Antifibrotic drugs as therapeutic tools in resistant melanoma

to related objects

Melanoma is the most aggressive form of skin cancer. Together with the recent advances in immunotherapy, targeted therapy with inhibitors of the Mitogen Activated Protein Kinase (MAPKi) pathway including BRAF and MEK inhibitors has greatly improved the clinical outcome of these patients. Unfortunately, due to genetic and non‐genetic events, many patients develop resistance to MAPKi. Melanoma phenotypic plasticity, understood as the ability of melanoma cells to dynamically transition between different states with varying levels of differentiation/dedifferentiation, is key for melanoma progression. Lineage plasticity has also emerged as an important mechanism of non‐genetic adaptive melanoma drug resistance in the clinic (Arozarena & Wellbrock, 2019), highlighting the need for a deeper characterization of the mechanisms that control this process. In this issue of EMBO Molecular Medicine, Diazzi et al (2022) identify a mechanism regulating MAPKi‐induced phenotypic plasticity and resistance, providing evidence to support the use of an anti‐fibrotic drug as a potential novel combinatorial therapeutic approach.

Location: Deutsche Nationalbibliothek Frankfurt am Main

Extent: Online-Ressource

Language: Englisch

Bibliographic citation: Antifibrotic drugs as therapeutic tools in resistant melanoma ; day:14 ; month:02 ; year:2022 ; extent:2
EMBO molecular medicine / European Molecular Biology Organization ; (14.02.2022) (gesamt 2)

Creator: Sanchez‐Laorden, Berta
Nieto, M. Angela

DOI: 10.15252/emmm.202115449

URN: urn:nbn:de:101:1-2022021414072690020003

Rights: Open Access; Der Zugriff auf das Objekt ist unbeschränkt möglich.

Last update: 15.08.2025, 7:33 AM CEST

Data provider

This object is provided by:
Deutsche Nationalbibliothek. If you have any questions about the object, please contact the data provider.

Show original at data provider

Associated

Sanchez‐Laorden, Berta
Nieto, M. Angela

Other Objects (12)

PPARG as therapeutic target for antifibrotic therapy

The AhR‐SRC axis as a therapeutic vulnerability in BRAFi ‐resistant melanoma

The therapeutic landscape of advanced melanoma

Cell mediated ECM-degradation as an emerging tool for anti-fibrotic strategy

Multi-organ landscape of therapy-resistant melanoma

Antifibrotic Therapies in the Liver

Antifibrotic therapies to control cardiac fibrosis

Enhanced IL-34 expression in Nivolumab-resistant metastatic melanoma

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

Aberrant DNA methylation in melanoma: biomarker and therapeutic opportunities

Melanoma-associated brain metastasis: Molecular mechanisms and therapeutic options

Antifibrotic therapy to normalize the tumor microenvironment

PPARG as therapeutic target for antifibrotic therapy

The AhR‐SRC axis as a therapeutic vulnerability in BRAFi ‐resistant melanoma

The therapeutic landscape of advanced melanoma

Cell mediated ECM-degradation as an emerging tool for anti-fibrotic strategy

Multi-organ landscape of therapy-resistant melanoma

Antifibrotic Therapies in the Liver

Antifibrotic therapies to control cardiac fibrosis

Enhanced IL-34 expression in Nivolumab-resistant metastatic melanoma

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

Aberrant DNA methylation in melanoma: biomarker and therapeutic opportunities

Melanoma-associated brain metastasis: Molecular mechanisms and therapeutic options

Antifibrotic therapy to normalize the tumor microenvironment

PPARG as therapeutic target for antifibrotic therapy

The AhR‐SRC axis as a therapeutic vulnerability in BRAFi ‐resistant melanoma

The therapeutic landscape of advanced melanoma

Cell mediated ECM-degradation as an emerging tool for anti-fibrotic strategy

Multi-organ landscape of therapy-resistant melanoma

Antifibrotic Therapies in the Liver

Antifibrotic therapies to control cardiac fibrosis

Enhanced IL-34 expression in Nivolumab-resistant metastatic melanoma

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

Aberrant DNA methylation in melanoma: biomarker and therapeutic opportunities

Melanoma-associated brain metastasis: Molecular mechanisms and therapeutic options

Antifibrotic therapy to normalize the tumor microenvironment

Cultural heritage institutions wishing to register will find more information here.

Fields marked * need to be filled in.

Username*

Please enter your username

Email*

Please enter your email address

Please do not fill this field

First name

Last name

Password*

Please enter your password

Confirm password*

Please enter the same password

I have read the terms of use and the privacy policy for the collection of personal data and accept them. *

This field is required.

I would like to subscribe to the newsletter of the Deutsche Digitale Bibliothek. See newsletter subscription info.

Account created

Your "My DDB" account has been successfully created. Before you can log in to your account, you must click the confirmation link in the message we just sent to the email address you provided.

Antifibrotic drugs as therapeutic tools in resistant melanoma

Object Details

References and Relationships

Contributors, Places and Time

Further information

Data provider

Associated

Other Objects (12)

PPARG as therapeutic target for antifibrotic therapy

The AhR‐SRC axis as a therapeutic vulnerability in BRAFi ‐resistant melanoma

The therapeutic landscape of advanced melanoma

Cell mediated ECM-degradation as an emerging tool for anti-fibrotic strategy

Multi-organ landscape of therapy-resistant melanoma

Antifibrotic Therapies in the Liver

Antifibrotic therapies to control cardiac fibrosis

Enhanced IL-34 expression in Nivolumab-resistant metastatic melanoma

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

Aberrant DNA methylation in melanoma: biomarker and therapeutic opportunities

Melanoma-associated brain metastasis: Molecular mechanisms and therapeutic options

Antifibrotic therapy to normalize the tumor microenvironment

PPARG as therapeutic target for antifibrotic therapy

The AhR‐SRC axis as a therapeutic vulnerability in BRAFi ‐resistant melanoma

The therapeutic landscape of advanced melanoma

Cell mediated ECM-degradation as an emerging tool for anti-fibrotic strategy

Multi-organ landscape of therapy-resistant melanoma

Antifibrotic Therapies in the Liver

Antifibrotic therapies to control cardiac fibrosis

Enhanced IL-34 expression in Nivolumab-resistant metastatic melanoma

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

Aberrant DNA methylation in melanoma: biomarker and therapeutic opportunities

Melanoma-associated brain metastasis: Molecular mechanisms and therapeutic options

Antifibrotic therapy to normalize the tumor microenvironment

PPARG as therapeutic target for antifibrotic therapy

The AhR‐SRC axis as a therapeutic vulnerability in BRAFi ‐resistant melanoma

The therapeutic landscape of advanced melanoma

Cell mediated ECM-degradation as an emerging tool for anti-fibrotic strategy

Multi-organ landscape of therapy-resistant melanoma

Antifibrotic Therapies in the Liver

Antifibrotic therapies to control cardiac fibrosis

Enhanced IL-34 expression in Nivolumab-resistant metastatic melanoma

Gene Expression Signature of BRAF Inhibitor Resistant Melanoma Spheroids

Aberrant DNA methylation in melanoma: biomarker and therapeutic opportunities

Melanoma-associated brain metastasis: Molecular mechanisms and therapeutic options

Antifibrotic therapy to normalize the tumor microenvironment

Related objects

Reset password