931A
Authority
HK
Hong Kong
Prior art keywords
acetyl
virus
bacteria
infections
glucosamine
Prior art date
Application number
HK06106070.4A
Other languages
Chinese (zh)
Inventor
Qiwang Xu
Junkang Liu
Zetao Yuan
Original Assignee
中国人民解放军第三军医大学
苏州市巴微医药开发研究所有限公司
北京中港大富生物波科技有限公司
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by 中国人民解放军第三军医大学, 苏州市巴微医药开发研究所有限公司, 北京中港大富生物波科技有限公司 filed Critical 中国人民解放军第三军医大学
Publication of HK1085931A publication Critical patent/HK1085931A/en

Links

Description

Technical field
The present invention relates to the use of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof in the treatment of local lesions and/or systematic symptoms caused by infections of virus and/or bacteria, and the use of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof in the manufacture of a medicament for the treatment of local lesions and/or systematic symptoms caused by infections of virus and/or bacteria.
Background Art
The systematic toxic symptoms caused by infections of virus and/or bacteria include systematic toxic symptoms caused by endotoxemia and local ectotoxic lesions, such as fever, headache, vertigo, delirium, nausea, emesis, general malaise, etc. At present, there are two main methods for treatment of systematic symptoms caused by infections of bacteria: 1) antibacterial therapy, and 2) supporting therapy.
Viral infections are commonly caused but not limited by Coxsackie virus, ECHO virus, orthomyxovirus, paramyxovirus, adenovirus, coronaviruses, reovirus, respiratory syncytial virus, rhinovirus, hepatitis A virus, hepatitis B virus, hepatitis C virus, and encephalitis B virus, which result in systematic symptoms such as fever, etc. accompanying by local mucosal lesions. The most usual symptoms are inflammations, including tracheitis, bronchitis, mucous hyperemia, and exhibit cough and asthma. At present, there is no means or drug to effectively control viral infections, except for some supporting therapies.
In the research of "bio-wave" theory, the present inventor has set up a organism wave-growth model. Through deeply researching the molecular mechanism of the organism wave-growth, the inventor puts forward a micro-heterology variation mechanism, wherein the biological wave of organism continuously changes; the change rate depends on the change extent of outer environments; after the organism is infected by bacteria and viruses, the environments in the organism changes quickly, which promotes the generation of micro-heterology and the non-equilibrium between the organism and environments, and causes local lesions and systematic toxic symptoms. According to molecular biological analysis, these lesions and toxic symptoms relate to the instability even loss of function of proteins, especially various enzymes under changed conditions, especially changed temperature in the presence of microorganism metabolism products. The systematic toxic symptoms mainly appear in nerve system, including headache, delirium, hypersomnia, coma, general malaise, muscular soreness, nausea, emesis, blurred vision, diplopia, respiration disorder (first tachypnea then bradypnea), arrhythmia, urinary and fecal incontinence, even torpidity or loss of reflex, local congestion, edema, blood clot and tissue necrosis.
It is found that N-acetyl-D-glucosamine as a regulating factor of biological wave affects not only the macro fluctuation, but also the stability of vibration of bio-macromolecular substances. This substance can maintain the physiological vibration of bio-macromolecular substances, alleviate and repulse harmful effects in organism, in order to maintain the physiological function of macromolecular substances. In general, said substance can control symptoms, alleviate lesions, promote heal, and eliminate toxic effects.
The inventor surprisingly finds that N-acetyl-D-glucosamine or pharmaceutically acceptable salts in combination with various pharmaceutically acceptable carriers can form a liquid dose form for treatment of local lesions or systematic toxic symptoms caused by infections of virus or bacteria.
Contents of the invention
One object of the present invention is to provide a use of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof in the treatment and control of local lesions and systematic symptoms caused by infections of virus or bacteria.
Another object of the present invention is to provide a use of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof in the manufacture of a medicament for the treatment and control of local lesions and systematic symptoms caused by infections of virus or bacteria.
