Bid chimeras indicate that most BH3-only proteins can directly activate Bak and Bax, and show no preference for Bak versus Bax

Hockings, Colin; Anwari, Khatira; Ninnis, Robert L; Brouwer, J.M.; O’Hely, Martin; Evangelista, Marco; Hinds, Mark G.; Czabotar, P.E.; Lee, Erinna F.; Fairlie, W. Douglas; Dewson, Grant; Kluck, Ruth M.

doi:10.1038/cddis.2015.105

Cited by 78 publications

(120 citation statements)

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“…In Jurkat and SKW6.4 cells, the tolerance for BIK, BMF or NOXA is similar to that of BIM EL or PUMA (Figures 3k and l), consistent with claims that BIK, BMF and NOXA might also be direct activators in at least some contexts. 2,20,23,52 In contrast, the tolerance for BAD is much higher than the tolerance for BIM and PUMA in all cell lines examined (Figures 3k, 3l, 5b and c). This difference between BAD and the other BH3-only proteins was particularly evident in cells with relatively low expression of BCL2 and BCLX L (Figures 3k and l).…”

Section: Discussionmentioning

confidence: 83%

“…15,16 Upon activation, the proapoptotic family members BAK and BAX can breach the mitochondrial outer membrane (MOM), leading to cytochrome c release, caspase 9 activation and subsequent apoptotic events. Genetic 2,17 as well as biochemical experiments [18][19][20][21][22][23] have indicated that the BH3-only proteins BIM, PUMA, a protease generated BID fragment (tBID), and, in some studies, NOXA can directly bind and activate BAK and/or BAX. To counteract these effects, antiapoptotic BCL2 family members such as BCL2, BCLX L and MCL1 bind and neutralize activated BAX and/or BAK 2,6,16,24 as well as activated or overexpressed BH3-only family members, [25][26][27][28][29][30] thereby preserving MOM integrity.…”

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confidence: 99%

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Measurement of BH3-only protein tolerance

et al. 2017

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The BCL2 family of proteins regulates cellular life and death decisions. Among BCL2 family members, BH3-only proteins have critical roles by neutralizing antiapoptotic family members, as well as directly activating BAX and BAK. Despite widespread occurrence of BH3-only protein upregulation in response to various stresses, this process is rarely quantified. Moreover, it is unclear whether all BH3-only proteins are equipotent at inducing cell death. Here we show that BH3-only proteins increase as much as 15-to 20-fold after various treatments and define a parameter, termed BH3-only tolerance, which measures how many copies of a particular BH3-only protein can be expressed before the majority of cells in a population undergo apoptosis. We not only assess the relative contributions of anti-and proapoptotic BCL2 family members to BH3-only tolerance, but also illustrate how the study of this parameter can be used to understand cellular sensitivity to anticancer drugs and new combinations. These observations provide a new quantitative framework for assessing apoptotic susceptibility under various conditions.

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Section: Discussionmentioning

confidence: 83%

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Measurement of BH3-only protein tolerance

et al. 2017

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“…WT cBID (which lacks cysteine in the activating p15 fragment) and cBID I83C and R84C variants were incubated with cytosolic extracts from cells stably expressing BAK/BAXCS with cysteines engineered in either the groove (H99C or K113C) or α6 (R156C, D160C, or H164C). Disulphide linkage was induced with oxidant [copper (II) (1,10-phenanthroline) 3 , CuPhe] and assessed on nonreducing SDS/PAGE following coimmunoprecipitation. Disulphide-linked cBID:BAK heterodimers were evident between the cBID R84C variant with cysteine at H99 in the BAK groove ( Fig.…”

Section: Bak Conformation Change Destabilizes the Cbid:bak Interactiomentioning

confidence: 99%

“…They are activated by interaction with BCL-2 homology 3 (BH3)-only proteins including BID and BIM (3). Structures show that peptides based on the BH3 domains of activator BH3-only proteins can bind directly to BAK and BAX via a hydrophobic groove (comprising α-helices 2-5) that is also shared with their prosurvival homologs (4)(5)(6)(7)(8).…”

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confidence: 99%

BAK α6 permits activation by BH3-only proteins and homooligomerization via the canonical hydrophobic groove

