Mechanistic influence of discreet conformation of human telomerase linker region.

J Biomol Struct Dyn

Amity Institute of Biotechnology, Amity University Mumbai, Mumbai, Maharashtra, India.

Published: February 2024

AI Article Synopsis

  • Approximately 90% of cancers show human telomerase activity, making it an important target for cancer treatment.
  • Recent research has determined the crystal structure of telomerase, but the flexible linker region's tertiary structure is still unknown.
  • This study predicted the full-length structure of hTERT using two strategies, finding that a conjoined model showed better stability and flexibility compared to an iterative threading model, indicating significant structural changes in the linker region.

Article Abstract

Approximately 90% of malignancies have been shown to have human telomerase activity, establishing it as a viable therapeutic target. The crystal structure of telomerase was determined recently. However, the tertiary structure of the non-conserved flexible linker region remains unresolved. This study aims to predict the full-length tertiary structure of the human telomerase reverse transcriptase (hTERT). Two strategies were employed to determine the full-length structure of hTERT (1132 amino acids); iterative threading and a conjoined model generated from machine learning and energy functions. After energy minimization, Ramachandran Plot analysis, and simulation; the conjoined model was considered of better quality and stability. The linker region of the conjoined depicted two helices from approximately 275-284 and 201-211 amino acids respectively in contrast to the iterative threading model which has a single helix. Moreover, the region was observed to undergo major structural changes throughout the simulation. These changes signify its flexibility which might be due to the region having a significant number of glycine and proline and could enhance the clamping movement.Communicated by Ramaswamy H. Sarma.

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Source
http://dx.doi.org/10.1080/07391102.2024.2310212DOI Listing

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