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Current Chemical Biology

Editor-in-Chief

ISSN (Print): 2212-7968
ISSN (Online): 1872-3136

Research Article

Application of Bioinformatics to Investigate the Mutant Alleles of Multiple Endocrine Neoplasia Type 1 on its Structure, Function and Stability

Author(s): Muhammad A. Hassan, Muhammad Qasim, Aqib Z. Khan, Mohsin A. Nasir, Mohammad Bilal and Simon Manzoor

Volume 10, Issue 2, 2016

Page: [142 - 148] Pages: 7

DOI: 10.2174/2212796810666161028113113

Price: $65

Abstract

Background: Multiple Endocrine Neoplasia Type 1 is caused by mutation in MEN1 genes that leads to parathyroid adenoma, duodenopancreatic neuroendocrine tumors, and pituitary adenomas.It also initiator of benign Lipomas, angiiofibromas and carcinoid tumor of thymus and lungs. It also incorporated in many such as transcription regulation, apoptosis, cell cycle control and DNA damage repair mechanisms.

Methodology: The following mutations i.e. P12L, L22R, E45K, G110E, F144V, I147F, G161D, C170R, E184D and V220M in MEN1 were selected that were already reported. By using bioinformatics approaches check single amino acid substitution either their effect on protein structure, function and stability. In this methodology MODELLER, Chimera, NetSurfP, SNAP, IUPred, Polyphen and CDD were used.

Result: All the predicted structure were showing accuracy greater than 90%. Also checked that L22R, E45K, F144V, I147F, G161D, C170R and V220M mutation were present in helix of mutated model and P12L, G110E and E184D are present in coil region. In P12L, E184D and G110E, mutation in exposed amino and their relative surface accessibility were decreased. While in L22R, E45K, F114V, I147F, G161D, C170R and V220M were present in the form of buried amino acid and their relative surface accessibility increased. These prediction showing expected accuracy of 78%, 82%, and 96%, 63%, 78%, 78%, 96%, 93%, 87% and 78% respectively in functionality changes. In case of structural damaging all the mutation showing high damaging effect on their function but their disorder tendency were low.

Conclusion: Our results have shown that missense mutations P12L, L22R, E45K, G110E, F144V, I147F, G161D, C170R, E184D and V220M have strong structural, conformational, Function and pathogenic but low tendency order. This research helpful for clinical work at MEN1 genes to find out which mutation is responsible for disease causing.

Keywords: Conformational changes, disorder tendency, insilco.

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