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An intra-tumoral niche maintains and differentiates stem-like CD8 T cells

Author

Listed:
  • Caroline S. Jansen

    (Emory University School of Medicine)

  • Nataliya Prokhnevska

    (Emory University School of Medicine)

  • Viraj A. Master

    (Emory University School of Medicine
    Winship Cancer Institute of Emory University)

  • Martin G. Sanda

    (Emory University School of Medicine
    Winship Cancer Institute of Emory University)

  • Jennifer W. Carlisle

    (Winship Cancer Institute of Emory University
    Emory University School of Medicine)

  • Mehmet Asim Bilen

    (Winship Cancer Institute of Emory University
    Emory University School of Medicine)

  • Maria Cardenas

    (Emory University School of Medicine)

  • Scott Wilkinson

    (National Cancer Institute)

  • Ross Lake

    (National Cancer Institute)

  • Adam G. Sowalsky

    (National Cancer Institute)

  • Rajesh M. Valanparambil

    (Emory University School of Medicine
    Emory University School of Medicine)

  • William H. Hudson

    (Emory University School of Medicine
    Emory University School of Medicine)

  • Donald McGuire

    (Emory University School of Medicine
    Emory University School of Medicine)

  • Kevin Melnick

    (Emory University School of Medicine)

  • Amir I. Khan

    (Emory University School of Medicine)

  • Kyu Kim

    (Emory University School of Medicine)

  • Yun Min Chang

    (Emory University School of Medicine)

  • Alice Kim

    (Emory University School of Medicine)

  • Christopher P. Filson

    (Emory University School of Medicine
    Winship Cancer Institute of Emory University)

  • Mehrdad Alemozaffar

    (Emory University School of Medicine
    Winship Cancer Institute of Emory University)

  • Adeboye O. Osunkoya

    (Emory University School of Medicine
    Winship Cancer Institute of Emory University
    Emory University School of Medicine)

  • Patrick Mullane

    (Emory University School of Medicine)

  • Carla Ellis

    (Emory University School of Medicine)

  • Rama Akondy

    (Emory University School of Medicine
    Emory University School of Medicine)

  • Se Jin Im

    (Emory University School of Medicine
    Emory University School of Medicine)

  • Alice O. Kamphorst

    (Icahn School of Medicine at Mount Sinai)

  • Adriana Reyes

    (Emory University School of Medicine)

  • Yuan Liu

    (Winship Cancer Institute of Emory University
    Emory University)

  • Haydn Kissick

    (Emory University School of Medicine
    Winship Cancer Institute of Emory University
    Emory University School of Medicine
    Emory University School of Medicine)

Abstract

Tumour-infiltrating lymphocytes are associated with a survival benefit in several tumour types and with the response to immunotherapy1–8. However, the reason some tumours have high CD8 T cell infiltration while others do not remains unclear. Here we investigate the requirements for maintaining a CD8 T cell response against human cancer. We find that CD8 T cells within tumours consist of distinct populations of terminally differentiated and stem-like cells. On proliferation, stem-like CD8 T cells give rise to more terminally differentiated, effector-molecule-expressing daughter cells. For many T cells to infiltrate the tumour, it is critical that this effector differentiation process occur. In addition, we show that these stem-like T cells reside in dense antigen-presenting-cell niches within the tumour, and that tumours that fail to form these structures are not extensively infiltrated by T cells. Patients with progressive disease lack these immune niches, suggesting that niche breakdown may be a key mechanism of immune escape.

Suggested Citation

  • Caroline S. Jansen & Nataliya Prokhnevska & Viraj A. Master & Martin G. Sanda & Jennifer W. Carlisle & Mehmet Asim Bilen & Maria Cardenas & Scott Wilkinson & Ross Lake & Adam G. Sowalsky & Rajesh M. V, 2019. "An intra-tumoral niche maintains and differentiates stem-like CD8 T cells," Nature, Nature, vol. 576(7787), pages 465-470, December.
    • Handle: RePEc:nat:nature:v:576:y:2019:i:7787:d:10.1038_s41586-019-1836-5
    DOI: 10.1038/s41586-019-1836-5
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    Cited by:

