Your search keyword '"Lin, Su-Chang"' showing total 4 results

1. The versatile roles of CARDs in regulating apoptosis, inflammation, and NF-κB signaling

Author

Kao, Wen-Pin, primary, Yang, Chao-Yu, additional, Su, Tsung-Wei, additional, Wang, Yin-Ting, additional, Lo, Yu-Chih, additional, and Lin, Su-Chang, additional

Published

2014

2. Tandem DEDs and CARDs suggest novel mechanisms of signaling complex assembly

Author

Lo, Yu-Chih, primary, Lin, Su-Chang, additional, Yang, Chao-Yu, additional, and Tung, Jung-Yu, additional

Published

2014

3. Tandem DEDs and CARDs suggest novel mechanisms of signaling complex assembly.

Author

Lo, Yu-Chih, Lin, Su-Chang, Yang, Chao-Yu, and Tung, Jung-Yu

Abstract

Apoptosis is an important process to maintain cellular homeostasis. Deregulated apoptosis has linked to a number of diseases, such as inflammatory diseases, neurodegenerative disorder, and cancers. A major signaling complex in the death receptor signaling pathway leading to apoptosis is death-induced signaling complex (DISC), which is regulated mainly by death effector domain (DED)-containing proteins. There are seven DED-containing proteins in human, including FADD, c-FLIP, caspase-8, caspase-10, DEDD, DEDD2, and PEA-15. The main players in DISC formation employ tandem DEDs for regulating signaling complex formation. The regulatory mechanism of signaling complex formation is important and yet remains unclear. Interestingly, three caspase recruitment domain (CARD)-containing members, which belong to the same DD superfamily as DED-containing proteins, also contains similar tandem CARDs. Recent structural studies have shown that tandem CARDs are essential for the formation of a helical signaling complex. This review summarizes recent structural studies on DED-containing proteins and especially discusses the studies on tandem DEDs and tandem CARDs, which suggest new mechanisms of signaling complex assembly. [ABSTRACT FROM AUTHOR]

Published

2015

4. The versatile roles of CARDs in regulating apoptosis, inflammation, and NF-κB signaling.

Author

Kao, Wen-Pin, Yang, Chao-Yu, Su, Tsung-Wei, Wang, Yin-Ting, Lo, Yu-Chih, and Lin, Su-Chang

Abstract

CARD subfamily is the second largest subfamily in the DD superfamily that plays important roles in regulating various signaling pathways, including but not limited to NF-kB activation signaling, apoptosis signaling and inflammatory signaling. The CARD subfamily contains 33 human CARD-containing proteins, regulating the assembly of many signaling complexes, including apoptosome, inflammsome, nodosome, the CBM complex, PIDDosome, the TRAF2 complex, and the MAVS signalosome, by homotypic CARD-CARD interactions. The mechanism of how CARDs find the right binding partner to form a specific complex remains unclear. This review uses different classification schemes to update the classification of CARD-containing proteins. Combining the classification based on domain structures, functions, associated signaling complexes, and roles would help better understand the structural and function diversity of CARD-containing proteins. This review also summarizes recent structural studies on CARDs. Especially, the CARD-containing complexes can be divided into the homodimeric, heterodimeric, oligomeric, filamentous CARD complexes and the CARD-ubiquitin complex. This review will give an overview of the versatile roles of CARDs in regulating signaling transduction, as well as the therapeutic drugs targeting CARD-containing proteins. [ABSTRACT FROM AUTHOR]

Published

2015