Apoptosis: Reprogramming and the Fate of Mature Cells | Zendy

HoiHung Cheung | Zendy; Xiaozhuo Liu | Zendy; Owen M. Rennert | Zendy

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Apoptosis: Reprogramming and the Fate of Mature Cells

Author(s) -

HoiHung Cheung,

Xiaozhuo Liu,

Owen M. Rennert

Publication year - 2012

Publication title -

isrn cell biology

Language(s) - English

Resource type - Journals

eISSN - 2090-7389

pISSN - 2090-7370

DOI - 10.5402/2012/685852

Subject(s) - reprogramming , microbiology and biotechnology , embryonic stem cell , induced pluripotent stem cell , biology , stem cell , somatic cell , apoptosis , cellular differentiation , cell fate determination , cell , genetics , transcription factor , gene

Apoptosis is essential for embryogenesis, organ metamorphosis, and tissue homeostasis. In embryonic stem cells, self-renewal is balanced with proliferative potential, inhibition of differentiation, and prevention of senescence and apoptosis. Growing evidence supports the role of apoptosis in self-renewal, differentiation of pluripotent stem cells, and dedifferentiation (reprogramming) of somatic cells. In this paper we discuss the multiple roles of apoptosis in embryonic stem cells (ESCs) and reprogramming of differentiated cells to pluripotency. The role of caspases and p53 as key effectors in controlling the generation of iPSC is emphasized. Remarkably, the complication of apoptosis arising during reprogramming may provide insights into technical improvements for derivation of iPSC from senescent cells as a tool for modeling aging-related diseases.

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