Chemotherapy induces dynamic immune responses in breast cancers that impact treatment outcome

Author:

Park Yeon HeeORCID,Lal Samir,Lee Jeong Eon,Choi Yoon-LaORCID,Wen JiORCID,Ram SripadORCID,Ding Ying,Lee Soo-Hyeon,Powell Eric,Lee Se Kyung,Yu Jong Han,Ching Keith A.,Nam Jae-Yong,Kim Seok Won,Nam Seok Jin,Kim Ji-Yeon,Cho Soo YounORCID,Park SeriORCID,Kim JinhoORCID,Hwang Soohyn,Kim Yu Jin,Bonato Vinicius,Fernandez Diane,Deng Shibing,Wang Shuoguo,Shin Hyuntae,Kang Eun-Suk,Park Woong-Yang,Rejto Paul A.,Bienkowska Jadwiga,Kan ZhengyanORCID

Abstract

AbstractTo elucidate the effects of neoadjuvant chemotherapy (NAC), we conduct whole transcriptome profiling coupled with histopathology analyses of a longitudinal breast cancer cohort of 146 patients including 110 pairs of serial tumor biopsies collected before treatment, after the first cycle of treatment and at the time of surgery. Here, we show that cytotoxic chemotherapies induce dynamic changes in the tumor immune microenvironment that vary by subtype and pathologic response. Just one cycle of treatment induces an immune stimulatory microenvironment harboring more tumor infiltrating lymphocytes (TILs) and up-regulation of inflammatory signatures predictive of response to anti-PD1 therapies while residual tumors are immune suppressed at end-of-treatment compared to the baseline. Increases in TILs and CD8+ T cell proportions in response to NAC are independently associated with pathologic complete response. Further, on-treatment immune response is more predictive of treatment outcome than immune features in paired baseline samples although these are strongly correlated.

Funder

National Research Foundation of Korea

Ministry of Health and Welfare

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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