Differential Infiltration of Key Immune T-Cell Populations Across Malignancies Varying by Immunogenic Potential and the Likelihood of Response to Immunotherapy

Islam Eljilany; Sam Coleman; Aik Choon Tan; Martin D. McCarter; John Carpten; Howard Colman; Abdul Rafeh Naqash; Igor Puzanov; Susanne M. Arnold; Michelle L. Churchman; Daniel Spakowicz; Bodour Salhia; Julian Marin; Shridar Ganesan; Aakrosh Ratan; Craig Shriver; Patrick Hwu; William S. Dalton; George J. Weiner; Jose R. Conejo-Garcia; Paulo Rodriguez; Ahmad A. Tarhini

doi:10.3390/cells13231993

Differential Infiltration of Key Immune T-Cell Populations Across Malignancies Varying by Immunogenic Potential and the Likelihood of Response to Immunotherapy

Islam Eljilany
, Sam Coleman
, Aik Choon Tan
, Martin D. McCarter
, John Carpten
, Howard Colman
, Abdul Rafeh Naqash
, Igor Puzanov
, Susanne M. Arnold
, Michelle L. Churchman
, Daniel Spakowicz
, Bodour Salhia
, Julian Marin
, Shridar Ganesan
, Aakrosh Ratan
, Craig Shriver
, Patrick Hwu
, William S. Dalton
, George J. Weiner
, Jose R. Conejo-Garcia

Paulo Rodriguez, Ahmad A. Tarhini

Research output: Contribution to journal › Article › peer-review

4 Scopus citations

Abstract

Background: Solid tumors vary by the immunogenic potential of the tumor microenvironment (TME) and the likelihood of response to immunotherapy. The emerging literature has identified key immune cell populations that significantly impact immune activation or suppression within the TME. This study investigated candidate T-cell populations and their differential infiltration within different tumor types as estimated from mRNA co-expression levels of the corresponding cellular markers. Methods: We analyzed the mRNA co-expression levels of cellular biomarkers that define stem-like tumor-infiltrating lymphocytes (TILs), tissue-resident memory T-cells (TRM), early dysfunctional T-cells, late dysfunctional T-cells, activated-potentially anti-tumor (APA) T-cells and Butyrophilin 3A (BTN3A) isoforms, utilizing clinical and transcriptomic data from 1892 patients diagnosed with melanoma, bladder, ovarian, or pancreatic carcinomas. Real-world data were collected under the Total Cancer Care Protocol and the Avatar^® project (NCT03977402) across 18 cancer centers. Furthermore, we compared the survival outcomes following immune checkpoint inhibitors (ICIs) based on immune cell gene expression. Results: In melanoma and bladder cancer, the estimated infiltration of APA T-cells differed significantly (p = 4.67 × 10⁻¹² and p = 5.80 × 10⁻¹², respectively) compared to ovarian and pancreatic cancers. Ovarian cancer had lower TRM T-cell infiltration than melanoma, bladder, and pancreatic (p = 2.23 × 10⁻⁸, 3.86 × 10⁻²⁸, and 7.85 × 10⁻⁹, respectively). Similar trends were noted with stem-like, early, and late dysfunctional T-cells. Melanoma and ovarian expressed BTN3A isoforms more than other malignancies. Higher densities of stem-like TILs; TRM, early and late dysfunctional T-cells; APA T-cells; and BTN3A isoforms were associated with increased survival in melanoma (p = 0.0075, 0.00059, 0.013, 0.005, 0.0016, and 0.041, respectively). The TRM gene signature was a moderate predictor of survival in the melanoma cohort (AUROC = 0.65), with similar findings in testing independent public datasets of ICI-treated patients with melanoma (AUROC 0.61–0.64). Conclusions: Key cellular elements related to immune activation are more heavily infiltrated within ICI-responsive versus non-responsive malignancies, supporting a central role in anti-tumor immunity. In melanoma patients treated with ICIs, higher densities of stem-like TILs, TRM T-cells, early dysfunctional T-cells, late dysfunctional T-cells, APA T-cells, and BTN3A isoforms were associated with improved survival.

