ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization

SIMPLE SUMMARY: NRAS-mutant melanoma is a highly aggressive subtype with few treatment options. Although both BRAF-mutant and NRAS-mutant melanomas have activation of the MEK/ERK pathway, MEK inhibitors (MEKi) are only effective for the BRAF-mutant subtype. The aim of this study was to understand wh...

Descripción completa

Detalles Bibliográficos
Autores principales: Lyon, Anastasia, Tripathi, Rakshamani, Meeks, Christina, He, Daheng, Wu, Yuanyuan, Liu, Jinpeng, Wang, Chi, Chen, Jing, Zhu, Haining, Mukherjee, Sujata, Ganguly, Saptadwipa, Plattner, Rina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9913232/
https://www.ncbi.nlm.nih.gov/pubmed/36765910
http://dx.doi.org/10.3390/cancers15030954
_version_ 1784885374687903744
author Lyon, Anastasia
Tripathi, Rakshamani
Meeks, Christina
He, Daheng
Wu, Yuanyuan
Liu, Jinpeng
Wang, Chi
Chen, Jing
Zhu, Haining
Mukherjee, Sujata
Ganguly, Saptadwipa
Plattner, Rina
author_facet Lyon, Anastasia
Tripathi, Rakshamani
Meeks, Christina
He, Daheng
Wu, Yuanyuan
Liu, Jinpeng
Wang, Chi
Chen, Jing
Zhu, Haining
Mukherjee, Sujata
Ganguly, Saptadwipa
Plattner, Rina
author_sort Lyon, Anastasia
collection PubMed
description SIMPLE SUMMARY: NRAS-mutant melanoma is a highly aggressive subtype with few treatment options. Although both BRAF-mutant and NRAS-mutant melanomas have activation of the MEK/ERK pathway, MEK inhibitors (MEKi) are only effective for the BRAF-mutant subtype. The aim of this study was to understand why MEKi are ineffective in NRAS-mutant melanomas with the long-term goal of identifying new treatment regimens. Here, we show that ABL and DDR kinases are critically important for MEKi resistance because they cooperate to promote the stability of key proteins involved in driving melanoma growth and survival. FDA-approved drugs that inhibit ABL1/2 and DDR1 have been used for decades to treat leukemia. We showed that one such inhibitor prevents MEKi resistance from developing in a NRAS-mutant melanoma animal model. Thus, the data in this study provide the rationale for testing the use of drugs targeting ABL1/2 and DDR1 in combination with MEKi for patients with NRAS-mutant melanomas who have failed to respond to immunotherapy. ABSTRACT: Melanomas harboring NRAS mutations are a particularly aggressive and deadly subtype. If patients cannot tolerate or the melanomas are insensitive to immune checkpoint blockade, there are no effective 2nd-line treatment options. Drugs targeting the RAF/MEK/ERK pathway, which are used for BRAF-mutant melanomas, do little to increase progression-free survival (PFS). Here, using both loss-of-function and gain-of-function approaches, we show that ABL1/2 and DDR1 are critical nodes during NRAS-mutant melanoma intrinsic and acquired MEK inhibitor (MEKi) resistance. In some acquired resistance cells, ABL1/2 and DDR1 cooperate to stabilize RAF proteins, activate ERK cytoplasmic and nuclear signaling, repress p27/KIP1 expression, and drive RAF homodimerization. In contrast, other acquired resistance cells depend solely on ABL1/2 for their survival, and are sensitive to highly specific allosteric ABL1/2 inhibitors, which prevent β-catenin nuclear localization and destabilize MYC and ETS1 in an ERK-independent manner. Significantly, targeting ABL1/2 and DDR1 with an FDA-approved anti-leukemic drug, reverses intrinsic MEKi resistance, delays acquisition of acquired resistance, and doubles the survival time in a NRAS-mutant mouse model. These data indicate that repurposing FDA-approved drugs targeting ABL1/2 and DDR1 may be a novel and effective strategy for treating patients with treatment-refractory NRAS-driven melanomas.
format Online
Article
Text
id pubmed-9913232
