Literature DB >> 22355009

BRAF(V600) inhibitor GSK2118436 targeted inhibition of mutant BRAF in cancer patients does not impair overall immune competency.

David S Hong1, Luis Vence, Gerald Falchook, Laszlo G Radvanyi, Chengwen Liu, Vicki Goodman, Jeffery J Legos, Sam Blackman, Antonio Scarmadio, Razelle Kurzrock, Gregory Lizee, Patrick Hwu.   

Abstract

PURPOSE: An intact immune system likely contributes to the outcome of treatment and may be important for clearance of drug-resistant tumor cells and for prevention of recurrence. Although pharmacologic inhibition of BRAF(V600E) in melanoma patients, which is linked to immune suppression, results in an initial response rate, these responses are typically of limited duration. Combining immunotherapeutic drugs with kinase-targeted agents is an attractive strategy to increase clinical efficacy. Evidence suggesting that mitogen-activated protein kinase pathway activation in tumor cells contributes to immune suppression suggests that the two approaches may be synergistic, provided that BRAF(V600E) inhibitors are nontoxic to immune cells.
METHODS: To assess effects of mutant BRAF inhibition on systemic immunity, we studied 13 patients with tumors carrying a BRAF mutation who underwent treatment with GSK2118436, a V600 mutant BRAF-specific inhibitor. We carried out peripheral blood immunomonitoring before and following one or two 28-day cycles of treatment.
RESULTS: GSK2118436 treatment had no detectable impact on most immune parameters tested, including serum cytokine levels, peripheral blood cell counts, leukocyte subset frequencies, and memory CD4(+) and CD8(+) T-cell recall responses. A slight increase in serum TNF-α over the course of treatment was observed. In addition, three of the four human leukocyte antigen-A2-positive patients experienced a modest increase in circulating tumor antigen-specific CD8(+) T cells following BRAF(V600) inhibitor therapy.
CONCLUSIONS: GSK2118436 treatment results in no detectable negative impact on existing systemic immunity or the de novo generation of tumor-specific T cells. These findings suggest that future trials combining specific BRAF(V600E) inhibition with immunotherapy should not impair immune response. ©2012 AACR.

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Year:  2012        PMID: 22355009     DOI: 10.1158/1078-0432.CCR-11-2515

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  44 in total

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Review 2.  BRAF and MEK gene rearrangements in melanoma: implications for targeted therapy.

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3.  Differential influence of vemurafenib and dabrafenib on patients' lymphocytes despite similar clinical efficacy in melanoma.

Authors:  B Schilling; W Sondermann; F Zhao; K G Griewank; E Livingstone; A Sucker; H Zelba; B Weide; U Trefzer; T Wilhelm; C Loquai; C Berking; J Hassel; K C Kähler; J Utikal; P Al Ghazal; R Gutzmer; S M Goldinger; L Zimmer; A Paschen; U Hillen; D Schadendorf
Journal:  Ann Oncol       Date:  2014-02-06       Impact factor: 32.976

4.  CAR-T cells and combination therapies: What's next in the immunotherapy revolution?

Authors:  Maria C Ramello; Eric B Haura; Daniel Abate-Daga
Journal:  Pharmacol Res       Date:  2017-12-01       Impact factor: 7.658

5.  Paradoxical activation of T cells via augmented ERK signaling mediated by a RAF inhibitor.

Authors:  Taha Merghoub; Maria Jure-Kunkel; Jedd D Wolchok; Margaret K Callahan; Gregg Masters; Christine A Pratilas; Charlotte Ariyan; Jessica Katz; Shigehisa Kitano; Valerie Russell; Ruth Ann Gordon; Shachi Vyas; Jianda Yuan; Ashok Gupta; Jon M Wigginton; Neal Rosen
Journal:  Cancer Immunol Res       Date:  2014-01       Impact factor: 11.151

6.  Future perspectives in melanoma research: meeting report from the "Melanoma Bridge", Napoli, December 5th-8th 2013.

Authors:  Paolo A Ascierto; Antonio M Grimaldi; Ana Carrizosa Anderson; Carlo Bifulco; Alistair Cochran; Claus Garbe; Alexander M Eggermont; Mark Faries; Soldano Ferrone; Jeffrey E Gershenwald; Thomas F Gajewski; Ruth Halaban; F Stephen Hodi; Richard Kefford; John M Kirkwood; James Larkin; Sancy Leachman; Michele Maio; Richard Marais; Giuseppe Masucci; Ignacio Melero; Giuseppe Palmieri; Igor Puzanov; Antoni Ribas; Yvonne Saenger; Bastian Schilling; Barbara Seliger; David Stroncek; Ryan Sullivan; Alessandro Testori; Ena Wang; Gennaro Ciliberto; Nicola Mozzillo; Francesco M Marincola; Magdalena Thurin
Journal:  J Transl Med       Date:  2014-10-28       Impact factor: 5.531

7.  Identification and synthesis of N-(thiophen-2-yl) benzamide derivatives as BRAF(V600E) inhibitors.

Authors:  Yunfeng Xie; Xianjie Chen; Jie Qin; Xiangqian Kong; Fei Ye; Yuren Jiang; Hong Liu; Hualiang Jiang; Ronen Marmorstein; Cheng Luo
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8.  Converting biology into clinical benefit: lessons learned from BRAF inhibitors.

Authors:  Jennifer McQuade; Michael A Davies
Journal:  Melanoma Manag       Date:  2015

9.  BRAF inhibition increases tumor infiltration by T cells and enhances the antitumor activity of adoptive immunotherapy in mice.

Authors:  Chengwen Liu; Weiyi Peng; Chunyu Xu; Yanyan Lou; Minying Zhang; Jennifer A Wargo; Jie Qing Chen; Haiyan S Li; Stephanie S Watowich; Yan Yang; Dennie Tompers Frederick; Zachary A Cooper; Rina M Mbofung; Mayra Whittington; Keith T Flaherty; Scott E Woodman; Michael A Davies; Laszlo G Radvanyi; Willem W Overwijk; Gregory Lizée; Patrick Hwu
Journal:  Clin Cancer Res       Date:  2012-11-30       Impact factor: 12.531

Review 10.  Pathways and therapeutic targets in melanoma.

Authors:  Emma Shtivelman; Michael Q A Davies; Patrick Hwu; James Yang; Michal Lotem; Moshe Oren; Keith T Flaherty; David E Fisher
Journal:  Oncotarget       Date:  2014-04-15
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