Cooperative Behaviour and Phenotype Plasticity Evolve During Melanoma Progression

Overview

Journal Pigment Cell Melanoma Res

Date 2020 Mar 8

PMID 32145051

Citations 13

Authors

Emily J Rowling

Zsofia Miskolczi

Raghavendar Nagaraju

Daniel J Wilcock

Ping Wang

Brian Telfer

Yaoyong Li

Irene Lasheras-Otero

Marta Redondo-Munoz

Andrew D Sharrocks

Imanol Arozarena

Claudia Wellbrock

Affiliations

Soon will be listed here.

Abstract

A major challenge for managing melanoma is its tumour heterogeneity based on individual co-existing melanoma cell phenotypes. These phenotypes display variable responses to standard therapies, and they drive individual steps of melanoma progression; hence, understanding their behaviour is imperative. Melanoma phenotypes are defined by distinct transcriptional states, which relate to different melanocyte lineage development phases, ranging from a mesenchymal, neural crest-like to a proliferative, melanocytic phenotype. It is thought that adaptive phenotype plasticity based on transcriptional reprogramming drives melanoma progression, but at which stage individual phenotypes dominate and moreover, how they interact is poorly understood. We monitored melanocytic and mesenchymal phenotypes throughout melanoma progression and detected transcriptional reprogramming at different stages, with a gain in mesenchymal traits in circulating melanoma cells (CTCs) and proliferative features in metastatic tumours. Intriguingly, we found that distinct phenotype populations interact in a cooperative manner, which generates tumours of greater "fitness," supports CTCs and expands organotropic cues in metastases. Fibronectin, expressed in mesenchymal cells, acts as key player in cooperativity and promotes survival of melanocytic cells. Our data reveal an important role for inter-phenotype communications at various stages of disease progression, suggesting these communications could act as therapeutic target.

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References

Aceto N, Bardia A, Miyamoto D, Donaldson M, Wittner B, Spencer J . Circulating tumor cell clusters are oligoclonal precursors of breast cancer metastasis. Cell. 2014; 158(5):1110-1122. PMC: 4149753. DOI: 10.1016/j.cell.2014.07.013. View

Widmer D, Cheng P, Eichhoff O, Belloni B, Zipser M, Schlegel N . Systematic classification of melanoma cells by phenotype-specific gene expression mapping. Pigment Cell Melanoma Res. 2012; 25(3):343-53. DOI: 10.1111/j.1755-148X.2012.00986.x. View

Pasqualini R, Bourdoulous S, Koivunen E, Woods Jr V, Ruoslahti E . A polymeric form of fibronectin has antimetastatic effects against multiple tumor types. Nat Med. 1996; 2(11):1197-203. DOI: 10.1038/nm1196-1197. View

Ennen M, Keime C, Gambi G, Kieny A, Coassolo S, Thibault-Carpentier C . -High and -Low Cells and a Novel Subpopulation Expressing Genes of Both Cell States Contribute to Intra- and Intertumoral Heterogeneity of Primary Melanoma. Clin Cancer Res. 2017; 23(22):7097-7107. DOI: 10.1158/1078-0432.CCR-17-0010. View

Arozarena I, Bischof H, Gilby D, Belloni B, Dummer R, Wellbrock C . In melanoma, beta-catenin is a suppressor of invasion. Oncogene. 2011; 30(45):4531-43. PMC: 3160497. DOI: 10.1038/onc.2011.162. View

Pastushenko I, Brisebarre A, Sifrim A, Fioramonti M, Revenco T, Boumahdi S . Identification of the tumour transition states occurring during EMT. Nature. 2018; 556(7702):463-468. DOI: 10.1038/s41586-018-0040-3. View

Rambow F, Rogiers A, Marin-Bejar O, Aibar S, Femel J, Dewaele M . Toward Minimal Residual Disease-Directed Therapy in Melanoma. Cell. 2018; 174(4):843-855.e19. DOI: 10.1016/j.cell.2018.06.025. View

