Proteomics

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Proteome analysis of GCN1 CKO mouse duodenum


ABSTRACT: Tamoxifen-inducible conditional knockout (CKO) mice were generated to explore the function of Gcn1 in adult mice using the Cre/loxP system. To analyze the function of GCN1 in the intestinal epithelium, we compared the whole cell proteome of duodenum harvested from GCN1 CKO mice with that of wild-type mice.

ORGANISM(S): Mus Musculus (mouse)

SUBMITTER: Ken Itoh 

PROVIDER: PXD030517 | JPOST Repository | Sun Mar 31 00:00:00 GMT 2024

REPOSITORIES: jPOST

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Publications

Inducible Systemic <i>Gcn1</i> Deletion in Mice Leads to Transient Body Weight Loss upon Tamoxifen Treatment Associated with Decrease of Fat and Liver Glycogen Storage.

Liu Jun J   Kasai Shuya S   Tatara Yota Y   Yamazaki Hiromi H   Mimura Junsei J   Mizuno Seiya S   Sugiyama Fumihiro F   Takahashi Satoru S   Sato Tsubasa T   Ozaki Taku T   Tanji Kunikazu K   Wakabayashi Koichi K   Maeda Hayato H   Mizukami Hiroki H   Shinkai Yasuhiro Y   Kumagai Yoshito Y   Tomita Hirofumi H   Itoh Ken K  

International journal of molecular sciences 20220316 6


GCN1 is an evolutionarily-conserved ribosome-binding protein that mediates the amino acid starvation response as well as the ribotoxic stress response. We previously demonstrated that <i>Gcn1</i> mutant mice lacking the GCN2-binding domain suffer from growth retardation and postnatal lethality via GCN2-independent mechanisms, while <i>Gcn1</i>-null mice die early in embryonic development. In this study, we explored the role of GCN1 in adult mice by generating tamoxifen-inducible conditional knoc  ...[more]

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