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Expression Differences in BCL2 Family Members between Uveal and Cutaneous Melanomas Account for Varying Sensitivity to BH3 Mimetics

Authors :
Nabanita Mukherjee
Chiara R. Dart
Carol M. Amato
Adam Honig-Frand
James R. Lambert
Karoline A. Lambert
William A. Robinson
Richard P. Tobin
Martin D. McCarter
Kasey L. Couts
Mayumi Fujita
David A. Norris
Yiqun G. Shellman
Source :
J Invest Dermatol
Publication Year :
2021

Abstract

Uveal melanoma (UM) is a subtype of melanoma. Although they share a melanocytic origin with cutaneous melanoma (CM), patients with UM have few treatment options. BCL2 homologous 3 mimetics are small-molecule drugs that mimic proapoptotic BCL2 family members. We compared BCL2 family member expression between UM and CM using immunoblot and The Cancer Genome Atlas transcriptomic analysis. UM has a unique signature of low BFL1 and high PUMA proteins compared with CM and 30 other cancer types, making them an attractive candidate for BCL2 homologous 3 protein mimetics. We tested the efficacy of a BCL2 inhibitor and MCL1 inhibitor (MCL1i) in UM, with viability assays, live-cell imaging, sphere assays, and mouse xenograft models. UM had a higher sensitivity to MCL1i than CM. Overexpression of BFL1 or knockdown of PUMA made the UM more resistant to MCL1i. In contrast, MAPK/extracellular signal‒regulated kinase inhibitor treatment in CM made them more sensitive to MCL1i. However, MCL1i-alone treatment was not very effective to reduce the UM initiating cells; to overcome this, we employed a combination of MCL1i with BCL2 inhibitor that synergistically inhibited UM initiating cell's capacity to expand. Overall, we identify a distinct expression profile of BCL2 family members for UM that makes them susceptible to BCL2 homologous 3 mimetics.

Details

ISSN :
15231747
Volume :
142
Issue :
7
Database :
OpenAIRE
Journal :
The Journal of investigative dermatology
Accession number :
edsair.doi.dedup.....e2eec9379cf9bce62a838d548bf3bf55