Tan

Stephen

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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BAK and BAX are the essential effectors of apoptosis because without them a cell is resistant to most apoptotic stimuli. BAK and BAX undergo conformation changes to homooligomerize then permeabilize the mitochondrial outer membrane during apoptosis. How BCL-2 homology 3 (BH3)-only proteins bind to activate BAK and BAX is unclear. We report that BH3-only proteins bind inactive full-length BAK at mitochondria and then dissociate following exposure of the BAK BH3 and BH4 domains before BAK homodimerization. Using a functional obstructive labeling approach, we show that activation of BAK involves important interactions of BH3-only proteins with both the canonical hydrophobic binding groove (α2-5) and α6 at the rear of BAK, with interaction at α6 promoting an open groove to receive a BH3-only protein. Once activated, how BAK homodimers multimerize to form the putative apoptotic pore is unknown. Obstructive labeling of BAK beyond the BH3 domain and hydrophobic groove did not inhibit multimerization and mitochondrial damage, indicating that critical protein-protein interfaces in BAK self-association are limited to the α2-5 homodimerization domain.AK and BAX are the pivotal effectors of intrinsic apoptosis, with one or the other being required for mitochondrial damage and cell death (1, 2). They are activated by interaction with BCL-2 homology 3 (BH3)-only proteins including BID and BIM (3). Structures show that peptides based on the BH3 domains of activator BH3-only proteins can bind directly to BAK and BAX via a hydrophobic groove (comprising α-helices 2-5) that is also shared with their prosurvival homologs (4-8). BAX has been proposed to have an additional activation site, distinct from the hydrophobic groove, at the rear of the molecule comprising α-helices 1 and 6 (9). Binding of stapled BH3 peptides at this site induced the dissociation of the BAX C-terminal transmembrane domain from the hydrophobic groove to facilitate mitochondrial localization (10, 11). Interaction of BH3-only proteins at this noncanonical site is not thought to be necessary for BAK activity because BAK is constitutively anchored in the mitochondrial outer membrane (MOM) via its transmembrane domain (12). However, recent reports that both BAX (13, 14) and BAK (15) are constantly "retrotranslocated" from the mitochondria to the cytosol suggest conserved mechanisms of activation for BAK and BAX.Characterizing the interaction of BH3-only proteins with fulllength BAK at mitochondria has proven difficult because the bound BH3-only protein dissociates during consequent BAK conformation changes, including exposure of the N-terminus (amino terminus) and and dissociation of their α2-5 helices ("core") from their α6-8 helices ("latch") (6, 7) to facilitate selfassociation. Additionally, structural studies have been largely confined to truncated protein or peptides in the absence of a membrane where interactions between BH3-only proteins and BAK occur.Once activated BAK and BAX self-associate to form pores that damage the MOM to release cytochrome c and...

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“…Addition of substoichiometric amounts of a "direct activator" BH3-only protein or BH3 peptide induces potent BAX activation, including membrane insertion, oligomerization, and membrane permeabilization, blocked effectively by BCL-X and the like (Kuwana et al 2005;Lovell et al 2008). However, over the years, the list of BH3-only proteins with "direct activator" potential became increasingly long (adding PUMA, BMF, and NOXA, leaving only BAD, BIK, and HRK as "sensitizers" behind), suggesting that experimental design can strongly impact BH3 peptide or BH3-only protein-mediated BAX/ BAK activation or MOMP in in vitro assays (Hockings et al 2015).…”

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confidence: 99%

MOMP in the absence of BH3-only proteins

Saez

Villunger

2016

Genes Dev.

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The minimum requirement for mitochondrial apoptosis has been controversial ever since the discovery of BCL-2 as a cell death regulator. In this issue of Genes & Development, O'Neill and colleagues (pp. 973–988) end a long-standing debate by creating a cellular system free of BCL-2 family proteins, thereby identifying the outer mitochondrial membrane rather than BH3-only proteins as the only requirement for BAX/BAK activation and mitochondrial outer membrane permeabilization (MOMP).

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Bid chimeras indicate that most BH3-only proteins can directly activate Bak and Bax, and show no preference for Bak versus Bax

Cited by 78 publications

References 57 publications

Measurement of BH3-only protein tolerance

Measurement of BH3-only protein tolerance

BAK α6 permits activation by BH3-only proteins and homooligomerization via the canonical hydrophobic groove

MOMP in the absence of BH3-only proteins

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