Anti-apoptotic capacity of Mcl-1Δ127

The anti-apoptotic ability of Mcl-1Δ127, a caspase cleavage product of Mcl-1, is debated. We here used fluorescence imaging to assess the anti-apoptotic capacity of Mcl-1Δ127 in living cells. Fluorescence imaging of living cells expressing CFP-Mcl-1Δ127 showed that Mcl-1Δ127 existed mainly in cytopl...

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Veröffentlicht in:Biochemical and biophysical research communications 2020-06, Vol.526 (4), p.1042-1048
Hauptverfasser: Wang, Yong, Su, Wenhua, Mai, Zihao, Yu, Si, Wang, Xiaoping, Chen, Tongsheng
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Sprache:eng
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Zusammenfassung:The anti-apoptotic ability of Mcl-1Δ127, a caspase cleavage product of Mcl-1, is debated. We here used fluorescence imaging to assess the anti-apoptotic capacity of Mcl-1Δ127 in living cells. Fluorescence imaging of living cells expressing CFP-Mcl-1Δ127 showed that Mcl-1Δ127 existed mainly in cytoplasm. Fluorescence imaging of living cells co-expressing CFP-Mcl-1Δ127 and YFP-Bak, CFP-Mcl-1Δ127 and YFP-BimL, CFP-Mcl-1Δ127 and YFP-Puma or CFP-Mcl-1Δ127 and YFP-tBid showed that Mcl-1Δ127 markedly inhibited the oligomerization of Bak, BimL, Puma and tBid on mitochondria and also inhibited the Bak-, BimL-, Puma- or tBid-mediated cell death, resulting in their partial localization in cytoplasm. Fluorescence resonance energy transfer (FRET) imaging proved that Mcl-1Δ127 bound to Bak, BimL, Puma and tBid, respectively. Fluorescence loss in photobleaching (FLIP) analyses showed that Mcl-1Δ127 did prevent Bak oligomerization by retrotranslocating Bak from mitochondria into cytoplasm. Collectively, Mcl-1Δ127 has the same anti-apoptotic capacity as Mcl-1, and prevents apoptosis by sequestering BH3-only or Bak proteins, thus inhibiting their oligomerization on mitochondria. •Mcl-1Δ127 has the same anti-apoptotic capacity as Mcl-1.•Mcl-1Δ127 inhibits apoptosis by sequestering BH3-only and Bak proteins.•Mcl-1Δ127 inhibits mitochondrial Bak oligomerization.•Mcl-1Δ127 retrotranslocates Bak from mitochondria into cytosol.•Mcl-1Δ127 exists mainly in cytoplasm.
ISSN:0006-291X
1090-2104
DOI:10.1016/j.bbrc.2020.03.181