Communications in Computer and Information Science.
Springer Science and Business Media Deutschland GmbH.
Vol. 1748 CCIS.
2023.
P. 29-41
Spectrum of PRSS1, SPINK1, CTRC, CFTR, and CPA1 Gene Variants in Chronic Pancreatitis Patients in Russia
The aim of the study was to define the spectrum of genetic risk factors of chronic pancreatitis (CP) development in patients living in the European part of the Russian Federation. Materials and Methods. The study group included 105 patients with CP, with the age of the disease onset under 40 years old (the average age of onset was 26.9 years). The control group consisted of 76 persons without clinical signs of pancreatitis. The diagnosis of chronic pancreatitis in patients was made on the basis of clinical manifestations and the results of laboratory and instrumental investigations. Genetic examination of patients was conducted using the next-generation sequencing (NGS) technology and included targeted sequencing of all exons and exon-intron boundaries of the PRSS1, SPINK1, CTRC, CFTR, and CPA1 genes. The genotyping of the rs61734659 locus of the PRSS2 gene was also conducted. Results. Genetic risk factors of the CP development were found in 61% of patients. Pathogenic and likely-pathogenic variants associated with the risk of CP development were identified in the following genes: CTRC (37.1% of patients), CFTR (18.1%), SPINK1 (8.6%), PRSS1 (8.6%), and CPA1 (6.7%). The frequent gene variants in Russian patients with CP were as follows: CTRC gene — c.180C>T (rs497078), c.760C>T (rs121909293), c.738_761del24 (rs746224507); cumulative odds ratio (OR) for all risk alleles was 1.848 (95% CI: 1.054–3.243); CFTR gene — c.3485G>T (rs1800120), c.1521_1523delCTT (p.Phe508del, rs113993960), and c.650A>G (rs121909046); OR=2.432 (95% CI: 1.066–5.553). In the SPINK1, PRSS1, and CPA1 genes, pathogenic variants were found only in the group of patients with CP. The frequent variants of the SPINK1 gene include c.101A>G (p.Asn34Ser, rs17107315) and c.194+2T>C (rs148954387); of the PRSS1 gene — c.86A>T (p.Asn29Ile, rs111033566); of the CPA1 gene — c.586-30C>T (rs782335525) and c.696+23_696+24delGG. The OR for the CP development for the c.180TT genotype (rs497078) CTRC according to the recessive model (TT vs. CT+CC) was 7.05 (95% CI: 0.86–263, p=0.011). In the CTRC gene, the variant c.493+49G>C (rs6679763) appeared to be benign, the c.493+51C>A (rs10803384) variant was frequently detected among both the diseased and healthy persons and did not demonstrate a protective effect. The protective factor c.571G>A (p.Gly191Arg, rs61734659) of the PRSS2 gene was detected only in the group of healthy individuals and confirmed its protective role. 12.4% of the patients with CP had risk factors in 2 or 3 genes. Conclusion. Sequencing of the coding regions of the PRSS1, SPINK1, CTRC, CFTR, and CPA1 genes allowed to identify genetic risk factors of the CP development in 61% of cases. Determining the genetic cause of CP helps to predict the disease course, perform preventive measures in the proband’s relatives, and facilitate a personalized treatment of the patient in future. © 2023, Privolzhsky Research Medical University. All rights reserved.
Authors
Litvinova M.M.
,
Khafizov K.F. ,
Speranskaya A.S. ,
Matsvay A.D. ,
Asanov A.Yu. ,
Nikolskaya K.A. ,
Vinokurova L.V. ,
Dubtsova E.A. ,
Ipatova M.G. ,
Mukhina T.F. ,
Karnaushkina M.A. ,
Bordin D.S.
Publisher
Nizhny Novgorod State Medical Academy
Number of issue
2
Language
English
Pages
60-70
Status
Published
Link
Volume
15
Year
2023
Organizations
- 1 I.M. Sechenov First Moscow State Medical University (Sechenov University), 8/2 Malaya Trubetskaya St, Moscow, 119991, Russian Federation
- 2 The Loginov Moscow Clinical Scientific Center of Moscow Healthcare Department, 86 Entuziastov Shosse, Moscow, 111123, Russian Federation
- 3 Central Research Institute of Epidemiology, Russian Federal Service for Surveillance on Consumer Rights Protection and Human Wellbeing, 3A Novogireevskaya St, Moscow, 111123, Russian Federation
- 4 Scientific Research Institute for Systems Biology and Medicine, Russian Federal Service for Surveillance on Consumer Rights Protection and Human Wellbeing, 18 Nauchniy Proezd, Moscow, 117246, Russian Federation
- 5 Lomonosov Moscow State University, 1 Leninskiye Gory, Moscow, 119991, Russian Federation
- 6 Centre for Strategic Planning and Management of Biomedical Health Risks of FMBA of Russia, 10/1 Pogodinskaya St, Moscow, 119121, Russian Federation
- 7 Pirogov Russian National Research Medical University, 1 Ostrovitianova St, Moscow, 117997, Russian Federation
- 8 N.F. Filatov Children’s City Hospital of Moscow Healthcare Department, 15 Sadovaya-Kudrinskaya St, Moscow, 123001, Russian Federation
- 9 Morozovskaya Children’s City Clinical Hospital of Moscow Healthcare Department, 1/9, 4thDobrininskiy Pereulok, Moscow, 119049, Russian Federation
- 10 Peoples’ Friendship University of Russia (RUDN University), 6 Miklukho-Maklaya St, Moscow, 117198, Russian Federation
- 11 A.I. Yevdokimov Moscow State University of Medicine and Dentistry, 20/1 Delegatskaya St, Moscow, 127473, Russian Federation
- 12 Tver State Medical University, 4 Sovetaskaya St, Tver, 170100, Russian Federation
Keywords
CFTR; chronic pancreatitis; CPA1; CTRC; gene variants; genetic risk factors; hereditary pancreatitis; idiopathic pancreatitis; mutations; PRSS1; Russian population; SPINK1
Other records
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Vol. 11.
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P. 243-253