Resistance to BRAF Inhibition in BRAF-Mutant Colon Cancer Can Be Overcome with PI3K Inhibition or Demethylating Agents

Mao, Muling; Tian, Feng; Mariadason, John M.; Tsao, Chun C.; Lemos, Robert; Dayyani, Farshid; Gopal, Y.N. Vashisht; Jiang, Zhi Qin; Wistuba, Ignacio I.; Tang, Xi; Bornman, William G.; Bollag, Gideon; Mills, Gordon B.; Powis, Garth; Desai, Jayesh; Gallick, Gary E.; Davies, Michael A.; Kopetz, Scott

doi:10.1158/1078-0432.ccr-11-1446

Cited by 257 publications

(223 citation statements)

References 48 publications

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“…K-ras and BRAF mutations were linked with activation of AKT and ERK signaling pathway. [19][20][21][22][23][24] Therefore, the involvement of AKT and ERK activation in the increase of Bcl-2 expression can be expected in colorectal cancer. All cell lines used in this study harbored either K-ras mutation or BRAF mutation (Supplementary Figure 7a).…”

Section: Discussionmentioning

confidence: 99%

Bcl-2 stabilization by paxillin confers 5-fluorouracil resistance in colorectal cancer

Huang

Chang

et al. 2014

Cell Death Differ

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5-Fluorouracil (5-FU) is chemotherapeutic agent widely used for the treatment of colorectal cancer. Unfortunately, advanced colorectal cancer is often resistance to such chemotherapy and poor outcome. An adaptor protein paxillin (PXN) is phosphorylated at Y31/Y118 (pPXN-Y31/Y118) by Src contributes to cell mobility and Ser (S)272 of PXN in LD4 domain is important to the interaction between PXN and Bcl-2. We thus hypothesized that pPXN-Y31/Y118 may be required for Bcl-2 protein stability via PXN interacting with Bcl-2 to confer 5-FU resistance in colorectal cancer. Mechanistically, pPXN-S272 is phosphorylated through pPXN-Y31/Y118-mediated p21 protein-activated kinase 1 (PAK1) activation and pPXN-S272 is required for PXN to interact with Bcl-2. The interaction between PXN and Bcl-2 is essential for Bcl-2 protein stability through phosphorylation of Bcl-2 at S87 (pBcl-2-S87) by pPXN-Y31/ Y118-mediated ERK activation. An increase in Bcl-2 expression by PXN is responsible for resistance to 5-FU. The resistance to 5-FU can be abolished by inhibitor of Src and PAK1 or Bcl-2 antagonist in cell and animal models. Among patients, Bcl-2 expression is positively correlated with expression of PXN and pPXN-S272, respectively. Patients with high PXN/high Bcl-2 or high pPXN-S272/high Bcl-2 tumors are commonly to have an unfavorable response to 5-FU-based chemotherapy, compared with patients who have high PXN, high pPXN-S272 or high Bcl-2 tumors alone. Therefore, we suggest that Src, PAK1 or Bcl-2 inhibitor may potentially overcome the resistance of 5-FU-based chemotherapy and consequently to improve outcomes in patients with PXN/Bcl-2 and pPXN-S272/Bcl-2-positive tumors. Cell Death and Differentiation (2015) 22, 779-789; doi:10.1038/cdd.2014.170; published online 17 October 2014The incidence of colorectal cancer has markedly increased over the past two decades and became the third leading cancer death in Taiwan.1,2 Patients with colorectal cancer commonly receive 5-fluorouracil (5-FU)-based chemotherapy after surgical resection. 3 The 5-year survival of Dukes B patients is approximately 75%, indicating that~25% of Dukes B patients may potentially benefit from adjuvant chemotherapy. 4 However, the response rate of advancedstage patients to 5-FU-based chemotherapy was only 10-15%. 5 Therefore, there is an urgent need to establish therapeutic biomarkers and available clinical approaches to improve the response of colorectal patients who received 5-FU-based chemotherapy.Paxillin (PXN) has been shown to promote tumor aggressiveness, including that of colorectal cancer. 6 A recent report indicated that PXN may promote cell proliferation in SW480 colon cancer cells and PXN expression was associated with overall survival (OS) but not related with Bcl-2 in colorectal cancer patients. 7 Our previous report indicated that phosphorylation of PXN at Y31/Y118 (pPXN-Y31/Y118) by Src signaling pathway increased Bcl-2 expression at a transcriptional level in lung cancer cells via ERK activation.8 Surprisingly, our preliminary data showed that ...

