Your search keyword '"Aastha Chhabra"' showing total 2 results

1. Analysis of human collagen sequences

Author

Pracheta Anand, Aastha Chhabra, Manisha Nassa, Vibha Rani, Umang Malhotra, Aditi Jain, and Astha Jaiswal

Subjects

Scaffold, Comparative characterization, General Medicine, Computational biology, Extracellular matrix, Biology, Hypothesis, Bioinformatics, FACIT collagen, Biocomputational tools, Complex protein, Glycine, Proline, Collagen

Abstract

The extracellular matrix is fast emerging as important component mediating cell-cell interactions, along with its established role as a scaffold for cell support. Collagen, being the principal component of extracellular matrix, has been implicated in a number of pathological conditions. However, collagens are complex protein structures belonging to a large family consisting of 28 members in humans; hence, there exists a lack of in depth information about their structural features. Annotating and appreciating the functions of these proteins is possible with the help of the numerous biocomputational tools that are currently available. This study reports a comparative analysis and characterization of the alpha-1 chain of human collagen sequences. Physico-chemical, secondary structural, functional and phylogenetic classification was carried out, based on which, collagens 12, 14 and 20, which belong to the FACIT collagen family, have been identified as potential players in diseased conditions, owing to certain atypical properties such as very high aliphatic index, low percentage of glycine and proline residues and their proximity in evolutionary history. These collagen molecules might be important candidates to be investigated further for their role in skeletal disorders.

Published

2012

2. Comparative analysis of human matrix metalloproteinases: Emerging therapeutic targets in diseases

Author

Shrey Kohli, Astha Jaiswal, Umang Malhotra, Aastha Chhabra, and Vibha Rani

Subjects

Protein family, business.industry, In silico, Liver fibrosis, A protein, General Medicine, Disease, Hypothesis, Matrix metalloproteinase, Bioinformatics, Extracellular matrix, Medicine, Identification (biology), business

Abstract

The identification of specific target proteins for any diseased condition involves extensive characterization of the potentially involved proteins. Members of a protein family demonstrating comparable features may show certain unusual features when implicated in a pathological condition. Advancements in the field of computational biology and the use of various bioinformatics tools for analysis can aid researchers to comprehend their system of work in primary stages of research. This initial screening can help to reduce time and cost of testing and experimentation in laboratory. Human matrix metalloproteinase (MMP) family of endopeptidases is one such family of 23 members responsible for the remodeling of extracellular matrix (ECM) by degradation of the ECM proteins. Though their role has been implicated in various pathological conditions such as arthritis, atherosclerosis, cancer, liver fibrosis, cardio-vascular and neurodegenerative disorders, little is known about the specific involvement of members of the large MMP family in diseases. A comparative in silico characterization of the MMP protein family has been carried out to analyze their physico-chemical, secondary structural and functional properties. Based on the observed patterns of occurrence of atypical features, we hypothesize that cysteine rich and highly thermostable MMPs might be key players in diseased conditions. Thus, a plausible grouping of disease responsive MMPs that might be considered as promising clinical targets may be done. This study can be used as a fundamental approach to characterize, analyze and screen large protein families for the identification of signature patterns.

Published

2011