University of Illinois Urbana-Champaign

SGK196 controls stem cell fates by promoting the degradation of TGFβ family receptors

Tsang Mui Chung, Stephanie

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https://hdl.handle.net/2142/72931

Description

Title
SGK196 controls stem cell fates by promoting the degradation of TGFβ family receptors
Author(s)
Tsang Mui Chung, Stephanie
Issue Date
2015-01-21
Director of Research (if dissertation) or Advisor (if thesis)
Chen, Jie
Doctoral Committee Chair(s)
Belmont, Andrew S.
Committee Member(s)
  • Chen, Jie
  • Bolton, Eric
  • Henry, Jonathan
Department of Study
Cell & Developmental Biology
Discipline
Cell and Developmental Biology
Degree Granting Institution
University of Illinois at Urbana-Champaign
Degree Name
Ph.D.
Degree Level
Dissertation
Keyword(s)
  • SGK196
  • cell signaling
  • TGFβ family signaling pathway
  • transmembrane domain
  • human embryonic stem cells
  • cell fate
Abstract
Much remains to be understood regarding the molecular mechanisms controlling stem cell fate. Through studies in human pluripotent stem cells (hPSCs), I have identified SGK196, an atypical kinase of relatively unknown function, as a novel regulator of cell fate and the TGFβ family signaling pathway. SGK196 depletion in human embryonic stem cells (hESCs) inhibits neural induction and enhances mesoderm induction, while SGK196 overexpression represses mesoderm and endoderm induction. SGK196 negatively regulates TGFβ family signaling by interacting with and promoting the degradation of TGFβ family receptors. Interactions were observed to occur within the SGK196 transmembrane (TM) domain. Mutation of specific Asn, Asp, and His residues in the SGK196 TM domain resulted in the diminished degradation of TGFβ family receptors and reduced interactions with the type I BMP receptor (BMPR1B), suggesting that these polar residues may play a key role in arbitrating SGK196 activity. The functional effects of Sgk196 in Xenopus laevis animal caps and embryos are in agreement with the results in hESCs. Defects in Sgk196 depleted Xenopus embryos include impaired development of neural tissues and increased development of mesodermal tissues. Overall, I demonstrate that SGK196 is an essential regulator of stem cell fate determination and early development. Through uncovering the regulatory mechanism of SGK196 I unveil valuable insight into receptor-level regulation of the TGFβ family pathway.
Graduation Semester
2014-12
Permalink
http://hdl.handle.net/2142/72931
Copyright and License Information
Copyright 2014 Stephanie Tsang Mui Chung

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