Increased expression of cFLIPL in colonic adenocarcinoma

Ryu, Byeol; Lee, Min Goo; Gil, Sung; Kim, Youn Wha; Park, Jae Hoon

doi:10.1002/path.835

Cited by 122 publications

(110 citation statements)

References 22 publications

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“…These data indicate that thymocytes and T cells respond in type I mode, whereas hepatocytes and pancreatic b cells behave in type II manner vis-a-vis Fas signaling. Further evidence supports the existence of similar type I versus II mechanisms in Apo2L/TRAIL signaling as well (Figure 2 (Ryu et al, 2001), pancreatic carcinoma (Elnemr et al, 2001), malignant melanoma (Irmler et al, 1997) and Burkitt's lymphoma (Tepper and Seldin, 1999). Another potential determinant is XIAP.…”

Section: Apoptosis Signaling By Apo2l/trailsupporting

confidence: 56%

New insights into apoptosis signaling by Apo2L/TRAIL

2010

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Section: Apoptosis Signaling By Apo2l/trailsupporting

confidence: 56%

New insights into apoptosis signaling by Apo2L/TRAIL

2010

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“…It is possible that the relatively high levels of c-FLIP S in the two c-FLIP S -overexpressing cell lines (in particular HFS44) may be superphysiological and promote DISC-independent clustering and activation of caspase 8. In contrast, the levels of c-FLIP L overexpression in the HFL17 and HFL24 cell lines (B4-fold) are similar to the levels of overexpression observed by Ryu et al (2001) in colonic tumours. The different effects of overexpressing each splice form may be due to c-FLIP L being a more potent inhibitor of death receptor-mediated apoptosis (Irmler et al, 1997).…”

Section: Discussionmentioning

confidence: 49%

“…Our findings indicate that overexpression of c-FLIP L inhibits apoptosis of CRC cells in response to the chemotherapeutic agents used in the treatment of CRC. This has particular clinical relevance given the high incidence of c-FLIP L overexpression observed in colon cancer (Ryu et al, 2001). Interestingly, c-FLIP S overexpression failed to protect CRC cells from 5-FU-and OXA-induced apoptosis, and only moderately protected against CPT-11-induced apoptosis.…”

Section: Discussionmentioning

confidence: 96%

“…Furthermore, clinical studies have demonstrated significantly elevated c-FLIP expression in colorectal and gastric tumours (Ryu et al, 2001;Zhou et al, 2004), suggesting that c-FLIP may be a relevant clinical target not only in CRC but also in gastric cancer, where 5-FU-based chemotherapy regimens are also used. Moreover, our data suggest that c-FT therapeutic strategies may be effective against colorectal tumours irrespective of p53 mutational status.…”

Section: Discussionmentioning

confidence: 99%

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c-FLIP inhibits chemotherapy-induced colorectal cancer cell death

et al. 2005

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c-FLIP inhibits caspase 8 activation and apoptosis mediated by death receptors such as Fas and DR5. We studied the effect of c-FLIP on the apoptotic response to chemotherapies used in colorectal cancer (CRC) (5-fluorouracil, oxaliplatin and irinotecan). Simultaneous downregulation of both c-FLIP splice forms c-FLIP L and c-FLIP S with siRNA synergistically enhanced chemotherapy-induced apoptosis in p53 wild-type (HCT116p53 þ / þ , RKO), null (HCT116p53 À/À ) and mutant (H630) CRC cell lines. Furthermore, overexpression of c-FLIP L , but not c-FLIP S , potently inhibited apoptosis induced by chemotherapy in HCT116p53 þ / þ cells, suggesting that c-FLIP L was the more important splice form in mediating chemoresistance. In support of this, siRNA specifically targeted against c-FLIP L synergistically enhanced chemotherapy-induced apoptosis in a manner similar to the siRNA targeted against both splice forms. Inhibition of caspase 8 blocked the enhanced apoptosis induced by c-FLIP-targeted (FT) siRNA and chemotherapy. Furthermore, we found that downregulating cell surface DR5, but not Fas, also inhibited apoptosis induced by FT siRNA and chemotherapy. Interestingly, these effects were not dependent on activation of DR5 by its ligand TRAIL. These results indicate that c-FLIP inhibits TRAILindependent, DR5-and caspase 8-dependent apoptosis in response to chemotherapy in CRC cells. Moreover, targeting c-FLIP in combination with existing chemotherapies may have therapeutic potential for the treatment of CRC.

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“…FLIP has been found to be overexpressed in many human cancers (Ryu et al, 2001;Zhou et al, 2004;Valnet-Rabier et al, 2005), and has emerged through our work and that of others, as a potential anti-cancer drug target (Hyer et al, 2005;Wilson et al, 2007). Furthermore, XIAP has been found to be overexpressed in several cancers, and small molecule and antisense approaches to target XIAP are in development (Hu et al, 2003;LaCasse et al, 2006).…”

Section: Discussionmentioning

confidence: 72%

Combined inhibition of FLIP and XIAP induces Bax-independent apoptosis in type II colorectal cancer cells

et al. 2008

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Death receptors can directly (type I cells) or indirectly induce apoptosis by activating mitochondrial-regulated apoptosis (type II cells). The level of caspase 8 activation is thought to determine whether a cell is type I or II, with type II cells less efficient at activating this caspase following death receptor activation. FLICE-inhibitory protein (FLIP) blocks death receptor-mediated apoptosis by inhibiting caspase 8 activation; therefore, we assessed whether silencing FLIP could convert type II cells into type I. FLIP silencing-induced caspase 8 activation in Bax wild-type and null HCT116 colorectal cancer cells; however, complete caspase 3 processing and apoptosis were only observed in Bax wild-type cells. Bax-null cells were also more resistant to chemotherapy and tumor necrosis factor-related apoptosis inducing ligand and, unlike the Bax wild-type cells, were not sensitized to these agents by FLIP silencing. Further analyses indicated that release of second mitochondrial activator of caspases from mitochondria and subsequent inhibition of X-linked inhibitor of apoptosis protein (XIAP) was required to induce full caspase 3 processing and apoptosis following FLIP silencing. These results indicate that silencing FLIP does not necessarily bypass the requirement for mitochondrial involvement in type II cells. Furthermore, targeting FLIP and XIAP may represent a therapeutic strategy for the treatment of colorectal tumors with defects in mitochondrial-regulated apoptosis.

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Increased expression of cFLIPL in colonic adenocarcinoma

Cited by 122 publications

References 22 publications

New insights into apoptosis signaling by Apo2L/TRAIL

New insights into apoptosis signaling by Apo2L/TRAIL

c-FLIP inhibits chemotherapy-induced colorectal cancer cell death

Combined inhibition of FLIP and XIAP induces Bax-independent apoptosis in type II colorectal cancer cells

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