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Midkine rewires the melanoma microenvironment toward a tolerogenic and immune-resistant state

Authors :
Gonzalo Gómez-López
Maria S. Soengas
Cynthia Mucientes
José Luis Rodríguez-Peralto
Lola Martínez
Paula Comune Pennacchi
David Olmeda
Cristina Tejedo
Javier Munoz
Fatima Al-Shahrour
Daniela Cerezo-Wallis
Andrew X. Chen
Kevin Troulé
Pablo L. Ortiz-Romero
Osvaldo Graña-Castro
Mitchell P. Levesque
Raul Rabadan
Marta Contreras-Alcalde
Xavier Catena
Sabrina A. Hogan
Peter Kölblinger
Héctor Tejero
Estela Cañón
Nuria Ibarz
Tonantzin G. Calvo
Source :
Nature medicine. 26(12)
Publication Year :
2019

Abstract

An open question in aggressive cancers such as melanoma is how malignant cells can shift the immune system to pro-tumorigenic functions. Here we identify midkine (MDK) as a melanoma-secreted driver of an inflamed, but immune evasive, microenvironment that defines poor patient prognosis and resistance to immune checkpoint blockade. Mechanistically, MDK was found to control the transcriptome of melanoma cells, allowing for coordinated activation of nuclear factor-κB and downregulation of interferon-associated pathways. The resulting MDK-modulated secretome educated macrophages towards tolerant phenotypes that promoted CD8+ T cell dysfunction. In contrast, genetic targeting of MDK sensitized melanoma cells to anti-PD-1/anti-PD-L1 treatment. Emphasizing the translational relevance of these findings, the expression profile of MDK-depleted tumors was enriched in key indicators of a good response to immune checkpoint blockers in independent patient cohorts. Together, these data reveal that MDK acts as an internal modulator of autocrine and paracrine signals that maintain immune suppression in aggressive melanomas.

Details

ISSN :
1546170X
Volume :
26
Issue :
12
Database :
OpenAIRE
Journal :
Nature medicine
Accession number :
edsair.doi.dedup.....848a065b4bf5ff3cde0a36093c2cf05b