Association of the myosin heavy chain 9 gene single nucleotide polymorphism with inflammatory bowel disease

Background: To date, the cause of inflammatory bowel disease (IBD) remains a mystery. A balance between cell proliferation and apoptosis maintains intestinal tissue homeostasis. Dissociation-induced myosin-actin contraction results in stem cell apoptosis. This study aiming to evaluate the influence...

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Bibliographic Details
Main Authors: Ahmed Ezz El-Arab Abd Al-Aliem, Eman A.E. Badr, Elsayed Ibrahem El-Shayeb, Ahmed Megahed Ahmed Taman, Abd El-naser Abd El-atty Gadallah
Format: Article
Language:English
Published: Elsevier 2021-12-01
Series:Biochemistry and Biophysics Reports
Subjects:
IBD
SNP
Online Access:http://www.sciencedirect.com/science/article/pii/S2405580821002089
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Summary:Background: To date, the cause of inflammatory bowel disease (IBD) remains a mystery. A balance between cell proliferation and apoptosis maintains intestinal tissue homeostasis. Dissociation-induced myosin-actin contraction results in stem cell apoptosis. This study aiming to evaluate the influence of the myosin heavy chain 9 (MYH9) gene single nucleotide polymorphisms (SNPs) on inflammatory bowel disease. Subjects: and methods: The study carried on eighty patients with IBD and seventy controls. All participants subjected to history taking, thorough physical examination, colonoscopy and laboratory investigations. Genotyping performed for rs4821480 and rs3752462 by SNP assay real-time PCR methods. Results: On analyzing rs3752462 CT and TT genotypes were significantly more frequent in IBD patients as compared to controls with 4.6 fold increase in the risk of IBD. While on analyzing rs4821480, The TG and GG genotypes have significant increased distribution among the IBD patients as compared to the controls with 5.3 fold increase in the risk of IBD and higher prevalence of GG genotype in patients with low hemoglobin level and higher BMI. Conclusion: The rs3752462 T allele and rs4821480 G allele of MYH9 are associated with more susceptibility to IBD.
ISSN:2405-5808