[HTML][HTML] A different pathway in the endoplasmic reticulum stress-induced expression of human HRD1 and SEL1 genes
M Kaneko, S Yasui, Y Niinuma, K Arai, T Omura… - Febs letters, 2007 - Elsevier
M Kaneko, S Yasui, Y Niinuma, K Arai, T Omura, Y Okuma, Y Nomura
Febs letters, 2007•ElsevierHuman HRD1 and SEL1 are components of endoplasmic reticulum-associated degradation
(ERAD), which is a retrograde transport mechanism from the ER to the cytosol for removing
unfolded proteins. The expression of HRD1 and SEL1 was induced by ER stress-inducing
agents and overexpression of both ER stress-responsive transcription factors, ATF6 and
XBP1. Inhibition of IRE1 and ATF6 revealed that ER stress-induced HRD1 and SEL1
expressions are mediated by IRE1-XBP1-and ATF6-dependent pathways, respectively …
(ERAD), which is a retrograde transport mechanism from the ER to the cytosol for removing
unfolded proteins. The expression of HRD1 and SEL1 was induced by ER stress-inducing
agents and overexpression of both ER stress-responsive transcription factors, ATF6 and
XBP1. Inhibition of IRE1 and ATF6 revealed that ER stress-induced HRD1 and SEL1
expressions are mediated by IRE1-XBP1-and ATF6-dependent pathways, respectively …
Human HRD1 and SEL1 are components of endoplasmic reticulum-associated degradation (ERAD), which is a retrograde transport mechanism from the ER to the cytosol for removing unfolded proteins. The expression of HRD1 and SEL1 was induced by ER stress-inducing agents and overexpression of both ER stress-responsive transcription factors, ATF6 and XBP1. Inhibition of IRE1 and ATF6 revealed that ER stress-induced HRD1 and SEL1 expressions are mediated by IRE1-XBP1- and ATF6-dependent pathways, respectively. These results suggest that the ER stress-induced ERAD gene expressions are mediated by different pathways, which are attributed to the differences in the promoter regions.
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