Mutation Spectrum in TPO Gene of Bangladeshi Patients with Thyroid Dyshormonogenesis and Analysis of the Effects of Different Mutations on the Structural Features and Functions of TPO Protein through In Silico Approach | Zendy

Mst. Noorjahan Begum | Zendy; Md Tarikul Islam | Zendy; Shekh Rezwan Hossain | Zendy; Golam Sarower Bhuyan | Zendy; Mohammad A. Halim | Zendy; Imrul Shahriar | Zendy; Suprovath Kumar Sarker | Zendy; Shahinur Haque | Zendy; Tasnia Kawsar Konika | Zendy; Md. Sazzadul Islam | Zendy; Asifuzzaman Rahat | Zendy; Syeda Kashfi Qadri | Zendy; Rosy Sultana | Zendy; Suraiya Begum | Zendy; Sadia Sultana | Zendy; Narayan Chandra Saha | Zendy; Mizanul Hasan | Zendy; Muhammad Abul Hasanat | Zendy; Hurjahan Banu | Zendy; Hossain Uddin Shekhar | Zendy; Emran Kabir Chowdhury | Zendy; Abu Ashfaqur Sajib | Zendy; Abul Bashar Mir Md. Khademul Islam | Zendy; Syed Saleheen Qadri | Zendy; Firdausi Qadri | Zendy; Sharif Akhteruzzaman | Zendy; Kaiissar Mannoor | Zendy

Open Access

Mutation Spectrum in TPO Gene of Bangladeshi Patients with Thyroid Dyshormonogenesis and Analysis of the Effects of Different Mutations on the Structural Features and Functions of TPO Protein through In Silico Approach

Author(s) -

Mst. Noorjahan Begum,

Md Tarikul Islam,

Shekh Rezwan Hossain,

Golam Sarower Bhuyan,

Mohammad A. Halim,

Imrul Shahriar,

Suprovath Kumar Sarker,

Shahinur Haque,

Tasnia Kawsar Konika,

Md. Sazzadul Islam,

Asifuzzaman Rahat,

Syeda Kashfi Qadri,

Rosy Sultana,

Suraiya Begum,

Sadia Sultana,

Narayan Chandra Saha,

Mizanul Hasan,

Muhammad Abul Hasanat,

Hurjahan Banu,

Hossain Uddin Shekhar,

Emran Kabir Chowdhury,

Abu Ashfaqur Sajib,

Abul Bashar Mir Md. Khademul Islam,

Syed Saleheen Qadri,

Firdausi Qadri,

Sharif Akhteruzzaman,

Kaiissar Mannoor

Publication year - 2019

Publication title -

biomed research international

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.772

H-Index - 126

eISSN - 2314-6141

pISSN - 2314-6133

DOI - 10.1155/2019/9218903

Subject(s) - nonsynonymous substitution , mutant , thyroid peroxidase , mutation , homology modeling , gene , chemistry , wild type , genetics , microbiology and biotechnology , in silico , biology , biochemistry , thyroid , genome , enzyme

Although thyroid dyshormonogenesis (TDH) accounts for 10-20% of congenital hypothyroidism (CH), the molecular etiology of TDH is unknown in Bangladesh. Thyroid peroxidase (TPO) is most frequently associated with TDH and the present study investigated the spectrum of TPO mutations in Bangladeshi patients and analyzed the effects of mutations on TPO protein structure through in silico approach. Sequencing-based analysis of TPO gene revealed four mutations in 36 diagnosed patients with TDH including three nonsynonymous mutations, namely, p.Ala373Ser, p.Ser398Thr, and p.Thr725Pro, and one synonymous mutation p.Pro715Pro. Homology modelling-based analysis of predicted structures of MPO-like domain (TPO 142-738 ) and the full-length TPO protein (TPO 1-933 ) revealed differences between mutant and wild type structures. Molecular docking studies were performed between predicted structures and heme. TPO 1-933 predicted structure showed more reliable results in terms of interactions with the heme prosthetic group as the binding energies were -11.5 kcal/mol, -3.2 kcal/mol, -11.5 kcal/mol, and -7.9 kcal/mol for WT, p.Ala373Ser, p.Ser398Thr, and p.Thr725Pro, respectively, implying that p.Ala373Ser and p.Thr725Pro mutations were more damaging than p.Ser398Thr. However, for the TPO 142-738 predicted structures, the binding energies were -11.9 kcal/mol, -10.8 kcal/mol, -2.5 kcal/mol, and -5.3 kcal/mol for the wild type protein, mutant proteins with p.Ala373Ser, p.Ser398Thr, and p.Thr725Pro substitutions, respectively. However, when the interactions between the crucial residues including residues His239, Arg396, Glu399, and His494 of TPO protein and heme were taken into consideration using both TPO 1-933 and TPO 142-738 predicted structures, it appeared that p.Ala373Ser and p.Thr725Pro could affect the interactions more severely than the p.Ser398Thr. Validation of the molecular docking results was performed by computer simulation in terms of quantum mechanics/molecular mechanics (QM/MM) and molecular dynamics (MD) simulation. In conclusion, the substitutions mutations, namely, p.Ala373Ser, p.Ser398Thr, and p.Thr725Pro, had been involved in Bangladeshi patients with TDH and molecular docking-based study revealed that these mutations had damaging effect on the TPO protein activity.

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