Original language	English
Article number	1993
Journal	Cells
Volume	13
Issue number	23
DOIs	https://doi.org/10.3390/cells13231993
State	Published - Dec 2024

Bibliographical note

Publisher Copyright:
© 2024 by the authors.

Funding

This work was supported by an ORIEN FOUNDATION NOVA (New Oncologic Visionary Award) Grant and the Community Foundation of Tampa Bay: 69-21295-01-01 (PI: A. Tarhini).

Funders	Funder number
ORIEN FOUNDATION NOVA	69-21295-01-01

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

RNA expression
T-cell
bladder cancer
immune cell infiltration
immune response
melanoma
ovarian cancer
pancreatic cancer

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

Access to Document

10.3390/cells13231993

Cite this

Eljilany, I., Coleman, S., Tan, A. C., McCarter, M. D., Carpten, J., Colman, H., Naqash, A. R., Puzanov, I., Arnold, S. M., Churchman, M. L., Spakowicz, D., Salhia, B., Marin, J., Ganesan, S., Ratan, A., Shriver, C., Hwu, P., Dalton, W. S., Weiner, G. J., ... Tarhini, A. A. (2024). Differential Infiltration of Key Immune T-Cell Populations Across Malignancies Varying by Immunogenic Potential and the Likelihood of Response to Immunotherapy. Cells, 13(23), Article 1993. https://doi.org/10.3390/cells13231993

@article{c38be1bda2d946d4a23e35e084930a80,

title = "Differential Infiltration of Key Immune T-Cell Populations Across Malignancies Varying by Immunogenic Potential and the Likelihood of Response to Immunotherapy",

abstract = "Background: Solid tumors vary by the immunogenic potential of the tumor microenvironment (TME) and the likelihood of response to immunotherapy. The emerging literature has identified key immune cell populations that significantly impact immune activation or suppression within the TME. This study investigated candidate T-cell populations and their differential infiltration within different tumor types as estimated from mRNA co-expression levels of the corresponding cellular markers. Methods: We analyzed the mRNA co-expression levels of cellular biomarkers that define stem-like tumor-infiltrating lymphocytes (TILs), tissue-resident memory T-cells (TRM), early dysfunctional T-cells, late dysfunctional T-cells, activated-potentially anti-tumor (APA) T-cells and Butyrophilin 3A (BTN3A) isoforms, utilizing clinical and transcriptomic data from 1892 patients diagnosed with melanoma, bladder, ovarian, or pancreatic carcinomas. Real-world data were collected under the Total Cancer Care Protocol and the Avatar{\textregistered} project (NCT03977402) across 18 cancer centers. Furthermore, we compared the survival outcomes following immune checkpoint inhibitors (ICIs) based on immune cell gene expression. Results: In melanoma and bladder cancer, the estimated infiltration of APA T-cells differed significantly (p = 4.67 × 10−12 and p = 5.80 × 10−12, respectively) compared to ovarian and pancreatic cancers. Ovarian cancer had lower TRM T-cell infiltration than melanoma, bladder, and pancreatic (p = 2.23 × 10−8, 3.86 × 10−28, and 7.85 × 10−9, respectively). Similar trends were noted with stem-like, early, and late dysfunctional T-cells. Melanoma and ovarian expressed BTN3A isoforms more than other malignancies. Higher densities of stem-like TILs; TRM, early and late dysfunctional T-cells; APA T-cells; and BTN3A isoforms were associated with increased survival in melanoma (p = 0.0075, 0.00059, 0.013, 0.005, 0.0016, and 0.041, respectively). The TRM gene signature was a moderate predictor of survival in the melanoma cohort (AUROC = 0.65), with similar findings in testing independent public datasets of ICI-treated patients with melanoma (AUROC 0.61–0.64). Conclusions: Key cellular elements related to immune activation are more heavily infiltrated within ICI-responsive versus non-responsive malignancies, supporting a central role in anti-tumor immunity. In melanoma patients treated with ICIs, higher densities of stem-like TILs, TRM T-cells, early dysfunctional T-cells, late dysfunctional T-cells, APA T-cells, and BTN3A isoforms were associated with improved survival.",

keywords = "RNA expression, T-cell, bladder cancer, immune cell infiltration, immune response, melanoma, ovarian cancer, pancreatic cancer",