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-99132322023-02-11 ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization Lyon, Anastasia Tripathi, Rakshamani Meeks, Christina He, Daheng Wu, Yuanyuan Liu, Jinpeng Wang, Chi Chen, Jing Zhu, Haining Mukherjee, Sujata Ganguly, Saptadwipa Plattner, Rina Cancers (Basel) Article SIMPLE SUMMARY: NRAS-mutant melanoma is a highly aggressive subtype with few treatment options. Although both BRAF-mutant and NRAS-mutant melanomas have activation of the MEK/ERK pathway, MEK inhibitors (MEKi) are only effective for the BRAF-mutant subtype. The aim of this study was to understand why MEKi are ineffective in NRAS-mutant melanomas with the long-term goal of identifying new treatment regimens. Here, we show that ABL and DDR kinases are critically important for MEKi resistance because they cooperate to promote the stability of key proteins involved in driving melanoma growth and survival. FDA-approved drugs that inhibit ABL1/2 and DDR1 have been used for decades to treat leukemia. We showed that one such inhibitor prevents MEKi resistance from developing in a NRAS-mutant melanoma animal model. Thus, the data in this study provide the rationale for testing the use of drugs targeting ABL1/2 and DDR1 in combination with MEKi for patients with NRAS-mutant melanomas who have failed to respond to immunotherapy. ABSTRACT: Melanomas harboring NRAS mutations are a particularly aggressive and deadly subtype. If patients cannot tolerate or the melanomas are insensitive to immune checkpoint blockade, there are no effective 2nd-line treatment options. Drugs targeting the RAF/MEK/ERK pathway, which are used for BRAF-mutant melanomas, do little to increase progression-free survival (PFS). Here, using both loss-of-function and gain-of-function approaches, we show that ABL1/2 and DDR1 are critical nodes during NRAS-mutant melanoma intrinsic and acquired MEK inhibitor (MEKi) resistance. In some acquired resistance cells, ABL1/2 and DDR1 cooperate to stabilize RAF proteins, activate ERK cytoplasmic and nuclear signaling, repress p27/KIP1 expression, and drive RAF homodimerization. In contrast, other acquired resistance cells depend solely on ABL1/2 for their survival, and are sensitive to highly specific allosteric ABL1/2 inhibitors, which prevent β-catenin nuclear localization and destabilize MYC and ETS1 in an ERK-independent manner. Significantly, targeting ABL1/2 and DDR1 with an FDA-approved anti-leukemic drug, reverses intrinsic MEKi resistance, delays acquisition of acquired resistance, and doubles the survival time in a NRAS-mutant mouse model. These data indicate that repurposing FDA-approved drugs targeting ABL1/2 and DDR1 may be a novel and effective strategy for treating patients with treatment-refractory NRAS-driven melanomas. MDPI 2023-02-02 /pmc/articles/PMC9913232/ /pubmed/36765910 http://dx.doi.org/10.3390/cancers15030954 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Lyon, Anastasia
Tripathi, Rakshamani
Meeks, Christina
He, Daheng
Wu, Yuanyuan
Liu, Jinpeng
Wang, Chi
Chen, Jing
Zhu, Haining
Mukherjee, Sujata
Ganguly, Saptadwipa
Plattner, Rina
ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization
title ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization
title_full ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization
title_fullStr ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization
title_full_unstemmed ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization
title_short ABL1/2 and DDR1 Drive MEKi Resistance in NRAS-Mutant Melanomas by Stabilizing RAF/MYC/ETS1 and Promoting RAF Homodimerization
title_sort abl1/2 and ddr1 drive meki resistance in nras-mutant melanomas by stabilizing raf/myc/ets1 and promoting raf homodimerization
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9913232/
https://www.ncbi.nlm.nih.gov/pubmed/36765910
http://dx.doi.org/10.3390/cancers15030954
work_keys_str_mv AT lyonanastasia abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT tripathirakshamani abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT meekschristina abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT hedaheng abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT wuyuanyuan abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT liujinpeng abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT wangchi abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT chenjing abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT zhuhaining abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT mukherjeesujata abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT gangulysaptadwipa abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization
AT plattnerrina abl12andddr1drivemekiresistanceinnrasmutantmelanomasbystabilizingrafmycets1andpromotingrafhomodimerization

Ejemplares similares