Brian Plucinsky scite author profile

Brian Plucinsky

2Publications

11Citation Statements Received

64Citation Statements Given

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The Wistar Institute

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A non-natural nucleotide uses a specific pocket to selectively inhibit telomerase activity

et al. 2019

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Telomerase, a unique reverse transcriptase that specifically extends the ends of linear chromosomes, is up-regulated in the vast majority of cancer cells. Here, we show that an indole nucleotide analog, 5-methylcarboxyl-indolyl-2′-deoxyriboside 5′-triphosphate (5-MeCITP), functions as an inhibitor of telomerase activity. The crystal structure of 5-MeCITP bound to the Tribolium castaneum telomerase reverse transcriptase reveals an atypical interaction, in which the nucleobase is flipped in the active site. In this orientation, the methoxy group of 5-MeCITP extends out of the canonical active site to interact with a telomerase-specific hydrophobic pocket formed by motifs 1 and 2 in the fingers domain and T-motif in the RNA-binding domain of the telomerase reverse transcriptase. In vitro data show that 5-MeCITP inhibits telomerase with a similar potency as the clinically administered nucleoside analog reverse transcriptase inhibitor azidothymidine (AZT). In addition, cell-based studies show that treatment with the cell-permeable nucleoside counterpart of 5-MeCITP leads to telomere shortening in telomerase-positive cancer cells, while resulting in significantly lower cytotoxic effects in telomerase-negative cell lines when compared with AZT treatment.

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Structure of TERT in complex with a novel telomerase inhibitor

Hernandez-Sanchez¹,

Huang²,

Plucinsky³

et al. 2019

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Brian Plucinsky

A non-natural nucleotide uses a specific pocket to selectively inhibit telomerase activity

Structure of TERT in complex with a novel telomerase inhibitor

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