An In Silico Analysis of Troponin I Mutations in Hypertrophic Cardiomyopathy of Indian Origin

Hypertrophic Cardiomyopathy (HCM) is an autosomal dominant disorder of the myocardium which is hypertrophied resulting in arrhythmias and heart failure leading to sudden cardiac death (SCD). Several sarcomeric proteins and modifier genes have been implicated in this disease. Troponin I, being a part of the Troponin complex (troponin I, troponin C, troponin T), is an important gene for sarcomeric function. Four mutations (1 novel) were identified in Indian HCM cases, namely, Pro82Ser, Arg98Gln, Arg141Gln and Arg162Gln in Troponin I protein, which are in functionally significant domains. In order to analyse the effect of the mutations on protein stability and protein-protein interactions within the Troponin complex, an in silico study was carried out. The freely available X-ray crystal structure (PDB ID: 1JIE) was used as the template to model the protein followed by loop generation and development of troponin complex for both the troponin I wild type and four mutants (NCBI ID: PRJNA194382). The structural study was carried out to determine the effect of mutation on the structural stability and protein-protein interactions between three subunits in the complex. These mutations, especially the arginine to glutamine substitutions were found to result in local perturbations within the troponin complex by creating/removing inter/intra molecular hydrogen bonds with troponin T and troponin C. This has led to a decrease in the protein stability and loss of important interactions between the three subunits. It could have a significant impact on the disease progression when coupled with allelic heterogeneity which was observed in the cases carrying these mutations. However, this can be further confirmed by functional studies on protein levels in the identified cases.

• Publication year

  2013

• Venue

  PLoS ONE

• Publication date

  2013-08-13

• Fields of study

  Biology, Medicine

• Identifiers
  DOI 10.1371/journal.pone.0070704PMID 23967088PMCID 3742764
• External record

  Open on Semantic Scholar

• Source metadata

  Semantic Scholar, PubMed

• No claims are published for this paper.

• No concepts are published for this paper.

• High prevalence of Arginine to Glutamine Substitution at 98, 141 and 162 positions in Troponin I (TNNI3) associated with hypertrophic cardiomyopathy among Indians

  2012cited by this paper
• Novel mutations in beta-myosin heavy chain, actin and troponin-I genes associated with dilated cardiomyopathy in Indian population

  2009cited by this paper
• The dominant role of side‐chain backbone interactions in structural realization of amino acid code. ChiRotor: A side‐chain prediction algorithm based on side‐chain backbone interactions

  2007cited by this paper
• Dilated and Hypertrophic Cardiomyopathy Mutations in Troponin and &agr;-Tropomyosin Have Opposing Effects on the Calcium Affinity of Cardiac Thin Filaments

  2007cited by this paper
• Statistical potential for assessment and prediction of protein structures

  2006cited by this paper
• Increased Ca2+ Affinity of Cardiac Thin Filaments Reconstituted with Cardiomyopathy-related Mutant Cardiac Troponin I*

  2006cited by this paper
• The relationship between synonymous codon usage and protein structure in Escherichia coli and Homo sapiens.

  2004cited by this paper
• Amino‐Acid Properties and Consequences of Substitutions

  2003cited by this paper
• Structure of the core domain of human cardiac troponin in the Ca2+-saturated form

  2003cited by this paper
• Two mutations in troponin I that cause hypertrophic cardiomyopathy have contrasting effects on cardiac muscle contractility.

  2002influential reference
• Expression patterns and gene distribution in the human genome.

  2002cited by this paper
• Troponin I isoforms and chimeras: tuning the molecular switch of cardiac contraction.

  2001cited by this paper
• Degradation of mutant proteins, underlying "loss of function" phenotypes, plays a major role in genetic disease.

  2001cited by this paper
• Expression profiling of cardiac genes in human hypertrophic cardiomyopathy: insight into the pathogenesis of phenotypes.

  2001cited by this paper
• Transgenic modeling of a cardiac troponin I mutation linked to familial hypertrophic cardiomyopathy.

  2000cited by this paper
• Modeling of loops in protein structures

  2000cited by this paper
• Phenotypes of patients with "simple" Mendelian disorders are complex traits: thresholds, modifiers, and systems dynamics.

  2000cited by this paper
• Monogenic traits are not simple: lessons from phenylketonuria.

  1999cited by this paper
• The relationship between synonymous codon usage and protein structure

  1998cited by this paper
• Regulatory Properties of the NH2- and COOH-terminal Domains of Troponin T

  1998cited by this paper
• Some Convergence Properties of Descent Methods

  1997cited by this paper
• VERIFY3D: assessment of protein models with three-dimensional profiles.

  1997cited by this paper
• Relationship between genotype and phenotype in monogenic diseases: Relevance to polygenic diseases

  1996cited by this paper
• Comparative protein modelling by satisfaction of spatial restraints.

  1993cited by this paper
• PROCHECK: a program to check the stereochemical quality of protein structures

  1993cited by this paper
• Validation of the general purpose QUANTA ®3.2/CHARMm® force field

  1992cited by this paper
• CHARMM: A program for macromolecular energy, minimization, and dynamics calculations

  1983cited by this paper
• Optimization by Simulated Annealing

  1983cited by this paper
• Proton-magnetic-resonance studies on the interaction of rabbit skeletal-muscle troponin I with troponin C and actin.

  1982cited by this paper
• Codon catalog usage and the genome hypothesis.

  1980cited by this paper
• Function minimization by conjugate gradients

  1964cited by this paper

• Troponin I – a comprehensive review of its function, structure, evolution, and role in muscle diseases

  2025cites this paper
• Novel MYBPC3 Mutations in Indian Population with Cardiomyopathies

  2023cites this paper
• Cardiac biomarkers and detection methods for myocardial infarction

  2022cites this paper
• Novel Mutations in β-MYH7 Gene in Indian Patients With Dilated Cardiomyopathy

  2021cites this paper
• A Complete Absence of Missense Mutation in Myosin Regulatory and Essential Light Chain Genes of South Indian Hypertrophic and Dilated Cardiomyopathies

  2019cites this paper
• Identification of novel L2HGDH mutation in a large consanguineous Pakistani family- a case report

  2018cites this paper
• Impact of Variant Reclassification in the Clinical Setting of Cardiovascular Genetics

  2017cites this paper
• Modulation of the picosecond dynamics of troponin by the cardiomyopathy-causing mutation K247R of troponin T observed by quasielastic neutron scattering.

  2017cites this paper
• Recent Advances in the Molecular Genetics of Familial Hypertrophic Cardiomyopathy in South Asian Descendants

  2016cites this paper
• Coexistence of Digenic Mutations in Both Thin (TPM1) and Thick (MYH7) Filaments of Sarcomeric Genes Leads to Severe Hypertrophic Cardiomyopathy in a South Indian FHCM

  2015influential citation
• Cardiac troponin I Pro82Ser variant induces diastolic dysfunction, blunts β-adrenergic response, and impairs myofilament cooperativity.

  2015cites this paper
• A Novel Arginine to Tryptophan (R144W) Mutation in Troponin T (cTnT) Gene in an Indian Multigenerational Family with Dilated Cardiomyopathy (FDCM)

  2014cites this paper