Peripheral Blood Immune Cell Profiling as Predictive Biomarkers for Neoadjuvant Therapy Response in Early Breast Cancer Patients

Rahma Ben Ayed

doi:10.20373/uniupo/openthesis/220663

Peripheral Blood Immune Cell Profiling as Predictive Biomarkers for Neoadjuvant Therapy Response in Early Breast Cancer Patients

Rahma Ben Ayed

Research output: Types of Thesis › Doctoral Thesis

Abstract

Background: In breast cancer (BC), pathological complete response (pCR) to neoadjuvant therapy (NAT) improves survival. Escalated NATs aim to increase pCR, requiring predictive biomarkers. Tumor-induced T cell exhaustion and senescence impair anti-tumor immunity, but their role in NAT response is unclear. We assessed their potential as pCR biomarkers across BC subtypes. Methods: In this prospective study at Maggiore Hospital (Novara, Italy), blood samples from BC patients were collected before and after NAT. Circulating CD3⁺CD4⁺ and CD3⁺CD8⁺ T cells were profiled by flow cytometry for exhaustion markers (PD-1, LAG-3, TIGIT) and senescence markers (CD57, KLRG-1). Myeloid-derived suppressor cells (MDSCs) were also evaluated and classified into monocytic (M-MDSCs) and polymorphonuclear (PMN-MDSCs), the latter characterized by LOX-1 expression. Systemic inflammation indices (NLR, LMR) were calculated. Results: At baseline, ER⁺ tumors showed high NLR and exhausted CD8⁺PD-1⁺TIGIT⁺ cells; HER2⁺ tumors had more senescent CD8⁺CD57⁺KLRG-1⁺ cells. TN patients had elevated LMR. Lower NLR (OR=0.57, p=0.026) and higher LMR (OR=1.36, p=0.033) correlated with pCR. In HER2⁺ cases, fewer CD8⁺CD28⁻CD57⁻KLRG-1⁺ T cells were linked to better response (OR=0.68, p=0.029). Non-responders had higher NLR and more CD4⁺PD-1⁺TIGIT⁺ cells. ER⁺ non-responders showed increased exhausted and senescent CD4⁺ subsets. Post-NAT, HER2⁺ and TN patients displayed expansions in exhausted and senescent T cells. MDSC levels did not differ by pCR status but showed subtype-specific correlations: LOX-1⁺ PMN-MDSCs correlated with exhausted T cells in ER⁺, M-MDSCs with senescent T cells in HER2⁺, and inversely with LAG-3⁺ cells in TN. Conclusion: T cell exhaustion and senescence predict poor pCR in ER+ and HER2+ BC. Low NLR and high LMR correlate with better response. MDSCs may contribute to immune suppression via subtype-specific interactions with dysfunctional T cells.

Original language	English
Awarding Institution	Universita' degli Studi del Piemonte Orientale "Amedeo Avogadro"
Supervisors/Advisors	Gennari, Alessandra, Supervisor
DOIs	https://doi.org/10.20373/uniupo/openthesis/220663
Publication status	Published - 2025
Externally published	Yes

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

SDG 3 Good Health and Well-being

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10.20373/uniupo/openthesis/220663

https://hdl.handle.net/11579/220663

Cite this

@phdthesis{19faaaf7baf9443ea8bf17a82cc80cea,

title = "Peripheral Blood Immune Cell Profiling as Predictive Biomarkers for Neoadjuvant Therapy Response in Early Breast Cancer Patients",

abstract = "Background: In breast cancer (BC), pathological complete response (pCR) to neoadjuvant therapy (NAT) improves survival. Escalated NATs aim to increase pCR, requiring predictive biomarkers. Tumor-induced T cell exhaustion and senescence impair anti-tumor immunity, but their role in NAT response is unclear. We assessed their potential as pCR biomarkers across BC subtypes. Methods: In this prospective study at Maggiore Hospital (Novara, Italy), blood samples from BC patients were collected before and after NAT. Circulating CD3⁺CD4⁺ and CD3⁺CD8⁺ T cells were profiled by flow cytometry for exhaustion markers (PD-1, LAG-3, TIGIT) and senescence markers (CD57, KLRG-1). Myeloid-derived suppressor cells (MDSCs) were also evaluated and classified into monocytic (M-MDSCs) and polymorphonuclear (PMN-MDSCs), the latter characterized by LOX-1 expression. Systemic inflammation indices (NLR, LMR) were calculated. Results: At baseline, ER⁺ tumors showed high NLR and exhausted CD8⁺PD-1⁺TIGIT⁺ cells; HER2⁺ tumors had more senescent CD8⁺CD57⁺KLRG-1⁺ cells. TN patients had elevated LMR. Lower NLR (OR=0.57, p=0.026) and higher LMR (OR=1.36, p=0.033) correlated with pCR. In HER2⁺ cases, fewer CD8⁺CD28⁻CD57⁻KLRG-1⁺ T cells were linked to better response (OR=0.68, p=0.029). Non-responders had higher NLR and more CD4⁺PD-1⁺TIGIT⁺ cells. ER⁺ non-responders showed increased exhausted and senescent CD4⁺ subsets. Post-NAT, HER2⁺ and TN patients displayed expansions in exhausted and senescent T cells. MDSC levels did not differ by pCR status but showed subtype-specific correlations: LOX-1⁺ PMN-MDSCs correlated with exhausted T cells in ER⁺, M-MDSCs with senescent T cells in HER2⁺, and inversely with LAG-3⁺ cells in TN. Conclusion: T cell exhaustion and senescence predict poor pCR in ER+ and HER2+ BC. Low NLR and high LMR correlate with better response. MDSCs may contribute to immune suppression via subtype-specific interactions with dysfunctional T cells.",

author = "\{Ben Ayed\}, Rahma",

year = "2025",

doi = "10.20373/uniupo/openthesis/220663",

language = "English",

school = "Universita' degli Studi del Piemonte Orientale {"}Amedeo Avogadro{"}",

}

TY - BOOK

T1 - Peripheral Blood Immune Cell Profiling as Predictive Biomarkers for Neoadjuvant Therapy Response in Early Breast Cancer Patients