Another object of the present invention is to provide a method for treating local lesions and systematic symptoms caused by infections of virus or bacteria.
The N-acetyl-D-glucosamine used in the present invention is a compound having a molecular formula of C8H15NO6 and a structure formula (I).
The examples of pharmaceutical acceptable salts of N-acetyl-D-glucosamine that can be used in the present invention include, but are not limited to: the salts formed with inorganic acids, such as hydrochloride, hydrobromide, borate, phosphate, sulfate, hydrosulfate and hydrophosphate, and the salts formed with organic acids, such as citrate, benzoate, ascorbate, methylsulfate, picrate, fumarate, maleate, malonate, succinate, tartrate, mesylate, and glucose-1-phosphate.
In a pharmaceutical composition of the present invention, the content of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof is generally 0.1-10% by weight.
Besides N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof, said pharmaceutical composition further comprises excipients or carriers well known in the art to form a preparation suitable for intravenous injection, subcutaneous injection, intramuscular injection, intraperitoneal injection, etc.
Said pharmaceutical composition can be administered in a manner of single dose per day or multidoses per day, such as 3-4 doses per day. The dose of said pharmaceutical composition depends on patient's age, condition, symptom, and administration manner. In general, as to an adult patient having a bodyweight of 75 kg, the dose of said pharmaceutical composition is 1-100000 mg per day, preferably 100-10000 mg per day based on active component, and is administered one to four times daily.
According to a preferable model, N-acetyl-D-glucosamine is administered in a manner of intervenous drop infusion during the therapeutical procedure in order to potentiate power of resistance, to replenish water, and to maintain stability in vivo.
As compared to conventional supporting therapy, N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof are more effective in reducing local inflammations and alleviating local lesions and systematic toxic symptoms, act quickly and roundly, and facilitate better prognostic results.
Although the inventor does not intend to be restricted by any theory, it is believed that N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof can stabilize important molecules of organism and maintain the physiological function of bio-macromolecules, thereby avoiding some complications after infections of virus or bacteria and expediting the healing. Thus, N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof are desired drug for supporting therapy.
Embodiments for carrying out the invention
The present invention and beneficial effects thereof are further demonstrated by the following examples, but it shall be understood that these examples are merely to illustrate the present invention, rather than to restrict the scope of the present invention in any aspect.
Example 1. Promoting wave test of the compound of formula (I) 1. Experimental materials and method: 1.1 Sample: pure compound of formula (I) 1.2 Experimental materials:
  • Strain: Proteus Mirabilis that meets the following biochemical reaction characteristics: dynamics (+), urease (+), lactose (-), glucose (+), H2S (-),phenylalanine deaminase (+).
  • Culture medium: modified LB culture medium (components: 1% tryptones, 0.5% yeast extract, 1% sodium chloride, 0.1 % glucose, 0.002% TTC, and pH = 7.2 to 7.4).
1.3 Experimental method:
  • Control sample: the Proteus Mirabilis were inoculated at the center of LB plate, incubating at 37°C for 9 hours;
  • Test sample: the compound of formula (I) with a final concentration of 0.5% was added to the LB plate, then the Proteus Mirabilis were inoculated by the same method, and cultured at 37°C for 9 hours.
2. Experimental results and evaluation:
The control sample exhibited concentric rings with an interval of 3 hours, which extended outward continually. The test sample showed not only concentric rings with an interval of 3 hours, but also many fine waves on each ring in comparison with the control sample.
The experiment adopts a bio-wave model to research the promoting wave function of the compound of formula (I). The results showed that the compound of formula (I) was not only able to cause bacterial cell to reveal a normal bio-wave characteristic, but also cause the wave reveal finer wave mode. These indicated that the compound of formula (I) has a function of promoting bio-waves. This wave-promoting function may explain the effects of using N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof for treating and controlling local lesions and systematic symptoms caused by infections of virus or bacteria.
