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Autophagy driven by a master regulator of hematopoiesis.

Molecular and cellular biology (2011-10-26)
Yoon-A Kang, Rajendran Sanalkumar, Henriette O'Geen, Amelia K Linnemann, Chan-Jung Chang, Eric E Bouhassira, Peggy J Farnham, Sunduz Keles, Emery H Bresnick
RESUMEN

Developmental and homeostatic remodeling of cellular organelles is mediated by a complex process termed autophagy. The cohort of proteins that constitute the autophagy machinery functions in a multistep biochemical pathway. Though components of the autophagy machinery are broadly expressed, autophagy can occur in specialized cellular contexts, and mechanisms underlying cell-type-specific autophagy are poorly understood. We demonstrate that the master regulator of hematopoiesis, GATA-1, directly activates transcription of genes encoding the essential autophagy component microtubule-associated protein 1 light chain 3B (LC3B) and its homologs (MAP1LC3A, GABARAP, GABARAPL1, and GATE-16). In addition, GATA-1 directly activates genes involved in the biogenesis/function of lysosomes, which mediate autophagic protein turnover. We demonstrate that GATA-1 utilizes the forkhead protein FoxO3 to activate select autophagy genes. GATA-1-dependent LC3B induction is tightly coupled to accumulation of the active form of LC3B and autophagosomes, which mediate mitochondrial clearance as a critical step in erythropoiesis. These results illustrate a novel mechanism by which a master regulator of development establishes a genetic network to instigate cell-type-specific autophagy.

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Imprint® Ultra Chromatin Immunoprecipitation Kit, Without Controls, ChIP kit for maximum sensitivity, compatible with Next-Gen sequencing
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ChIP Next Gen Seq Sepharose
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Imprint® Ultra Chromatin Optimization Kit, Kit designed to optimize sonication parameters for ChIP experiments