AU - Ben Ayed, Rahma

PY - 2025

Y1 - 2025

N2 - Background: In breast cancer (BC), pathological complete response (pCR) to neoadjuvant therapy (NAT) improves survival. Escalated NATs aim to increase pCR, requiring predictive biomarkers. Tumor-induced T cell exhaustion and senescence impair anti-tumor immunity, but their role in NAT response is unclear. We assessed their potential as pCR biomarkers across BC subtypes. Methods: In this prospective study at Maggiore Hospital (Novara, Italy), blood samples from BC patients were collected before and after NAT. Circulating CD3⁺CD4⁺ and CD3⁺CD8⁺ T cells were profiled by flow cytometry for exhaustion markers (PD-1, LAG-3, TIGIT) and senescence markers (CD57, KLRG-1). Myeloid-derived suppressor cells (MDSCs) were also evaluated and classified into monocytic (M-MDSCs) and polymorphonuclear (PMN-MDSCs), the latter characterized by LOX-1 expression. Systemic inflammation indices (NLR, LMR) were calculated. Results: At baseline, ER⁺ tumors showed high NLR and exhausted CD8⁺PD-1⁺TIGIT⁺ cells; HER2⁺ tumors had more senescent CD8⁺CD57⁺KLRG-1⁺ cells. TN patients had elevated LMR. Lower NLR (OR=0.57, p=0.026) and higher LMR (OR=1.36, p=0.033) correlated with pCR. In HER2⁺ cases, fewer CD8⁺CD28⁻CD57⁻KLRG-1⁺ T cells were linked to better response (OR=0.68, p=0.029). Non-responders had higher NLR and more CD4⁺PD-1⁺TIGIT⁺ cells. ER⁺ non-responders showed increased exhausted and senescent CD4⁺ subsets. Post-NAT, HER2⁺ and TN patients displayed expansions in exhausted and senescent T cells. MDSC levels did not differ by pCR status but showed subtype-specific correlations: LOX-1⁺ PMN-MDSCs correlated with exhausted T cells in ER⁺, M-MDSCs with senescent T cells in HER2⁺, and inversely with LAG-3⁺ cells in TN. Conclusion: T cell exhaustion and senescence predict poor pCR in ER+ and HER2+ BC. Low NLR and high LMR correlate with better response. MDSCs may contribute to immune suppression via subtype-specific interactions with dysfunctional T cells.

AB - Background: In breast cancer (BC), pathological complete response (pCR) to neoadjuvant therapy (NAT) improves survival. Escalated NATs aim to increase pCR, requiring predictive biomarkers. Tumor-induced T cell exhaustion and senescence impair anti-tumor immunity, but their role in NAT response is unclear. We assessed their potential as pCR biomarkers across BC subtypes. Methods: In this prospective study at Maggiore Hospital (Novara, Italy), blood samples from BC patients were collected before and after NAT. Circulating CD3⁺CD4⁺ and CD3⁺CD8⁺ T cells were profiled by flow cytometry for exhaustion markers (PD-1, LAG-3, TIGIT) and senescence markers (CD57, KLRG-1). Myeloid-derived suppressor cells (MDSCs) were also evaluated and classified into monocytic (M-MDSCs) and polymorphonuclear (PMN-MDSCs), the latter characterized by LOX-1 expression. Systemic inflammation indices (NLR, LMR) were calculated. Results: At baseline, ER⁺ tumors showed high NLR and exhausted CD8⁺PD-1⁺TIGIT⁺ cells; HER2⁺ tumors had more senescent CD8⁺CD57⁺KLRG-1⁺ cells. TN patients had elevated LMR. Lower NLR (OR=0.57, p=0.026) and higher LMR (OR=1.36, p=0.033) correlated with pCR. In HER2⁺ cases, fewer CD8⁺CD28⁻CD57⁻KLRG-1⁺ T cells were linked to better response (OR=0.68, p=0.029). Non-responders had higher NLR and more CD4⁺PD-1⁺TIGIT⁺ cells. ER⁺ non-responders showed increased exhausted and senescent CD4⁺ subsets. Post-NAT, HER2⁺ and TN patients displayed expansions in exhausted and senescent T cells. MDSC levels did not differ by pCR status but showed subtype-specific correlations: LOX-1⁺ PMN-MDSCs correlated with exhausted T cells in ER⁺, M-MDSCs with senescent T cells in HER2⁺, and inversely with LAG-3⁺ cells in TN. Conclusion: T cell exhaustion and senescence predict poor pCR in ER+ and HER2+ BC. Low NLR and high LMR correlate with better response. MDSCs may contribute to immune suppression via subtype-specific interactions with dysfunctional T cells.

UR - https://iris.uniupo.it/handle/11579/220663

U2 - 10.20373/uniupo/openthesis/220663

DO - 10.20373/uniupo/openthesis/220663

M3 - Doctoral Thesis

ER -

Peripheral Blood Immune Cell Profiling as Predictive Biomarkers for Neoadjuvant Therapy Response in Early Breast Cancer Patients

Abstract

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