Expanding the landscape of oncogenic drivers and treatment options in acral and mucosal melanomas by targeted genomic profiling

被引:0
|
作者
Turner, Jacqueline A. [1 ]
Van Gulick, Robert J. [1 ,2 ]
Robinson, William A. [1 ,2 ]
Mughal, Tariq [3 ]
Tobin, Richard P. [2 ,4 ]
Macbeth, Morgan L. [1 ,2 ]
Holman, Blair [1 ,2 ]
Classon, Anthony [5 ]
Bagby, Stacey M. [1 ,2 ]
Yacob, Betelehem W. [1 ]
Hartman, Sarah J. [1 ]
Silverman, Ian [6 ,9 ]
Vorwald, Victoria M. [2 ,4 ]
Gorden, Nicholas [1 ]
Gonzalez, Rita [1 ]
Gay, Laurie M. [5 ]
Ali, Siraj M. [5 ]
Benson, Adam [5 ]
Miller, Vincent A. [5 ]
Ross, Jeffrey S. [5 ,7 ]
Pitts, Todd M. [1 ,2 ]
Rioth, Matthew J. [1 ,2 ,8 ]
Lewis, Karl D. [1 ,2 ]
Medina, Theresa [1 ,2 ]
Mccarter, Martin D. [2 ,4 ]
Gonzalez, Rene [1 ,2 ]
Couts, Kasey L. [1 ,2 ]
机构
[1] Univ Colorado, Div Med Oncol, Anschutz Med Campus, Aurora, CO USA
[2] Univ Colorado, Ctr Rare Melanomas, Dept Med, Anschutz Med Campus, Aurora, CO USA
[3] Tufts Univ, Div Hematol Oncol, Canc Ctr, Boston, MA USA
[4] Univ Colorado, Dept Surg, Anschutz Med Campus, Aurora, CO USA
[5] Fdn Med Inc, Cambridge, MA USA
[6] Ignyta Inc, San Diego, CA USA
[7] Upstate Med Univ, Dept Pathol, Syracuse, NY USA
[8] Univ Colorado, Dept Med, Div Biomed Informat & Personalized Med, Anschutz Med Campus, Aurora, CO USA
[9] Incyte Res Inst, Wilmington, DE USA
来源
INTERNATIONAL JOURNAL OF CANCER | 2024年 / 155卷 / 10期
关键词
acral; CRKL; dasatinib; fusions; melanoma; mucosal; MYC; NF2; LENTIGINOUS-MELANOMA; MUTATIONAL BURDEN; UVEAL MELANOMA; MEK INHIBITION; PAN-RAF; CANCER; BRAF; ABERRATIONS; SURVIVAL; FUSIONS;
D O I
10.1002/ijc.35087
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Despite advancements in treating cutaneous melanoma, patients with acral and mucosal (A/M) melanomas still have limited therapeutic options and poor prognoses. We analyzed 156 melanomas (101 cutaneous, 28 acral, and 27 mucosal) using the Foundation One cancer-gene specific clinical testing platform and identified new, potentially targetable genomic alterations (GAs) in specific anatomic sites of A/M melanomas. Using novel pre-clinical models of A/M melanoma, we demonstrate that several GAs and corresponding oncogenic pathways associated with cutaneous melanomas are similarly targetable in A/M melanomas. Other alterations, including MYC and CRKL amplifications, were unique to A/M melanomas and susceptible to indirect targeting using the BRD4 inhibitor JQ1 or Src/ABL inhibitor dasatinib, respectively. We further identified new, actionable A/M-specific alterations, including an inactivating NF2 fusion in a mucosal melanoma responsive to dasatinib in vivo. Our study highlights new molecular differences between cutaneous and A/M melanomas, and across different anatomic sites within A/M, which may change clinical testing and treatment paradigms for these rare melanomas.
引用
收藏
页码:1792 / 1807
页数:16
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