The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response

M. E. Vazquez-Cruz; P. Basurto-Lozada; C. Molina-Aguilar; S. Orozco-Ruiz; B. Van Haastrecht; I. Simonin-Wilmer; H. Martinez-Said; A. Alvarez-Cano; D. Y. Garcia-Ortega; A. Hidalgo-Miranda; D. Hinojosa-Ugarte; I. Ferreira; L. A. Tavares-de-la-Paz; J. E. Olguin; I. Salinas; A. Rodriguez-Perez; J. M. Martinez-Gomez; I. van der Zee; D. R. Grimes; H. Vidaurri de la Cruz; J. Saez-Rodriguez; J. A. Newton-Bishop; D. T. Bishop; M. P. Levesque; P. A. Possik; D. J. Adams; C. D. Robles-Espinoza; Carla Daniela Robles-Espinoza

doi:10.1101/2025.05.05.25325616

The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response

M. E. Vazquez-Cruz
, P. Basurto-Lozada
, C. Molina-Aguilar
, S. Orozco-Ruiz
, B. Van Haastrecht
, I. Simonin-Wilmer
, H. Martinez-Said
, A. Alvarez-Cano
, D. Y. Garcia-Ortega
, A. Hidalgo-Miranda
, D. Hinojosa-Ugarte
, I. Ferreira
, L. A. Tavares-de-la-Paz
, J. E. Olguin
, I. Salinas
, A. Rodriguez-Perez
, J. M. Martinez-Gomez
, I. van der Zee
, D. R. Grimes
, H. Vidaurri de la Cruz

J. Saez-Rodriguez, J. A. Newton-Bishop, D. T. Bishop, M. P. Levesque, P. A. Possik, D. J. Adams, C. D. Robles-Espinoza, Carla Daniela Robles-Espinoza^*

^*Corresponding author for this work

Research output: Working paper › Preprint › Academic

Abstract

Acral melanoma (AM) is a distinct and understudied subtype of melanoma that is reported to represent the majority of melanoma diagnoses in various Latin American, African and Asian countries. Patients with ulcerated AM diagnoses face a worse prognosis and increased risk of recurrence. While tumour ulceration has been shown to influence therapy response in cutaneous melanoma patients, the clinical and molecular traits of AM tumours remain poorly understood. In this study, we performed transcriptomic profiling of 59 AM samples and proteomic analysis of 45 AM samples from patients with extensively annotated clinical information. Our analysis revealed immunological differences in ulcerated tumours, including a significant upregulation of processes related to humoral immunity and markers for macrophages/monocytes, alongside a downregulation of keratins, epidermis-associated processes and cell adhesion. Notably, ulcerated tumours exhibited disruption of tight junctions and desmosomes, potentially explaining their compromised tissue integrity. We identified a significant increase of plasma cells, M0 macrophages and eosinophils within the ulcerated tumour microenvironment, suggesting that inflammation and infection might accompany these lesions. Moreover, fibronectin, CD8, PD-1, CD14 and CD68 protein levels were useful in distinguishing between ulcerated and non-ulcerated samples using a random forest classifier. These findings indicate that persistent inflammation and dysregulated immune responses characterise ulcerated AM, potentially offering new avenues for targeted therapeutic interventions in this aggressive melanoma subtype.

Original language	English
Publisher	medRxiv
DOIs	https://doi.org/10.1101/2025.05.05.25325616
Publication status	Published - 7 May 2025

Keywords

genetic and genomic medicine

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2025.05.05.25325616v1.fullSubmitted manuscript, 11.5 MBLicence: CC BY-ND

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Vazquez-Cruz, M. E., Basurto-Lozada, P., Molina-Aguilar, C., Orozco-Ruiz, S., Van Haastrecht, B., Simonin-Wilmer, I., Martinez-Said, H., Alvarez-Cano, A., Garcia-Ortega, D. Y., Hidalgo-Miranda, A., Hinojosa-Ugarte, D., Ferreira, I., Tavares-de-la-Paz, L. A., Olguin, J. E., Salinas, I., Rodriguez-Perez, A., Martinez-Gomez, J. M., van der Zee, I., Grimes, D. R., ... Robles-Espinoza, C. D. (2025). The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response. medRxiv. https://doi.org/10.1101/2025.05.05.25325616

