RU2786314C1 - A method for predicting the risk of developing peptic ulcer disease in women based on genetic data - Google Patents

Abstract

FIELD: health care.

SUBSTANCE: invention relates to health care, namely to medical diagnostics, and can be used to predict the risk of peptic ulcer in unrelated Russian women according to genetic data, natives of the Central Black Earth region of the Russian Federation. Venous blood sampling, DNA isolation, analysis of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMR-9 gene are carried out. When the AAGG haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMR-9 gene is detected, a low risk of developing peptic ulcer disease in women is predicted.

EFFECT: method disclosed in the present invention provides new criteria for assessing the risk of peptic ulcer disease in women of Russian nationality, natives of the Central Black Earth region of the Russian Federation, based on data on polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the gene MMR-9.

1 cl, 4 dwg, 4 ex

Description

The invention relates to the field of medical diagnostics and is intended to predict the risk of developing peptic ulcer in women.

Peptic ulcer of the stomach and duodenum (PUD and duodenum) is a chronic polyetiological relapsing disease, the development of which involves systemic hypothalamic-pituitary, hypothalamic-pituitary-adrenal and local gastroduodenal processes, leading to trophic disorders in the mucous membrane of the stomach and duodenum. intestines, as a result of which a peptic ulcer is formed (Clinical and genetic features of duodenal ulcer / L. V. Volevach, A. S. Sarsenbayeva, L. V. Gabbasova [et al.] // Experimental and Clinical Gastroenterology. - 2019. - No. 9. - S. 45-49).

Peptic ulcer of the stomach and duodenum is one of the most common multifactorial human diseases, it affects up to 10% of the inhabitants of Europe and the USA (Schubert, M. L. Stomach and duodenum / M. L. Schubert // Curr. Opin. Gastroenterol. - 2016. - Vol. 32 , No. 6. - P. 450-451).

PUD and duodenal ulcer is one of the causes of disability in gastroenterological patients (PUD and duodenal ulcer accounts for about 40% of all cases of disability in patients of this group, which causes significant economic losses (Peptic ulcer: etiology, pathogenesis, clinic / S.N. Styazhkina, A. S. Andreeva, M. A. Volozhanina, S. R. Raimova // Modern Science. - 2020. - No. 10-2. - P. 310-313).

In the structure of the causes of disability among men with gastroenterological diseases, the share of GU and duodenum is maximum and amounts to 68.4% (Management of epithelial precancerous conditions and lesions in the stomach (MAPS II): European Society of Gastrointestinal Endoscopy (ESGE), European Helicobacter and Microbiota Study Group (EHMSG), European Society of Pathology (ESP), and Sociedade Portuguesa de Endoscopia Digestiva (SPED) guideline update 2019 / P. Pimentel-Nunes, D. Libânio, R. Marcos-Pinto [et al.] // Endoscopy - 2019. - Vol. 51, No. 4. - P. 365-388). At the same time, the financial losses from GU and duodenum are comparable to the economic damage from diseases of the vascular system.

A variety of pathogenetic mechanisms, both systemic and local, are involved in the development and progression of PU and duodenal ulcer (Rational use of non-steroidal anti-inflammatory drugs: clinical guidelines / A. E. Karateev, E. L. Nasonov, V. T. Ivashkin [et al.] // Scientific and Practical Rheumatology - 2018. - V. 56, No. 1, appendix 1. - P. 1-29).

The pathophysiology of gastric ulcer and duodenal ulcer is based on an imbalance between the factors of damage to the mucous membrane (impaired motor-evacuation function of the stomach, exposure to hydrochloric acid and pepsin, duodenogastric reflux) and mucoprotective protective factors (muco-bicarbonate barrier, adequate blood flow, epithelial regeneration, prostaglandins) (Fischbach , W. Helicobacter Pylori infection: when to eradicate, how to diagnose and treat / W. Fischbach, P. Malfertheiner // Dtsch Ärztebl Int. - 2018. - Vol. 115, No. 25. - P. 429-436) .

