Bone marrow adipocytes induce cancer‐associated fibroblasts and immune evasion, enhancing invasion and drug resistance

Author:

Sato Shinya123ORCID,Hiruma Toru4,Koizumi Mitsuyuki5,Yoshihara Mitsuyo1,Nakamura Yoshiyasu1,Tadokoro Hiroko2,Motomatsu Sadako1,Yamanaka Takashi6,Washimi Kota3,Okubo Yoichiro3,Yoshioka Emi3,Kasajima Rika2,Yamashita Toshinari6,Kishida Takeshi5,Yokose Tomoyuki3,Miyagi Yohei2

Affiliation:

1. Morphological Information Analysis Laboratory Kanagawa Cancer Center Research Institute Yokohama Japan

2. Molecular Pathology and Genetics Division Kanagawa Cancer Center Research Institute Yokohama Japan

3. Department of Pathology Kanagawa Cancer Center Yokohama Japan

4. Department of Musculoskeletal Tumor Surgery Kanagawa Cancer Center Yokohama Japan

5. Department of Urology Kanagawa Cancer Center Yokohama Japan

6. Department of Breast and Endocrine Surgery Kanagawa Cancer Center Yokohama Japan

Abstract

AbstractBone metastasis occurs frequently in cancer patients. Conventional therapies have limited therapeutic outcomes, and thus, exploring the mechanisms of cancer progression in bone metastasis is important to develop new effective therapies. In the bone microenvironment, adipocytes are the major stromal cells that interact with cancer cells during bone metastasis. However, the comprehensive functions of bone marrow adipocytes in cancer progression are not yet fully understood. To address this, we investigated the role of bone marrow adipocytes on cancer cells, by focusing on an invasive front that reflects the direct effects of stromal cells on cancer. In comprehensive histopathological and genetic analysis using bone metastasis specimens, we examined invasive fronts in bone metastasis and compared invasive fronts with adipocyte‐rich bone marrow (adipo‐BM) to those with hematopoietic cell‐rich bone marrow (hemato‐BM) as a normal counterpart of adipocytes. We found morphological complexity of the invasive front with adipo‐BM was significantly higher than that with hemato‐BM. Based on immunohistochemistry, the invasive front with adipo‐BM comparatively had a significantly increased cancer‐associated fibroblast (CAF) marker‐positive area and lower density of CD8+lymphocytes compared to that with hemato‐BM. RNA sequencing analysis of primary and bone metastasis cancer revealed that bone metastasized cancer cells acquired drug resistance‐related gene expression phenotypes. Clearly, these findings indicate that bone marrow adipocytes provide a favorable tumor microenvironment for cancer invasion and therapeutic resistance of bone metastasized cancers through CAF induction and immune evasion, providing a potential target for the treatment of bone metastasis.

Funder

Foundation for Promotion of Cancer Research

Japan Society for the Promotion of Science

Takeda Medical Research Foundation

Publisher

Wiley

Subject

Cancer Research,Oncology,General Medicine

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