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Section: Discussionmentioning

confidence: 99%

Bcl-2 stabilization by paxillin confers 5-fluorouracil resistance in colorectal cancer

Huang

Chang

et al. 2014

Cell Death Differ

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“…In vitro and in vivo xenograft models have shown that colorectal carcinoma that harbor BRAF V600E may be sensitive to proteasome inhibitors (14). Although colorectal carcinomas have very limited response to BRAF V600E inhibitor monotherapy (15,16), combinatorial strategies are currently under investigation to improve response, and outcome for these patients (17,18).…”

Section: Introductionmentioning

confidence: 99%

Assessment of BRAF V600E Status in Colorectal Carcinoma: Tissue-Specific Discordances between Immunohistochemistry and Sequencing

Estrella

Tetzlaff

Bassett

et al. 2015

Molecular Cancer Therapeutics

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Although sequencing provides the gold standard for identifying colorectal carcinoma with BRAF V600E mutation, immunohistochemistry (IHC) with the recently developed mouse monoclonal antibody VE1 for BRAF V600E protein has shown promise as a more widely available and rapid method. However, we identified anecdotal discordance between VE1 IHC and sequencing results and therefore analyzed VE1 staining by two different IHC methods (Leica Bond and Ventana BenchMark) in whole tissue sections from 480 colorectal carcinomas (323 BRAF wild-type, 142 BRAF V600E mutation, and 15 BRAF non-V600E mutation). We also compared the results with melanomas and papillary thyroid carcinomas (PTC). With the Bond method, among 142 BRAF V600E-mutated colorectal carcinomas, 77 (54%) had diffuse VE1 staining and 48 (33%) had heterogeneous staining, but 17 (12%) were negative. Among 323 BRAF wild-type colorectal carcinomas, 196 (61%) were negative, but 127 (39%) had staining, including 7 with diffuse staining. When positivity was defined as staining in !20% of tumor cells, VE1 IHC had sensitivity of 75% and specificity of 93% for BRAF V600E mutation. With the Ventana method, among 57 BRAF V600E-mutated colorectal carcinomas, 36 (63%) had diffuse VE1 staining, whereas 6 (11%) had no or weak (<20% of tumor cells) staining. Among 33 BRAF wildtype colorectal carcinomas, 16 (48%) had no or weak staining, whereas 15 (45%) had heterogeneous staining. In contrast with colorectal carcinoma, Bond and Ventana VE1 IHC in melanoma and PTC were highly concordant with sequencing results. We conclude that VE1 IHC produces suboptimal results in colorectal carcinoma and should not be used to guide patient management.

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“…Drugs available against other RAS-regulated signaling proteins, such as BRAF and MEK, have also shown moderate efficacy, although this is limited due to rapid development of acquired resistance, in many cases due to aberrant activation of parallel signaling pathways that in turn stimulate the PI3K pathway (8)(9)(10). Moreover, RAS itself has proved impossible to target effectively to date (11,12).…”

Section: Introductionmentioning

confidence: 99%

RAS interaction with PI3K p110α is required for tumor-induced angiogenesis

Murillo¹,

Zelenay²,

Nye³

et al. 2014

J. Clin. Invest.

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Resistance to BRAF Inhibition in BRAF-Mutant Colon Cancer Can Be Overcome with PI3K Inhibition or Demethylating Agents

Cited by 257 publications

References 48 publications

Bcl-2 stabilization by paxillin confers 5-fluorouracil resistance in colorectal cancer

Bcl-2 stabilization by paxillin confers 5-fluorouracil resistance in colorectal cancer

Assessment of BRAF V600E Status in Colorectal Carcinoma: Tissue-Specific Discordances between Immunohistochemistry and Sequencing

RAS interaction with PI3K p110α is required for tumor-induced angiogenesis

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