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André Patrick Arrigo

Researcher at Claude Bernard University Lyon 1

Publications -  9
Citations -  1116

André Patrick Arrigo is an academic researcher from Claude Bernard University Lyon 1. The author has contributed to research in topics: Heat shock protein & Cellular differentiation. The author has an hindex of 8, co-authored 9 publications receiving 1073 citations.

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Journal ArticleDOI

HSP27 inhibits cytochrome c-dependent activation of procaspase-9

TL;DR: It is demonstrated that HSP27 overexpression decreases U937 human leukemic cell sensitivity to etoposide‐induced cytotoxicity by preventing apoptosis, and also prevents procaspase‐9 activation.
Journal ArticleDOI

Heat shock proteins and heat shock factor 1 in carcinogenesis and tumor development: an update

TL;DR: The extensive work that has been carried out and is still in progress aimed at understanding the oncogenic mechanisms by which HSP genes are switched on, determining the roles of HSF 1/HSP in malignant transformation and discovering approaches to therapy based on disrupting the influence of the HSF1-controlled transcriptome in cancer are reviewed.
Journal ArticleDOI

In search of the molecular mechanism by which small stress proteins counteract apoptosis during cellular differentiation.

TL;DR: The fact that these proteins are induced independently of the signal that triggers differentiation, of the differentiation type, and of the cell type strongly suggests their involvement in fundamental mechanisms of cellular differentiation.
Book ChapterDOI

Expression of heat shock proteins during development in Drosophila.

TL;DR: The Hsps may play at least two roles, one as housekeeping proteins during development and/or differentiation and the second one in restoring cellular functions after environmental stress.
Journal ArticleDOI

Heat shock protein is a unique marker of growth arrest during macrophage differentiation of HL-60 cells

TL;DR: Observations implicate hsp28 as an intermediary in the myelomonocytic differentiative pathway of promyelocytic leukemic cells, and will shed light on the events regulating this process.