Bcl-2, Bcl-xL, and Bcl-w are not equivalent targets of ABT-737 and navitoclax (ABT-263) in lymphoid and leukemic cells

Mérino, Delphine; Khaw, Seong Lin; Glaser, S.; Anderson, Daniel J.; Belmont, Lisa D.; Wong, Chihunt; Peng, Yue; Robati, Mikara; Phipson, Belinda; Fairlie, W. Douglas; Lee, Erinna F.; Campbell, Kirsteen J.; Vandenberg, Cassandra J.; Cory, Suzanne; Roberts, Andrew W.; Ludlam, Mary J. C.; Huang, David C.S.; Bouillet, Philippe

doi:10.1182/blood-2011-12-400929

Cited by 166 publications

(164 citation statements)

References 50 publications

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“…24,25 Following exposure to cytotoxic agents, the level of BH3-only proteins increased in both WT and Mcl-1tg thymocytes, in a pattern consistent with previous findings. 26 Thus, for the DNA-damaging agent etoposide, there was a marked increase in Puma, Bim and Noxa (Figures 2b and f); for PMA, an increase in Bim and Puma; for ionomycin, an increase in Bim and Puma proteins and Noxa RNA; and for dexamethasone, an increase in Bim (Figure 2e).…”

Section: Resultssupporting

confidence: 89%

Elevated Mcl-1 inhibits thymocyte apoptosis and alters thymic selection

et al. 2012

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Section: Resultssupporting

confidence: 89%

Elevated Mcl-1 inhibits thymocyte apoptosis and alters thymic selection

et al. 2012

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“…BH3-mimetic compounds bind directly to and block the BCL-2 pro-survival proteins and thereby elicit apoptosis even in cells lacking upstream activators of BH3-only proteins, such as the tumour-suppressor p53, which is critical for transcriptional induction of Puma and Noxa However, as ABT-737 and ABT-263 bind only a subset of the BCL-2-like pro-survival proteins, overexpression of MCL1 or A1/BFL-1, both of which are not inhibited by these compounds, has the potential to confer resistance to therapy. 164 Some cancers (such as CLL) with very high expression of BCL-2 (and possibly also cancers expressing high levels of BCL-XL and/or BCL-W) respond robustly to the existing BH3-mimetics when used as single agents. However, in order to maximise treatment efficacy, in many cancers these BH3-mimetics are probably best employed in combination with drugs known to activate BH3-only proteins, such as BIM or PUMA, that can potently neutralise MCL-1 and/or A1.…”

Section: The Role Of the Bcl-2-regulated Apoptotic Pathway In Cancer mentioning

confidence: 99%

The BCL-2 protein family, BH3-mimetics and cancer therapy

2015

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Escape from apoptosis is a key attribute of tumour cells and facilitates chemo-resistance. The 'BCL-2-regulated' or 'intrinsic' apoptotic pathway integrates stress and survival signalling to govern whether a cancer cell will live or die. Indeed, many pro-apoptotic members of the BCL-2 family have demonstrated tumour-suppression activity in mouse models of cancer and are lost or repressed in certain human cancers. Conversely, overexpression of pro-survival BCL-2 family members promotes tumorigenesis in humans and in mouse models. Many of the drugs currently used in the clinic mediate their therapeutic effects (at least in part) through the activation of the BCL-2-regulated apoptotic pathway. However, initiators of this apoptotic pathway, such as p53, are mutated, lost or silenced in many human cancers rendering them refractory to treatment. To counter such resistance mechanisms, a novel class of therapeutics, 'BH3-mimetics', has been developed. These drugs directly activate apoptosis by binding and inhibiting select antiapoptotic BCL-2 family members and thereby bypass the requirement for upstream initiators, such as p53. In this review, we discuss the role of the BCL-2 protein family in the development and treatment of cancer, with an emphasis on mechanistic studies using well-established mouse models of cancer, before describing the development and already recognised potential of the BH3-mimetic compounds.