author = "Islam Eljilany and Sam Coleman and Tan, \{Aik Choon\} and McCarter, \{Martin D.\} and John Carpten and Howard Colman and Naqash, \{Abdul Rafeh\} and Igor Puzanov and Arnold, \{Susanne M.\} and Churchman, \{Michelle L.\} and Daniel Spakowicz and Bodour Salhia and Julian Marin and Shridar Ganesan and Aakrosh Ratan and Craig Shriver and Patrick Hwu and Dalton, \{William S.\} and Weiner, \{George J.\} and Conejo-Garcia, \{Jose R.\} and Paulo Rodriguez and Tarhini, \{Ahmad A.\}",

note = "Publisher Copyright: {\textcopyright} 2024 by the authors.",

year = "2024",

month = dec,

doi = "10.3390/cells13231993",

language = "English",

volume = "13",

number = "23",

}

Eljilany, I, Coleman, S, Tan, AC, McCarter, MD, Carpten, J, Colman, H, Naqash, AR, Puzanov, I, Arnold, SM, Churchman, ML, Spakowicz, D, Salhia, B, Marin, J, Ganesan, S, Ratan, A, Shriver, C, Hwu, P, Dalton, WS, Weiner, GJ, Conejo-Garcia, JR, Rodriguez, P & Tarhini, AA 2024, 'Differential Infiltration of Key Immune T-Cell Populations Across Malignancies Varying by Immunogenic Potential and the Likelihood of Response to Immunotherapy', Cells, vol. 13, no. 23, 1993. https://doi.org/10.3390/cells13231993

TY - JOUR

T1 - Differential Infiltration of Key Immune T-Cell Populations Across Malignancies Varying by Immunogenic Potential and the Likelihood of Response to Immunotherapy

AU - Eljilany, Islam

AU - Coleman, Sam

AU - Tan, Aik Choon

AU - McCarter, Martin D.

AU - Carpten, John

AU - Colman, Howard

AU - Naqash, Abdul Rafeh

AU - Puzanov, Igor

AU - Arnold, Susanne M.

AU - Churchman, Michelle L.

AU - Spakowicz, Daniel

AU - Salhia, Bodour

AU - Marin, Julian

AU - Ganesan, Shridar

AU - Ratan, Aakrosh

AU - Shriver, Craig

AU - Hwu, Patrick

AU - Dalton, William S.

AU - Weiner, George J.

AU - Conejo-Garcia, Jose R.

AU - Rodriguez, Paulo

AU - Tarhini, Ahmad A.

PY - 2024/12

Y1 - 2024/12

N2 - Background: Solid tumors vary by the immunogenic potential of the tumor microenvironment (TME) and the likelihood of response to immunotherapy. The emerging literature has identified key immune cell populations that significantly impact immune activation or suppression within the TME. This study investigated candidate T-cell populations and their differential infiltration within different tumor types as estimated from mRNA co-expression levels of the corresponding cellular markers. Methods: We analyzed the mRNA co-expression levels of cellular biomarkers that define stem-like tumor-infiltrating lymphocytes (TILs), tissue-resident memory T-cells (TRM), early dysfunctional T-cells, late dysfunctional T-cells, activated-potentially anti-tumor (APA) T-cells and Butyrophilin 3A (BTN3A) isoforms, utilizing clinical and transcriptomic data from 1892 patients diagnosed with melanoma, bladder, ovarian, or pancreatic carcinomas. Real-world data were collected under the Total Cancer Care Protocol and the Avatar® project (NCT03977402) across 18 cancer centers. Furthermore, we compared the survival outcomes following immune checkpoint inhibitors (ICIs) based on immune cell gene expression. Results: In melanoma and bladder cancer, the estimated infiltration of APA T-cells differed significantly (p = 4.67 × 10−12 and p = 5.80 × 10−12, respectively) compared to ovarian and pancreatic cancers. Ovarian cancer had lower TRM T-cell infiltration than melanoma, bladder, and pancreatic (p = 2.23 × 10−8, 3.86 × 10−28, and 7.85 × 10−9, respectively). Similar trends were noted with stem-like, early, and late dysfunctional T-cells. Melanoma and ovarian expressed BTN3A isoforms more than other malignancies. Higher densities of stem-like TILs; TRM, early and late dysfunctional T-cells; APA T-cells; and BTN3A isoforms were associated with increased survival in melanoma (p = 0.0075, 0.00059, 0.013, 0.005, 0.0016, and 0.041, respectively). The TRM gene signature was a moderate predictor of survival in the melanoma cohort (AUROC = 0.65), with similar findings in testing independent public datasets of ICI-treated patients with melanoma (AUROC 0.61–0.64). Conclusions: Key cellular elements related to immune activation are more heavily infiltrated within ICI-responsive versus non-responsive malignancies, supporting a central role in anti-tumor immunity. In melanoma patients treated with ICIs, higher densities of stem-like TILs, TRM T-cells, early dysfunctional T-cells, late dysfunctional T-cells, APA T-cells, and BTN3A isoforms were associated with improved survival.

