Abstract
Accumulating evidence suggests that Mcl-1 plays a critical pro-survival role in the development and maintenance of both normal and malignant tissues. Regulation of Mcl-1 expression occurs at multiple levels, allowing for either the rapid induction or elimination of the protein in response to different cellular events. This suggests that Mcl-1 can play an early role in response to signals directing either cell survival or cell death. Deregulation of pathways regulating Mcl-1 that result in its over-expression likely contribute to a cells inability to properly respond to death signals possibly leading to cell immortalization and tumorigenic conversion. Correspondingly, Mcl-1 has been shown to be up-regulated in numerous hematological and solid tumor malignancies. Moreover, this up-regulation appears to be a factor in the resistance of some cancer types to conventional cancer therapies. Mechanisms that abrogate the pro-survival function of Mcl-1 either by diminishing its levels or inactivating its functional BH3 groove have shown promise for the combinational treatment with existing cancer therapies and as single agents in certain malignancies. Here we review the various pathways that regulate Mcl-1 expression and describe agents that are currently under development to modulate Mcl-1 activity for therapeutic benefit in oncology.
Keywords: Cancer, apoptosis, Bcl-2 family, Mcl-1, Mcl-1 targeted therapeutics
Current Molecular Medicine
Title: Unique Biology of Mcl-1: Therapeutic Opportunities in Cancer
Volume: 8 Issue: 2
Author(s): Gordon C. Shore and Matthew R. Warr
Affiliation:
- Department of Biochemistry,McIntyre Medical Sciences Building, McGill University,3655 Promenade Sir William Osler, Montreal, Quebec, H3G 1Y6,Canada.,Canada
Keywords: Cancer, apoptosis, Bcl-2 family, Mcl-1, Mcl-1 targeted therapeutics
Abstract: Accumulating evidence suggests that Mcl-1 plays a critical pro-survival role in the development and maintenance of both normal and malignant tissues. Regulation of Mcl-1 expression occurs at multiple levels, allowing for either the rapid induction or elimination of the protein in response to different cellular events. This suggests that Mcl-1 can play an early role in response to signals directing either cell survival or cell death. Deregulation of pathways regulating Mcl-1 that result in its over-expression likely contribute to a cells inability to properly respond to death signals possibly leading to cell immortalization and tumorigenic conversion. Correspondingly, Mcl-1 has been shown to be up-regulated in numerous hematological and solid tumor malignancies. Moreover, this up-regulation appears to be a factor in the resistance of some cancer types to conventional cancer therapies. Mechanisms that abrogate the pro-survival function of Mcl-1 either by diminishing its levels or inactivating its functional BH3 groove have shown promise for the combinational treatment with existing cancer therapies and as single agents in certain malignancies. Here we review the various pathways that regulate Mcl-1 expression and describe agents that are currently under development to modulate Mcl-1 activity for therapeutic benefit in oncology.
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Cite this article as:
Shore C. Gordon and Warr R. Matthew, Unique Biology of Mcl-1: Therapeutic Opportunities in Cancer, Current Molecular Medicine 2008; 8(2) . https://dx.doi.org/10.2174/156652408783769580
| DOI https://dx.doi.org/10.2174/156652408783769580 |
Print ISSN 1566-5240 |
| Publisher Name Bentham Science Publisher |
Online ISSN 1875-5666 |
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