PUD and duodenal ulcer is a multifactorial disease, the development of which involves exogenous (nutrition, stress, bad habits and lifestyle, intake of non-steroidal anti-inflammatory drugs (NSAIDs), H. pylori infection, etc.) and endogenous (gender, age, ethnicity and other) risk factors (Lanas-Gimeno, A. Risk of gastrointestinal bleeding during anticoagulant treatment / A. Lanas-Gimeno, A. Lanas // Expert Opin. Drug Saf. - 2017. - Vol. 16, No. 6. - P 673-685).

Genetic factors play a significant role in the formation of the disease: hereditary burden in patients with gastric ulcer and duodenal ulcer is detected in 5.5 - 50% (Kolotilova, M. L. Neurogenic and genetic factors of the etiology and pathogenesis of peptic ulcer / M. L. Kolotilova, L. N Ivanov // Experimental and Clinical Gastroenterology - 2017. - No. 12. - P. 89-97).

According to the literature, matrix metalloproteinases (MMPs) play an important role in the etiopathogenesis of PU and duodenum. This family of extracellular zinc-dependent endopeptidases plays a key role in the breakdown of the components of the extracellular matrix, basement membranes and a number of cell surface proteins (Molecular genetic aspects of peptic ulcer / E. Kh. Shaimardanova, A. Kh. Nurgaliyeva, D. D. Nadyrshina, E. K. Khusnutdinova // Medical genetics. - 2014. - V. 13, No. 11. - P. 3-14). These medical and biological effects of matrix metalloproteinases, as evidenced by the literature, are important in the pathogenesis of PU and duodenum (Fields, G. B. The Rebirth of Matrix Metalloproteinase Inhibitors: Moving Beyond the Dogma / G. B. Fields. - DOI: 10.3390/cells8090984 // Cells. - 2019. - Vol. 8, No. 9. - 984. - URL: https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6769477/pdf/cells-08-00984.pdf (date of the application 05/02/2021)).

Foreign and domestic scientists are conducting research to search for associations of polymorphism of candidate genes with the formation of GU and duodenum, as a result of which a connection with the development of the disease of polymorphic loci of cytokine genes and their receptors, digestive enzymes, heat shock proteins, vascular endothelial growth factors, myeloperoxidases, cyclooxygenase -1, macrophage migration inhibition factor, etc. (Circulating concentration of interleukin-37 in Helicobacter pylori-infected patients with peptic ulcer: Its association with IL-37 related gene polymorphisms and bacterial virulence factor CagA / E. Davarpanah, A. Jafarzadeh, M. Nemati [et al.] - DOI: 10.1016/j.cyto.2019.154928 // Cytokine. - 2020. - Vol. 126. - Art. 154928. - URL: https://www.sciencedirect.com/ science/article/abs/pii/S1043466619303576?via%3Dihub (date of the application 05/12/2021)).

In some studies, associations with the development of GU and DPC of polymorphism of matrix metalloproteinase genes have been shown. However, it should be noted that the vast majority of these studies were carried out by foreign scientists, while in the Russian Federation such studies are rare. Also, it should be noted that the results obtained in different populations often differ from each other, which may be due to both the etiopathogenetic features of the occurrence and course of PU and duodenal ulcer in individuals from different ethnoterritorial population groups, and different research designs.

One of the important tasks of modern gastroenterology is to study the causes and mechanisms of peptic ulcer development in women, among which genetic factors play a significant role.

In the Russian Federation, studies of the involvement of the MMP-9 gene in the formation of predisposition to PU in women are rare, and there are no data on the role of genetic variants of the rs17576-rs3787268-rs2250889-rs17577 gene in the development of PU.

To assess the current patent situation, a search was performed on titles of protection for the period from 1990 to 2021. The analysis of documents was carried out in the direction: a method for predicting the risk of peptic ulcer in women based on molecular genetic data, depending on the polymorphic markers of the MMP-9 gene. Sources of information: sites of the Federal Institute of Industrial Property http://fips.ru.

In the studied scientific medical and available patent literature, the authors did not find a way to predict the risk of developing PU in women based on data on the polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene.

