Actinomycin D Targets NPM1c-Primed Mitochondria to Restore PML-Driven Senescence in AML Therapy.

Sylvie Rimsky,Jennifer J Trowbridge,Olivier Espéli ,Emmanuelle Clappier,Lionel Adès ,Rita Hleihel,Raphaël Itzykson ,Lorenzo Brunetti,Tak W Mak,Chengchen Wu,Lidio Conte,Takashi Sakamoto,Brunangelo Falini,Claudia Morganti,Paule Bénit,Emmanuel Raffoux,Jean Soulier,Sylvère Durand,Hiba El Hajj,Pierre Rustin,Shirine Benhenda,Hsin-Chieh Wu,Christine Berthier ,Hervé Dombret,Guido Kroemer,Sylvie Souquère ,Stéphanie Gachet,Hugues De Thé,Maria Paola Martelli,Samuel Quentin,Pierre Fenaux,Valérie Lallemand-Breitenbach,Ali Bazarbachi,Keisuke Ito,Domitille Rérolle,Marie Sébert

doi:10.1158/2159-8290.cd-21-0177

Actinomycin D Targets NPM1c-Primed Mitochondria to Restore PML-Driven Senescence in AML Therapy.

Sylvie Rimsky, Jennifer J Trowbridge + Show 34 more

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https://doi.org/10.1158/2159-8290.cd-21-0177

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#PML NBs #PML NB + Show 3 more

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Abstract

ActD induces complete remissions in NPM1-mutant AMLs. We found that NPM1c affects mitochondrial biogenesis and PML NBs. ActD targets mitochondria, yielding ROS which enforce PML NB biogenesis and restore senescence. Dual targeting of mitochondria with ActD and venetoclax sharply potentiates their anti-AML activities in vivo. This article is highlighted in the In This Issue feature, p. 2945.

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