AB - Background: Solid tumors vary by the immunogenic potential of the tumor microenvironment (TME) and the likelihood of response to immunotherapy. The emerging literature has identified key immune cell populations that significantly impact immune activation or suppression within the TME. This study investigated candidate T-cell populations and their differential infiltration within different tumor types as estimated from mRNA co-expression levels of the corresponding cellular markers. Methods: We analyzed the mRNA co-expression levels of cellular biomarkers that define stem-like tumor-infiltrating lymphocytes (TILs), tissue-resident memory T-cells (TRM), early dysfunctional T-cells, late dysfunctional T-cells, activated-potentially anti-tumor (APA) T-cells and Butyrophilin 3A (BTN3A) isoforms, utilizing clinical and transcriptomic data from 1892 patients diagnosed with melanoma, bladder, ovarian, or pancreatic carcinomas. Real-world data were collected under the Total Cancer Care Protocol and the Avatar® project (NCT03977402) across 18 cancer centers. Furthermore, we compared the survival outcomes following immune checkpoint inhibitors (ICIs) based on immune cell gene expression. Results: In melanoma and bladder cancer, the estimated infiltration of APA T-cells differed significantly (p = 4.67 × 10−12 and p = 5.80 × 10−12, respectively) compared to ovarian and pancreatic cancers. Ovarian cancer had lower TRM T-cell infiltration than melanoma, bladder, and pancreatic (p = 2.23 × 10−8, 3.86 × 10−28, and 7.85 × 10−9, respectively). Similar trends were noted with stem-like, early, and late dysfunctional T-cells. Melanoma and ovarian expressed BTN3A isoforms more than other malignancies. Higher densities of stem-like TILs; TRM, early and late dysfunctional T-cells; APA T-cells; and BTN3A isoforms were associated with increased survival in melanoma (p = 0.0075, 0.00059, 0.013, 0.005, 0.0016, and 0.041, respectively). The TRM gene signature was a moderate predictor of survival in the melanoma cohort (AUROC = 0.65), with similar findings in testing independent public datasets of ICI-treated patients with melanoma (AUROC 0.61–0.64). Conclusions: Key cellular elements related to immune activation are more heavily infiltrated within ICI-responsive versus non-responsive malignancies, supporting a central role in anti-tumor immunity. In melanoma patients treated with ICIs, higher densities of stem-like TILs, TRM T-cells, early dysfunctional T-cells, late dysfunctional T-cells, APA T-cells, and BTN3A isoforms were associated with improved survival.

KW - RNA expression

KW - T-cell

KW - bladder cancer

KW - immune cell infiltration

KW - immune response

KW - melanoma

KW - ovarian cancer

KW - pancreatic cancer

UR - https://www.scopus.com/pages/publications/85211788132

UR - https://www.scopus.com/pages/publications/85211788132#tab=citedBy

U2 - 10.3390/cells13231993

DO - 10.3390/cells13231993

M3 - Article

C2 - 39682743

AN - SCOPUS:85211788132

VL - 13

JO - Cells

JF - Cells

IS - 23

M1 - 1993

ER -

Differential Infiltration of Key Immune T-Cell Populations Across Malignancies Varying by Immunogenic Potential and the Likelihood of Response to Immunotherapy

Abstract

Bibliographical note

Funding

UN SDGs

Keywords

ASJC Scopus subject areas

Access to Document

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