A known method for predicting the risk of developing peptic ulcer (patent RU No. 2231794, published 06/27/2004), including studies of gastric samples, based on measuring the diffusion rate of hydrogen ions through the layer of mucus covering the gastric mucosa, by introducing a test 0.1 H solution into the stomach hydrochloric acid and studies of the dynamics of the penetration of hydrogen ions into the mucous membrane by evacuating the contents of the stomach, thereby determining the risk of developing peptic ulcer. in addition, the role of genetic polymorphisms is not taken into account.

A known method for predicting the development of gastric ulcer and duodenal ulcer (patent RU No. 2281037, published 10.08.2006). The essence of the method consists in determining the patient's calendar age, biological age, the ratio of biological and calendar ages, height, body weight, and quality of life indicators. Then the probability of developing a peptic ulcer is calculated using the formula:

where e is the exponent, the number of bases of the natural logarithm, equal to - 2.71, D1 is the sum of the indicators multiplied by the coefficient B of the discriminant functions for patients, D2 is the sum of the indicators multiplied by the coefficient A of the discriminant functions for healthy people, while the values of the coefficients A and B is selected from the table "Coefficients of discriminant functions" and at P1>P2, the risk of developing gastric ulcer and duodenal ulcer is predicted. The disadvantage of this method is that it does not take into account the role of genetic polymorphisms and gender specificity.

A known method for assessing the risk of developing duodenal ulcer in Khakass based on genetic analysis (patent RU No. 2563828, published on September 20, 2015), which is characterized by the fact that risk factors are established - interleukin IL-8 polymorphism is determined by restriction analysis when DNA is isolated from lymphocytes venous blood, and also determine the genotype of Helicobacter pylori by PCR when extracting DNA from biopsy specimens of the gastric mucosa in patients belonging to the indigenous inhabitants of the Republic of Khakassia. Risk factors are assigned numerical values and then predictive coefficients PI, P2 are determined. At P1>P2, a low risk is predicted, and at P1<P2, a high risk of developing peptic ulcer is predicted. The disadvantage of this method is the complexity of the calculation and is applicable only to the indigenous inhabitants of the Republic of Khakassia.

A known method and device for predicting the risk of developing peptic ulcer {patent RU No. 2318217, published 27.02.2008). The essence of the method lies in the fact that the diffusion (liquid) or membrane potential between the gastric juice and the test fluid is measured by the electrochemical method, and if the potential value is more than the threshold level set for the test fluid, the risk of developing peptic ulcer is predicted, water can be used as the test fluid. . In this case, the threshold level is 10 mV. simultaneously with the measurement of diffusion or membrane potential, the pH of gastric juice can be measured, while the risk of developing peptic ulcer is predicted when the diffusion or membrane potential is more than the threshold level set for the test fluid and pH is less than 1.5. The device for implementing the method in the study of gastric juice in vitro consists of two containers separated by a diaphragm: with gastric juice and test fluid. They omit the reference electrodes, the voltage between which is equal to the diffusion potential, the device for the study of gastric juice in vivo contains a chamber with a test liquid, through the diaphragm, in contact with gastric juice, and two reference electrodes, one of which is in contact with gastric juice, and the other - with test fluid. The voltage between the electrodes is equal to the diffusion potential. using the method allows timely start of prophylactic treatment of gastric ulcer and duodenal ulcer. The disadvantage of this method is its complexity, it does not take into account the role of genetic polymorphisms and gender.

The objective of this study is to expand the arsenal of diagnostic methods, namely, to create a method for predicting the risk of developing PU in women based on data on the rsl7576-rs3787268-rs2250889-rsl7577 polymorphic loci of the MMP-9 gene.

The technical result of using the invention is to obtain criteria for assessing the risk of developing ulcer in women of Russian nationality, a native of the Central Black Earth region of the Russian Federation, based on data on the polymorphic loci rsl7576-rs3787268-rs2250889-rsl7577 of the MMP-9 gene, including:

- venous blood sampling;

- isolation of DNA from peripheral venous blood;

- analysis of polymorphisms rsl7576-rs3787268-rs2250889-rsl7577 of the MMP-9 gene;

predicting a low risk of developing PU in women with the detection of the AAGG haplotype of polymorphic loci rsl7576-rs3787268-rs2250889-rsl7577 of the MMP-9 gene.