    1. Alessandra Castiglioni & Yagai Yang & Katherine Williams & Alvin Gogineni & Ryan S. Lane & Amber W. Wang & Justin A. Shyer & Zhe Zhang & Stephanie Mittman & Alan Gutierrez & Jillian L. Astarita & Minh, 2023. "Combined PD-L1/TGFβ blockade allows expansion and differentiation of stem cell-like CD8 T cells in immune excluded tumors," Nature Communications, Nature, vol. 14(1), pages 1-19, December.
    2. Siqi Li & Kun Li & Kang Wang & Haoyuan Yu & Xiangyang Wang & Mengchen Shi & Zhixing Liang & Zhou Yang & Yongwei Hu & Yang Li & Wei Liu & Hua Li & Shuqun Cheng & Linsen Ye & Yang Yang, 2023. "Low-dose radiotherapy combined with dual PD-L1 and VEGFA blockade elicits antitumor response in hepatocellular carcinoma mediated by activated intratumoral CD8+ exhausted-like T cells," Nature Communications, Nature, vol. 14(1), pages 1-21, December.
    3. Solhwi Lee & Kunhee Lee & Hyeonjin Bae & Kyungmin Lee & Junghwa Lee & Junhui Ma & Ye Ji Lee & Bo Ryeong Lee & Woong-Yang Park & Se Jin Im, 2023. "Defining a TCF1-expressing progenitor allogeneic CD8+ T cell subset in acute graft-versus-host disease," Nature Communications, Nature, vol. 14(1), pages 1-15, December.
    4. Xiaoqiong Zhang & Zhaohan Wei & Tuying Yong & Shiyu Li & Nana Bie & Jianye Li & Xin Li & Haojie Liu & Hang Xu & Yuchen Yan & Bixiang Zhang & Xiaoping Chen & Xiangliang Yang & Lu Gan, 2023. "Cell microparticles loaded with tumor antigen and resiquimod reprogram tumor-associated macrophages and promote stem-like CD8+ T cells to boost anti-PD-1 therapy," Nature Communications, Nature, vol. 14(1), pages 1-22, December.
    5. Hussein A. Abbas & Dapeng Hao & Katarzyna Tomczak & Praveen Barrodia & Jin Seon Im & Patrick K. Reville & Zoe Alaniz & Wei Wang & Ruiping Wang & Feng Wang & Gheath Al-Atrash & Koichi Takahashi & Jing , 2021. "Single cell T cell landscape and T cell receptor repertoire profiling of AML in context of PD-1 blockade therapy," Nature Communications, Nature, vol. 12(1), pages 1-13, December.
    6. Jia-Cheng Lu & Lei-Lei Wu & Yi-Ning Sun & Xiao-Yong Huang & Chao Gao & Xiao-Jun Guo & Hai-Ying Zeng & Xu-Dong Qu & Yi Chen & Dong Wu & Yan-Zi Pei & Xian-Long Meng & Yi-Min Zheng & Chen Liang & Peng-Fe, 2024. "Macro CD5L+ deteriorates CD8+T cells exhaustion and impairs combination of Gemcitabine-Oxaliplatin-Lenvatinib-anti-PD1 therapy in intrahepatic cholangiocarcinoma," Nature Communications, Nature, vol. 15(1), pages 1-23, December.
    7. Sruthi Ravindranathan & Tenzin Passang & Jian-Ming Li & Shuhua Wang & Rohan Dhamsania & Michael Brandon Ware & Mohammad Y. Zaidi & Jingru Zhu & Maria Cardenas & Yuan Liu & Sanjeev Gumber & Brian Robin, 2022. "Targeting vasoactive intestinal peptide-mediated signaling enhances response to immune checkpoint therapy in pancreatic ductal adenocarcinoma," Nature Communications, Nature, vol. 13(1), pages 1-18, December.
    8. Lei Guan & Bin Wu & Ting Li & Lynn A. Beer & Gaurav Sharma & Mingyue Li & Chin Nien Lee & Shujing Liu & Changsong Yang & Lili Huang & Dennie T. Frederick & Genevieve M. Boland & Guangcan Shao & Tatyan, 2022. "HRS phosphorylation drives immunosuppressive exosome secretion and restricts CD8+ T-cell infiltration into tumors," Nature Communications, Nature, vol. 13(1), pages 1-12, December.

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