Pathways and mechanisms of venetoclax resistance

Abstract: The approval of venetoclax, a “BH3-mimetic” antagonist of the BCL-2 anti-apoptotic protein, for chronic lymphocytic leukemia represents a major milestone in translational apoptosis research. Venetoclax has already received “breakthrough” designation for acute myeloid leukemia, and is being studied in many other tumor types. However, resistance to BCL-2 inhibitor monotherapy may rapidly ensue. Several studies have shown that the other two major anti-apoptotic BCL-2 family proteins, BCL-XL and MCL-1, are the mai… Show more

“…Ex vivo sensitivity to venetoclax correlated with levels of expression of BCL-2 protein, but not with levels of BCL extra long (BCL-XL) or myeloid cell leukemia 1 (MCL-1), the 2 other major antiapoptotic proteins in the BCL-2 family. Levels of MCL-1, a major mediator of resistance to venetoclax, 4 inversely correlated with those of BCL-2. Based on these preclinical efficacy data, the investigators administered venetoclax on a compassionate-use basis to 2 patients with R/R T-PLL, both of whose cells exhibited ex vivo sensitivity to venetoclax.…”

“…Indeed, given the central role of BCL-2 in the regulation of apoptosis, it is not surprising that venetoclax acts as a universal apoptosis sensitizer, lending itself to a very large number of rational combinations across tumor types. 4 As far as single-agent activity of venetoclax is concerned, an important determinant of the same is the extent of dependence of the specific tumor type on BCL-2 for survival, and the relative importance of other antiapoptotic BCL-2 family proteins, specifically BCL-XL and MCL-1. 4 For example, BH3 profiling has revealed a high degree of dependence of early T-cell precursor acute lymphoblastic leukemia (ALL) on BCL-2, correlating with in vitro and in vivo sensitivity to venetoclax.…”

“…4 As far as single-agent activity of venetoclax is concerned, an important determinant of the same is the extent of dependence of the specific tumor type on BCL-2 for survival, and the relative importance of other antiapoptotic BCL-2 family proteins, specifically BCL-XL and MCL-1. 4 For example, BH3 profiling has revealed a high degree of dependence of early T-cell precursor acute lymphoblastic leukemia (ALL) on BCL-2, correlating with in vitro and in vivo sensitivity to venetoclax. 8 Similarly, even though the majority of pediatric ALLs in xenograft studies seem to require…”

“…One of the mechanisms through which CDK9 inhibitors like SNS-032 induce cell death is by transcriptionally downregulating MCL-1, and the combination of CDK9 inhibitors with venetoclax or navitoclax is a well-recognized synergistic strategy. 4 The strength of the study by Boidol and colleagues lies in the clinical responses to venetoclax they describe. However, the underlying biologic heterogeneity of T-PLL is apparent even in these 2 cases, which differed markedly in terms of time to response and dose dependence of the clinical response.…”

T-PLL: another check on the venetoclax list?

“…Ex vivo sensitivity to venetoclax correlated with levels of expression of BCL-2 protein, but not with levels of BCL extra long (BCL-XL) or myeloid cell leukemia 1 (MCL-1), the 2 other major antiapoptotic proteins in the BCL-2 family. Levels of MCL-1, a major mediator of resistance to venetoclax, 4 inversely correlated with those of BCL-2. Based on these preclinical efficacy data, the investigators administered venetoclax on a compassionate-use basis to 2 patients with R/R T-PLL, both of whose cells exhibited ex vivo sensitivity to venetoclax.…”

“…Indeed, given the central role of BCL-2 in the regulation of apoptosis, it is not surprising that venetoclax acts as a universal apoptosis sensitizer, lending itself to a very large number of rational combinations across tumor types. 4 As far as single-agent activity of venetoclax is concerned, an important determinant of the same is the extent of dependence of the specific tumor type on BCL-2 for survival, and the relative importance of other antiapoptotic BCL-2 family proteins, specifically BCL-XL and MCL-1. 4 For example, BH3 profiling has revealed a high degree of dependence of early T-cell precursor acute lymphoblastic leukemia (ALL) on BCL-2, correlating with in vitro and in vivo sensitivity to venetoclax.…”

“…4 As far as single-agent activity of venetoclax is concerned, an important determinant of the same is the extent of dependence of the specific tumor type on BCL-2 for survival, and the relative importance of other antiapoptotic BCL-2 family proteins, specifically BCL-XL and MCL-1. 4 For example, BH3 profiling has revealed a high degree of dependence of early T-cell precursor acute lymphoblastic leukemia (ALL) on BCL-2, correlating with in vitro and in vivo sensitivity to venetoclax. 8 Similarly, even though the majority of pediatric ALLs in xenograft studies seem to require…”

“…One of the mechanisms through which CDK9 inhibitors like SNS-032 induce cell death is by transcriptionally downregulating MCL-1, and the combination of CDK9 inhibitors with venetoclax or navitoclax is a well-recognized synergistic strategy. 4 The strength of the study by Boidol and colleagues lies in the clinical responses to venetoclax they describe. However, the underlying biologic heterogeneity of T-PLL is apparent even in these 2 cases, which differed markedly in terms of time to response and dose dependence of the clinical response.…”

T-PLL: another check on the venetoclax list?

“…Loss of wild-type p53 activity is thought to be a major predictor of failure to respond to chemotherapy in a wide variety of malignant neoplasms [1]. It is increasingly recognised that different neoplasm types display different degrees of addiction to individual Bcl-2 family proteins in particular [2].…”

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An effective chemotherapy‐free regimen of ponatinib plus venetoclax for relapsed/refractory Philadelphia chromosome‐positive acute lymphoblastic leukemia