The novelty and inventive step lies in the fact that the possibility of predicting the development of ulcer in women based on data on the AAGG haplotype of polymorphic loci rsl7576-rs3787268-rs2250889-rsl7577 of the MMP-9 gene is not known from the prior art.

The method is carried out as follows:

Isolation of genomic DNA from peripheral blood is carried out by phenol-chloroform extraction (Miller, SA A simple salting out procedure for extracting DNA from human nucleated cells / SA Miller, DD Dykes, HF Polesky // Nucleic. Acids. Res. - 1988. - Vol 16, No. 3. - P. 1215) in two stages. At the first stage, 25 ml of lysis buffer containing 320 mM sucrose, 1% Triton X-100, 5 mM MgCl ₂ , 10 mM Tris-HCl (pH=7.6) is added to 4 ml of blood with EDTA. The resulting mixture is stirred and centrifuged at 4°C, 4000 rpm. within 20 minutes. After centrifugation, the supernatant is drained, 4 ml of a solution containing 25 mM EDTA (pH=8.0) and 75 mM NaCl is added to the sediment, and resuspended. Then add 0.4 ml of 10% SDS, 35 µl of proteinase K (10 mg/ml) and incubate the sample at 37°C for 16 hours.

At the second stage, DNA is sequentially extracted from the obtained lysate with equal volumes of phenol, phenol-chloroform (1:1) and chloroform with centrifugation at 4000 rpm. within 10 minutes. After each centrifugation produce the selection of the aqueous phase. DNA is precipitated from solution with two volumes of chilled 96% ethanol. After lyophilization, the resulting DNA is dissolved in bidistilled, deionized water and stored at -20°C.

Polymorphic markers rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene were analyzed by polymerase chain reaction (PCR) on a CFX-96 Real-Time System (Bio-Rad) thermal cycler using standard oligonucleotide primers and probes (synthesized at Test- Gen" (Ulyanovsk)).

Amplification of genomic DNA was carried out in a reaction mixture with a total volume of 10 µl, including a mixture for PCR MMP-9 - 4 µl, Taq polymerase - 2 µl, test sample (~30 ng DNA/µl) - 1 µl, deionized water - 3 µl.

Genotyping of the studied samples was carried out using the software "CFX-Manager ™" by the method of discrimination of alleles by the values of relative fluorescence units (RFU) (Fig. 1, Fig. 2, Fig. 3, Fig. 4)

The invention is characterized by figures:

- AA,

- GG,

- AG, ■ - отриц. контр.)Figure 1 - Allele discrimination by detection of TaqMan probes according to RFU values (relative fluorescence units) of each probe on a CFX96 amplifier with a real-time detection system for the rs17576 MMP-9 polymorphism (

-AA,

- GG,

- AG, ■ - negative. counter.)

- AA,

- GG,

- GA, ■ - отриц. контр.)Figure 2 - Allele discrimination by detection of TaqMan probes according to the RFU values (relative fluorescence units) of each probe on a CFX96 amplifier with a real-time detection system for the rs3787268 MMP-9 polymorphism (

-AA,

- GG,

- GA, ■ - negative. counter.)

- CC,

- GG,

-CG, ■ - отриц. контр.)Figure 3 - Allele discrimination by detection of TaqMan probes according to RFU values (relative fluorescence units) of each probe on a CFX96 amplifier with a real-time detection system for the rs2250889 MMP-9 polymorphism (

- CC,

- GG,

-CG, ■ - negative. counter.)

- AA,

- GG,

- GA, ■ - отриц. контр.)Figure 4 - Allele discrimination by detection of TaqMan probes according to the RFU values (relative fluorescence units) of each probe on a CFX96 amplifier with a real-time detection system for the rs17577 MMP-9 polymorphism (

-AA,

- GG,

- GA, ■ - negative. counter.)