Rowling E, Miskolczi Z, Nagaraju R, Wilcock D, Wang P, Telfer B . Cooperative behaviour and phenotype plasticity evolve during melanoma progression. Pigment Cell Melanoma Res. 2020; 33(5):695-708. PMC: 7496243. DOI: 10.1111/pcmr.12873. View

Tirosh I, Izar B, Prakadan S, Wadsworth 2nd M, Treacy D, Trombetta J . Dissecting the multicellular ecosystem of metastatic melanoma by single-cell RNA-seq. Science. 2016; 352(6282):189-96. PMC: 4944528. DOI: 10.1126/science.aad0501. View

10.

Cheli Y, Giuliano S, Guiliano S, Botton T, Rocchi S, Hofman V . Mitf is the key molecular switch between mouse or human melanoma initiating cells and their differentiated progeny. Oncogene. 2011; 30(20):2307-18. DOI: 10.1038/onc.2010.598. View

11.

Yu M, Ting D, Stott S, Wittner B, Ozsolak F, Paul S . RNA sequencing of pancreatic circulating tumour cells implicates WNT signalling in metastasis. Nature. 2012; 487(7408):510-3. PMC: 3408856. DOI: 10.1038/nature11217. View

12.

Caramel J, Papadogeorgakis E, Hill L, Browne G, Richard G, Wierinckx A . A switch in the expression of embryonic EMT-inducers drives the development of malignant melanoma. Cancer Cell. 2013; 24(4):466-80. DOI: 10.1016/j.ccr.2013.08.018. View

13.

Rambow F, Job B, Petit V, Gesbert F, Delmas V, Seberg H . New Functional Signatures for Understanding Melanoma Biology from Tumor Cell Lineage-Specific Analysis. Cell Rep. 2015; 13(4):840-853. PMC: 5970542. DOI: 10.1016/j.celrep.2015.09.037. View

14.

Smith M, Rowling E, Miskolczi Z, Ferguson J, Spoerri L, Haass N . Targeting endothelin receptor signalling overcomes heterogeneity driven therapy failure. EMBO Mol Med. 2017; 9(8):1011-1029. PMC: 5538298. DOI: 10.15252/emmm.201607156. View

15.

Cheli Y, Ohanna M, Ballotti R, Bertolotto C . Fifteen-year quest for microphthalmia-associated transcription factor target genes. Pigment Cell Melanoma Res. 2009; 23(1):27-40. DOI: 10.1111/j.1755-148X.2009.00653.x. View

16.

Strub T, Giuliano S, Ye T, Bonet C, Keime C, Kobi D . Essential role of microphthalmia transcription factor for DNA replication, mitosis and genomic stability in melanoma. Oncogene. 2011; 30(20):2319-32. DOI: 10.1038/onc.2010.612. View

17.

Marusyk A, Tabassum D, Altrock P, Almendro V, Michor F, Polyak K . Non-cell-autonomous driving of tumour growth supports sub-clonal heterogeneity. Nature. 2014; 514(7520):54-8. PMC: 4184961. DOI: 10.1038/nature13556. View

18.

Arozarena I, Wellbrock C . Phenotype plasticity as enabler of melanoma progression and therapy resistance. Nat Rev Cancer. 2019; 19(7):377-391. DOI: 10.1038/s41568-019-0154-4. View

19.

Simmons J, Pierce C, Al-Ejeh F, Boyle G . MITF and BRN2 contribute to metastatic growth after dissemination of melanoma. Sci Rep. 2017; 7(1):10909. PMC: 5589904. DOI: 10.1038/s41598-017-11366-y. View

20.

Lauss M, Haq R, Cirenajwis H, Phung B, Harbst K, Staaf J . Genome-Wide DNA Methylation Analysis in Melanoma Reveals the Importance of CpG Methylation in MITF Regulation. J Invest Dermatol. 2015; 135(7):1820-1828. PMC: 4720161. DOI: 10.1038/jid.2015.61. View