@techreport{9c4dfc15fff24bbe952af0122b6266dd,

title = "The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response",

abstract = "Acral melanoma (AM) is a distinct and understudied subtype of melanoma that is reported to represent the majority of melanoma diagnoses in various Latin American, African and Asian countries. Patients with ulcerated AM diagnoses face a worse prognosis and increased risk of recurrence. While tumour ulceration has been shown to influence therapy response in cutaneous melanoma patients, the clinical and molecular traits of AM tumours remain poorly understood. In this study, we performed transcriptomic profiling of 59 AM samples and proteomic analysis of 45 AM samples from patients with extensively annotated clinical information. Our analysis revealed immunological differences in ulcerated tumours, including a significant upregulation of processes related to humoral immunity and markers for macrophages/monocytes, alongside a downregulation of keratins, epidermis-associated processes and cell adhesion. Notably, ulcerated tumours exhibited disruption of tight junctions and desmosomes, potentially explaining their compromised tissue integrity. We identified a significant increase of plasma cells, M0 macrophages and eosinophils within the ulcerated tumour microenvironment, suggesting that inflammation and infection might accompany these lesions. Moreover, fibronectin, CD8, PD-1, CD14 and CD68 protein levels were useful in distinguishing between ulcerated and non-ulcerated samples using a random forest classifier. These findings indicate that persistent inflammation and dysregulated immune responses characterise ulcerated AM, potentially offering new avenues for targeted therapeutic interventions in this aggressive melanoma subtype.",

keywords = "genetic and genomic medicine",

author = "Vazquez-Cruz, \{M. E.\} and P. Basurto-Lozada and C. Molina-Aguilar and S. Orozco-Ruiz and \{Van Haastrecht\}, B. and I. Simonin-Wilmer and H. Martinez-Said and A. Alvarez-Cano and Garcia-Ortega, \{D. Y.\} and A. Hidalgo-Miranda and D. Hinojosa-Ugarte and I. Ferreira and Tavares-de-la-Paz, \{L. A.\} and Olguin, \{J. E.\} and I. Salinas and A. Rodriguez-Perez and Martinez-Gomez, \{J. M.\} and \{van der Zee\}, I. and Grimes, \{D. R.\} and \{Vidaurri de la Cruz\}, H. and J. Saez-Rodriguez and Newton-Bishop, \{J. A.\} and Bishop, \{D. T.\} and Levesque, \{M. P.\} and Possik, \{P. A.\} and \{J. Adams\}, D. and Robles-Espinoza, \{C. D.\} and Robles-Espinoza, \{Carla Daniela\}",

year = "2025",

month = may,

day = "7",

doi = "10.1101/2025.05.05.25325616",

language = "English",

publisher = "medRxiv",

type = "WorkingPaper",

institution = "medRxiv",

}

Vazquez-Cruz, ME, Basurto-Lozada, P, Molina-Aguilar, C, Orozco-Ruiz, S, Van Haastrecht, B, Simonin-Wilmer, I, Martinez-Said, H, Alvarez-Cano, A, Garcia-Ortega, DY, Hidalgo-Miranda, A, Hinojosa-Ugarte, D, Ferreira, I, Tavares-de-la-Paz, LA, Olguin, JE, Salinas, I, Rodriguez-Perez, A, Martinez-Gomez, JM, van der Zee, I, Grimes, DR, Vidaurri de la Cruz, H, Saez-Rodriguez, J, Newton-Bishop, JA, Bishop, DT, Levesque, MP, Possik, PA, J. Adams, D, Robles-Espinoza, CD & Robles-Espinoza, CD 2025 'The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response' medRxiv. https://doi.org/10.1101/2025.05.05.25325616

TY - UNPB

T1 - The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response

AU - Vazquez-Cruz, M. E.

AU - Basurto-Lozada, P.

AU - Molina-Aguilar, C.

AU - Orozco-Ruiz, S.

AU - Van Haastrecht, B.