Example 2. Toxicological test of the compound of formula (I)
The toxicological test of the compound of formula (I) includes:
  • 1. Acute toxicity test: including tests of oral administration, intravenous injection administration, and maximum limit amount for administration;
  • 2. Ames test;
  • 3. Micronucleus test of mouse bone marrow cell;
  • 4. Abnormality test of mouse sperm;
  • 5. Aberration test of mouse testis chromosome;
  • 6. Chronic lethal test;
  • 7. Sub-chronic toxicity (feed for 90 days) test;
  • 8. Traditional deformity-inducing test.
The results of these tests showed that in the acute toxicity test of the compound of formula (I), the acute toxicosis reaction had not appeared when the dosage more than 2 g/kg was taken; in the long-period toxicity test, the maximum dosage had reached up to 1 g/kg, and after the treatment and observation for four weeks, there was no intoxication reaction yet; and in the reproduction test, the mice were feed with a routine dosage of 7 mg/kg for 3 generations, it had been proved that the compound of formula (I) had no influence on the pregnancy, birth, nurse and the growth of baby mouse, so that the compound of formula (I) is a substance without toxicity.
Example 3. Cytological tests of regulating micro-heterology variation
Conventional incomplete 1640 culture media were used for cell culture, and B16 tumor cells (commercially obtained from the tumor cell library of Shanghai Institute of Cytobiology) were inoculated on said media. After being continuously cultured for more than 48 hours, the micro-heterology variation of cells and the control effects of N-acetyl-D-glucosamine thereon were observed under a condition where metabolic wastes affected the growth environment. After N-acetyl-D-glucosamine having a final concentration of 1 g/100ml was added to the culture media, the cell number stably increased with the culture time during the cell growth procedure. The control cells cultured without N-acetyl-D-glucosamine could not proliferate on the same culture media under same conditions. These tests indicated that in the presence of the compound of formula (1), cells could regulate the cell micro-heterology variation in order to adapt to the ever-changing environment, so that cells could proliferate continuously.
Example 4. Animal tests that N-acetyl-D-glucosamine regulates micro-heterology variation
B16 tumor cells were inoculated on superior parts of hind legs of 50 rats, and 5% aqueous solution of the compound of formula (1) was intraperitoneally injected to the rats for consecutive 7 days, 3 times per day, and 1 ml every time. Finally, solid tumor did not appear in 45 rats. In control group without the administration of the compound of formula (1), many proliferative corpuscles appeared in at least 40 among 50 rats within 1-3 days after the tumor cells were inoculated; many immature cells appeared within 3-5 days; and visible solid tumors finally appeared within about 10 days. As compared to the control group, this did not appear in the test group, which indicated that the compound of formula (1) could control the micro-heterology variation.
Example 5. Animal tests of controlling local lesions and systemic symptoms caused by infection of microorganism
10 rabbits were used in tests. The rabbits were administered with a culture of Gram-negative bacteria (Pseudomonas aeruginosa, serotype 8, wherein the bacterial number in the culture is about 3 x 1011) in a dose of 10 ml per day for consecutive 3 days. The rabbits exhibited serious toxic symptoms, such as fever, increased heart rate, tachypnea, hyperposia, bodyweight drop, and after 5 days, the rabbits exhibited watery stool, increased nasal secretion, systematic emaciation and exhaustion. The rabbits were intravenously administered with N-acetyl-D-glucosamine (10% aqueous solution) a dose of 2 ml every time, 3 times per day, for consecutive 3 days. The rabbits were gradually healed after one week, they began to eat, their symptoms were alleviated, their body temperatures dropped, and their defecation formed. After examination of nasal mucosa and respiratory tract of the rabbits, the inflammations were alleviated, and their secretion products were normal. In the test group, all 10 rabbits survived, while in the control group, 8/10 rabbits of the control group died within one week, and only 2 rabbits survived.
When N-acetyl-D-glucosamine was replaced with N-acetyl-D-glucosamine hydrochloride in the tests (other conditions were not changed), 7/10 rabbits of test group survived. The test group was significantly different from the control group.