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“…ABT-737 and the highly related ABT-263 both inhibit BCL2, BCLXL and BCLW [19][20][21] and were shown to be effective in killing cancer cells in vitro and in vivo 21 with a preference for BCL2. 19,22 As BCL2 protein expression is often upregulated in hematopoietic cancers, it represents a promising target, which was supported by high efficacy of these BH3 mimetics in animal experiments. 21 However, in vivo efficacy is limited due to thrombocytopenia, which relates to a dependence of platelets on BCLXL for survival.…”

mentioning

confidence: 97%

Decreased mitochondrial priming determines chemoresistance of colon cancer stem cells

et al. 2014

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Tumor heterogeneity is in part determined by the existence of cancer stem cells (CSCs) and more differentiated tumor cells. CSCs are considered to be the tumorigenic root of cancers and suggested to be chemotherapy resistant. Here we exploited an assay that allowed us to measure chemotherapy-induced cell death in CSCs and differentiated tumor cells simultaneously. This confirmed that CSCs are selectively resistant to conventional chemotherapy, which we revealed is determined by decreased mitochondrial priming. In agreement, lowering the anti-apoptotic threshold using ABT-737 and WEHI-539 was sufficient to enhance chemotherapy efficacy, whereas ABT-199 failed to sensitize CSCs. Our data therefore point to a crucial role of BCLXL in protecting CSCs from chemotherapy and suggest that BH3 mimetics, in combination with chemotherapy, can be an efficient way to target chemotherapy-resistant CSCs. Cell Death and Differentiation (2014) 21, 1170-1177 doi:10.1038/cdd.2014 published online 28 March 2014 Colorectal cancer is the third most common cancer worldwide.1,2 Patients with advanced stage colorectal cancer are routinely treated with 5-fluorouracil (5-FU), leucovorin and oxaliplatin (FOLFOX), or with 5-FU, leucovorin and irinotecan (FOLFIRI), often in combination with targeted agents such as anti-VEGF or anti-EGFR at metastatic disease.3-6 Despite this intensive treatment, therapy is still insufficiently effective and chemotherapy resistance occurs frequently. Although still speculative, it has been suggested that unequal sensitivity to chemotherapy is due to an intratumoral heterogeneity that is orchestrated by cancer stem cells (CSCs) that can self-renew and give rise to more differentiated progeny. 7,8 When isolated from patients, CSCs efficiently form tumors upon xenotransplantation into mice which resemble the primary tumor from which they originated. [9][10][11] In addition, many xenotransplantation studies have emphasized the importance of CSCs for tumor growth.9-12 Colon CSCs were originally isolated from primary human colorectal tumor specimens using CD133 as cell surface marker and shown to be highly tumorigenic when compared with the non-CSCs population within a tumor. 9,10 Later, other cell surface markers as well as the activity of the Wnt pathway have been used to isolate colon CSCs from tumors.12,13 Spheroid cultures have been established from human primary colorectal tumors that selectively enrich for the growth of colon CSCs,11,12 although it is important to realize that these spheres also contain more differentiated tumor cells.12 In agreement, we have shown that the Wnt activity reporter that directs the expression of enhanced green fluorescent protein (TOP-GFP) allows for the separation of CSCs from more differentiated progeny in the spheroid cultures. 12CSCs are suggested to be responsible for tumor recurrence after initial therapy, as they are considered to be selectively resistant to therapy.11,14 Conventional chemotherapy induces, among others, DNA damage and subsequent activation of the mito...

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Bcl-2, Bcl-xL, and Bcl-w are not equivalent targets of ABT-737 and navitoclax (ABT-263) in lymphoid and leukemic cells

Cited by 166 publications

References 50 publications

Elevated Mcl-1 inhibits thymocyte apoptosis and alters thymic selection

Elevated Mcl-1 inhibits thymocyte apoptosis and alters thymic selection

The BCL-2 protein family, BH3-mimetics and cancer therapy

Decreased mitochondrial priming determines chemoresistance of colon cancer stem cells

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