AU - Simonin-Wilmer, I.

AU - Martinez-Said, H.

AU - Alvarez-Cano, A.

AU - Garcia-Ortega, D. Y.

AU - Hidalgo-Miranda, A.

AU - Hinojosa-Ugarte, D.

AU - Ferreira, I.

AU - Tavares-de-la-Paz, L. A.

AU - Olguin, J. E.

AU - Salinas, I.

AU - Rodriguez-Perez, A.

AU - Martinez-Gomez, J. M.

AU - van der Zee, I.

AU - Grimes, D. R.

AU - Vidaurri de la Cruz, H.

AU - Saez-Rodriguez, J.

AU - Newton-Bishop, J. A.

AU - Bishop, D. T.

AU - Levesque, M. P.

AU - Possik, P. A.

AU - J. Adams, D.

AU - Robles-Espinoza, C. D.

AU - Robles-Espinoza, Carla Daniela

PY - 2025/5/7

Y1 - 2025/5/7

N2 - Acral melanoma (AM) is a distinct and understudied subtype of melanoma that is reported to represent the majority of melanoma diagnoses in various Latin American, African and Asian countries. Patients with ulcerated AM diagnoses face a worse prognosis and increased risk of recurrence. While tumour ulceration has been shown to influence therapy response in cutaneous melanoma patients, the clinical and molecular traits of AM tumours remain poorly understood. In this study, we performed transcriptomic profiling of 59 AM samples and proteomic analysis of 45 AM samples from patients with extensively annotated clinical information. Our analysis revealed immunological differences in ulcerated tumours, including a significant upregulation of processes related to humoral immunity and markers for macrophages/monocytes, alongside a downregulation of keratins, epidermis-associated processes and cell adhesion. Notably, ulcerated tumours exhibited disruption of tight junctions and desmosomes, potentially explaining their compromised tissue integrity. We identified a significant increase of plasma cells, M0 macrophages and eosinophils within the ulcerated tumour microenvironment, suggesting that inflammation and infection might accompany these lesions. Moreover, fibronectin, CD8, PD-1, CD14 and CD68 protein levels were useful in distinguishing between ulcerated and non-ulcerated samples using a random forest classifier. These findings indicate that persistent inflammation and dysregulated immune responses characterise ulcerated AM, potentially offering new avenues for targeted therapeutic interventions in this aggressive melanoma subtype.

AB - Acral melanoma (AM) is a distinct and understudied subtype of melanoma that is reported to represent the majority of melanoma diagnoses in various Latin American, African and Asian countries. Patients with ulcerated AM diagnoses face a worse prognosis and increased risk of recurrence. While tumour ulceration has been shown to influence therapy response in cutaneous melanoma patients, the clinical and molecular traits of AM tumours remain poorly understood. In this study, we performed transcriptomic profiling of 59 AM samples and proteomic analysis of 45 AM samples from patients with extensively annotated clinical information. Our analysis revealed immunological differences in ulcerated tumours, including a significant upregulation of processes related to humoral immunity and markers for macrophages/monocytes, alongside a downregulation of keratins, epidermis-associated processes and cell adhesion. Notably, ulcerated tumours exhibited disruption of tight junctions and desmosomes, potentially explaining their compromised tissue integrity. We identified a significant increase of plasma cells, M0 macrophages and eosinophils within the ulcerated tumour microenvironment, suggesting that inflammation and infection might accompany these lesions. Moreover, fibronectin, CD8, PD-1, CD14 and CD68 protein levels were useful in distinguishing between ulcerated and non-ulcerated samples using a random forest classifier. These findings indicate that persistent inflammation and dysregulated immune responses characterise ulcerated AM, potentially offering new avenues for targeted therapeutic interventions in this aggressive melanoma subtype.

KW - genetic and genomic medicine

U2 - 10.1101/2025.05.05.25325616

DO - 10.1101/2025.05.05.25325616

M3 - Preprint

BT - The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response

PB - medRxiv

ER -

The microenvironment of ulcerated acral melanoma is characterised by an inflammatory milieu and an enhanced humoral immune response

Abstract

Keywords

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