Abstract 7169: Longitudinal single-cell profiling of breast tumors reveals immune and epigenetic mechanisms of sensitivity and resistance to aromatase inhibitors

Abstract Background. Aromatase inhibitors like letrozole and exemestane play a pivotal role in the treatment algorithms for estrogen receptor (ER) positive breast cancer in all phases of the disease. However, resistance to such therapies is not fully understood and remains a major clinical challenge. Methods. To investigate the mechanisms of sensitivity and resistance to aromatase inhibitors in ER-positive HER2-negative breast cancer, we conducted single-cell RNA (scRNA-seq), T cell receptor (scTCR-seq), and B cell receptor (scBCR-seq) sequencing on tumor biopsies obtained before and during neoadjuvant therapy with letrozole and exemestane given in a randomized sequence for 6 months. Results. We examined 472,737 single cells from 73 biospecimens collected at baseline (n=25), at mid-therapy (n=24) and at the end of neoadjuvant treatment (n=24). We identified transcription start site usage at single cell level to study the role of enhancer activity in the evolution of breast tumors under treatment pressure. Malignant cells that were sensitive to treatment exhibited elevated ER-signaling and increased activity in enhancers containing ER binding sites. Conversely, resistant malignant cells showed upregulated androgen receptor (AR) signaling, cellular de-differentiation, and neuroendocrine-like characteristics. The activity of AR cis-regulome increased under treatment in non-responders, suggesting a role of epigenetic modifications in treatment resistance. Treatment-naïve tumor microenvironment was predictive of response. Non-responders displayed high proportions of naive lymphoid and undifferentiated myeloid cells, indicating an ineffective immune landscape. In contrast, responders were characterized by clonal expansion of T cells. Conclusions. Taken together our longitudinal single-cell analyses delineate the genetic, epigenetic and cellular mechanisms that drive sensitivity and resistance to aromatase inhibitors in ER positive breast cancer, opening avenues for improved treatment strategies. Footnotes. Ilayda Altinönder and Villads Winton are shared first authors. Jürgen Geisler, Xavier Tekpli have jointly supervised this work. Citation Format: Ilayda Altinönder, Villads Winton, Quy Khang Le, Marie Fongaard, Paal M. Bjornstad, Elin Edda Seland Agustsdottir, Stephanie Geisler, Kamilla Fjermeros, Manouchehr Seyedzadeh, Unn-Cathrin Buvarp, Marianne Lyngra, Arnoldo Frigessi, Diether Lambrechts, Vessela N. Kristensen, Anthony Mathelier, Victor Greiff, Jürgen Geisler, Xavier Tekpli. Longitudinal single-cell profiling of breast tumors reveals immune and epigenetic mechanisms of sensitivity and resistance to aromatase inhibitors abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 1 (Regular Abstracts); 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86(7 Suppl):Abstract nr 7169.