Determination of haplotype frequencies and analysis of associations of haplotypes with the development of PU in women were carried out using logistic regression analysis in the PLINK v. 2.050 (http://zzz.bwh.harvard.edu/plink/). When necessary, covariates (age, sex, body mass index) were included in the study. After the permutation test (1000 permutations were performed), p _perm <0.05 was taken as a statistically significant level.

The possibility of using the proposed method to assess the risk of developing ulcer in women is confirmed by the analysis of the results of observations of 441 patients, including 211 patients with peptic ulcer and 230 individuals in the control group. Among patients, the average age is 48.86±13.13, in the control group the average age is 48.47±13.69 years. The samples for the study included (inclusion criteria): 1) women of Russian nationality, born in the Central Black Earth region of Russia and living in the Belgorod region (Churnosov M.I., Sorokina I.N., Balanovskaya E.V. Gene pool of the population of the Belgorod region. Dynamics endogamy index in regional populations // Genetika, 2008, vol. 44, no. 2) the group of patients included patients with peptic ulcer, after establishing the diagnosis of the disease, confirmed using clinical, clinical-instrumental and clinical-laboratory research methods. The diagnosis of peptic ulcer was established on the basis of: anamnestic data (characteristic complaints, anamnesis of the disease was collected), physical examination (detection of soreness and resistance of the muscles of the abdominal wall during palpation), instrumental examination (detection of a peptic ulcer during endoscopic examination of the stomach and duodenum). (Clinical guidelines, 2019). Examination of patients with ulcer was carried out on the basis of the gastroenterological department of the Belgorod Regional Clinical Hospital of St. Joasaph; 3) the control group included patients who did not have clinical and endoscopic signs of PU. The control group was formed during preventive examinations (examination) of the population, conducted in the Belgorod Regional Clinical Hospital of St. Joasaph.

All studies were carried out under the supervision of the ethics committee of the St.

Typing of molecular genetic markers was carried out at the Department of Medical and Biological Disciplines of the Medical Institute of the National Research University "BelSU".

When calculating the frequencies of haplotypes and analyzing their associations in individuals, a relationship was established with the formation of PU in women of the AAGG haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene. The AAGG haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene is a protective risk factor for the development of PU in female patients (OR=0.12 p _perm =0.031).

As examples of the specific application of the developed method, a survey of Russian women, a native of the Central Black Earth region of the Russian Federation and who are not relatives to each other, is given: a genetic study was carried out at the rs17576-rs3787268-rs2250889-rs17577 loci of the MMP-9 gene.

Venous blood was taken from patient A., during the genotyping of DNA markers, the AAGG haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene was detected, which made it possible to include the patient in a group of women with a low risk of developing PU. Upon further observation, the diagnosis of peptic ulcer in patient A. was not confirmed.

Venous blood was taken from patient O., during the genotyping of DNA markers, the AACA haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene was detected, which made it possible to include the patient in the group of patients with an increased risk of developing PU. Further follow-up confirmed the diagnosis of peptic ulcer in patient O.

Venous blood was taken from the patient S., during the genotyping of DNA markers, the AACG haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene was detected, which made it possible to include the patient in the group of patients with an increased risk of developing PU. Further follow-up confirmed the diagnosis of peptic ulcer in the patient.

Venous blood was taken from patient I., during the genotyping of DNA markers, the GGCG haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene was detected, which made it possible to include the patient in the group of individuals with an increased risk of developing PU. With further observation, the diagnosis of peptic ulcer in patient I. was confirmed.

The use of this method will allow at the preclinical stage to form risk groups among women and timely implement in these groups the necessary therapeutic and prophylactic measures to prevent the development of PU.

Claims (1)

A method for predicting the risk of developing peptic ulcer in unrelated Russian women according to genetic data, a native of the Central Black Earth region of the Russian Federation, including venous blood sampling, DNA extraction from peripheral venous blood, analysis of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene and predicting low the risk of developing peptic ulcer in women with the detection of the AAGG haplotype of polymorphic loci rs17576-rs3787268-rs2250889-rs17577 of the MMP-9 gene.

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