Claims (7)

  1. A use of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof in the manufacture of a medicament for controlling local lesions and systematic symptoms caused by infections of virus or bacteria.
  2. A use according to claim 1, wherein said medicament is a preparation suitable for intravenous injection, subcutaneous injection, intramuscular injection, or intra-peritoneal administration.
  3. A use according to 1 or 2, wherein the dose of said medicament for an adult patient is 1-100000 mg per day based on the active component, and said medicament is administered 1-4 times daily.
  4. A method for controlling local lesions and systematic symptoms caused by infections of virus or bacteria, wherein a pharmaceutical composition comprising an effective amount of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof is administered to a patient.
  5. A method according to claim 4, wherein said pharmaceutical composition is a preparation suitable for intravenous injection, subcutaneous injection, intramuscular injection, or intra-peritoneal administration.
  6. A method according to 4 or 5, wherein the dose of said pharmaceutical composition for an adult patient is 1-100000 mg per day based on the active component.
  7. A use of N-acetyl-D-glucosamine or pharmaceutically acceptable salts thereof in controlling local lesions and systematic symptoms caused by infections of virus or bacteria.
HK06106070.4A 2003-03-27 2004-03-29 Use of acetyl-d-aminoglycosamine in treatment of local lesions and systematic symptoms related to infections of virus or bacteria HK1085931A (en)

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
CN03108280 2003-03-27

Publications (1)

Publication Number Publication Date
HK1085931A true HK1085931A (en) 2006-09-08

Family

ID=

Similar Documents

Publication Publication Date Title
CN102697784B (en) Enrofloxacin injection for livestock and preparation method thereof
US20070042995A1 (en) Use of acetyl-d-aminoglycosamine in treatment of local lesions and systematic symptoms related to infections of virus or bacteria
CN118562686B (en) A strain of Bifidobacterium bifidum for sobering up, protecting liver and reducing uric acid, and its postbiotics, composition and application
CN117530922B (en) High-stability compound injection for livestock and preparation method and application thereof
CN116077528B (en) Application of gallic acid carbon dots in resisting pseudorabies virus
CN115192593B (en) Application of daunorubicin in treating multi-drug resistant bacteria infection diseases
CN111440195B (en) Cefuroxime magnesium compound, composition, preparation method and application
HK1085931A (en) Use of acetyl-d-aminoglycosamine in treatment of local lesions and systematic symptoms related to infections of virus or bacteria
CN101829129B (en) Veterinary compound gentamycin sulfate injection and preparation method thereof
US20070207198A1 (en) Use Of N-Acety1-D-Glucosamine In The Manufacture Of Medicaments For Anti-Tumors And Anti-Metastasis
CN112438975B (en) Application of diabetes treatment medicine in bacteriostasis
EP1371371B1 (en) The use of n-acetyl-d-glucosamine in the manufacture of pharmaceutical useful for preventing and treating sexual disorder
US7704976B2 (en) Use of N-acetyl-D-glucosamine for preparing medicines for urogenital tract infection's treatment and prevention
US20070178161A1 (en) Use of n-acetryl-d-glucosamine in treating and controlling non-specific inflammations caused by physical or chemical factors
CN118021802B (en) Application of compound 0683-0042 as an NDM-1 inhibitor in antibacterial applications
CN119410593B (en) A Riemerella anatipestifer bacteriophage and its application
EP1611896A1 (en) Use of n-acetyl-d-aminoglycosamine in treatment of local lesions or systematic symptoms related to autoimmune reactions
CN118021828B (en) Use of compound 0449-0141 as NDM-1 inhibitor in antibacterial
HK1083591A (en) Use of n-acetyl-d-aminoglycosamine in treatment of local lesions or systematic symptoms related to autoimmune reactions
CN120437127A (en) Application of jatrorrhizine in the preparation of medicine for preventing and treating Mycoplasma hyopneumoniae infection
CN119345215A (en) A combined drug composition for resisting MRSA infection and its application
US7345030B2 (en) Use of n-acetyl-d-aminoglycosamine in treatment of organ lesions related to toxicosis of drugs or chemicals
CN113637025A (en) A kind of cefotaxime magnesium compound, its preparation method and application
CN120459117A (en) Cryptotanshinone derivative and fosfomycin combined antibacterial drug as well as preparation method and application thereof
US20050119224A1 (en) Use of n-acetyl-d-glucosamine in the manufacture of pharmaceutical useful for adjuvant treatment of perianal disease