TY - JOUR
T1 - Targeting resistance to radiation-immunotherapy in cold HNSCCs by modulating the Treg-dendritic cell axis
AU - Knitz, Michael W.
AU - Bickett, Thomas E.
AU - Darragh, Laurel B.
AU - Oweida, Ayman J.
AU - Bhatia, Shilpa
AU - Van Court, Benjamin
AU - Bhuvane, Shiv
AU - Piper, Miles
AU - Gadwa, Jacob
AU - Mueller, Adam C.
AU - Nguyen, Diemmy
AU - Nangia, Varuna
AU - Osborne, Douglas G.
AU - Bai, Xiyuan
AU - Ferrara, Sarah E.
AU - Boss, Mary Keara
AU - Goodspeed, Andrew
AU - Burchill, Matthew A.
AU - Tamburini, Beth A.Jirón
AU - Chan, Edward D.
AU - Pickering, Curtis R.
AU - Clambey, Eric T.
AU - Karam, Sana D.
N1 - Publisher Copyright:
© Author(s) 2021.
PY - 2021/4/21
Y1 - 2021/4/21
N2 - Background Numerous trials combining radiation therapy (RT) and immunotherapy in head and neck squamous cell carcinoma (HNSCC) are failing. Using preclinical immune cold models of HNSCC resistant to RT-immune checkpoint inhibitors, we investigate therapeutic approaches of overcoming such resistance by examining the differential microenvironmental response to RT. Methods We subjected two HPV-negative orthotopic mouse models of HNSCC to combination RT, regulatory T cells (Treg) depletion, and/or CD137 agonism. Tumor growth was measured and intratumorous and lymph node immune populations were compared among treatment groups. Human gene sets, genetically engineered mouse models DEREG and BATF3-/-, flow and time-of-flight cytometry, RNA-Seq, Treg adoptive transfer studies, and in vitro experiments were used to further evaluate the role of dendritic cells (DCs) and Tregs in these treatments. Results In MOC2 orthotopic tumors, we find no therapeutic benefit to targeting classically defined immunosuppressive myeloids, which increase with RT. In these radioresistant tumors, supplementing combination RT and Treg depletion with anti-CD137 agonism stimulates CD103 + DC activation in tumor-draining lymph nodes as characterized by increases in CD80 + and CCR7 + DCs, resulting in a CD8 T cell-dependent response. Simultaneously, Tregs are reprogrammed to an effector phenotype demonstrated by increases in interferon 3 +, tumor necrosis factorα +, PI3K +, pAKT + and Eomes + populations as well as decreases in CTLA4 + and NRP-1 + populations. Tumor eradication is observed when RT is increased to an 8 Gy x 5 hypofractionated regimen and combined with anti-CD25+ anti-CD137 treatment. In a human gene set from oral squamous cell carcinoma tumors, high Treg number is associated with earlier recurrence. Conclusions Regulating Treg functionality and DC activation status within the lymph node is critical for generating a T cell effector response in these highly radioresistant tumors. These findings underscore the plasticity of Tregs and represent a new therapeutic opportunity for reprogramming the tumor microenvironment in HNSCCs resistant to conventional radioimmunotherapy approaches.
AB - Background Numerous trials combining radiation therapy (RT) and immunotherapy in head and neck squamous cell carcinoma (HNSCC) are failing. Using preclinical immune cold models of HNSCC resistant to RT-immune checkpoint inhibitors, we investigate therapeutic approaches of overcoming such resistance by examining the differential microenvironmental response to RT. Methods We subjected two HPV-negative orthotopic mouse models of HNSCC to combination RT, regulatory T cells (Treg) depletion, and/or CD137 agonism. Tumor growth was measured and intratumorous and lymph node immune populations were compared among treatment groups. Human gene sets, genetically engineered mouse models DEREG and BATF3-/-, flow and time-of-flight cytometry, RNA-Seq, Treg adoptive transfer studies, and in vitro experiments were used to further evaluate the role of dendritic cells (DCs) and Tregs in these treatments. Results In MOC2 orthotopic tumors, we find no therapeutic benefit to targeting classically defined immunosuppressive myeloids, which increase with RT. In these radioresistant tumors, supplementing combination RT and Treg depletion with anti-CD137 agonism stimulates CD103 + DC activation in tumor-draining lymph nodes as characterized by increases in CD80 + and CCR7 + DCs, resulting in a CD8 T cell-dependent response. Simultaneously, Tregs are reprogrammed to an effector phenotype demonstrated by increases in interferon 3 +, tumor necrosis factorα +, PI3K +, pAKT + and Eomes + populations as well as decreases in CTLA4 + and NRP-1 + populations. Tumor eradication is observed when RT is increased to an 8 Gy x 5 hypofractionated regimen and combined with anti-CD25+ anti-CD137 treatment. In a human gene set from oral squamous cell carcinoma tumors, high Treg number is associated with earlier recurrence. Conclusions Regulating Treg functionality and DC activation status within the lymph node is critical for generating a T cell effector response in these highly radioresistant tumors. These findings underscore the plasticity of Tregs and represent a new therapeutic opportunity for reprogramming the tumor microenvironment in HNSCCs resistant to conventional radioimmunotherapy approaches.
KW - costimulatory and inhibitory t-cell receptors
KW - dendritic cells
KW - head and neck neoplasms
KW - radioimmunotherapy
KW - t-lymphocytes
UR - http://www.scopus.com/inward/record.url?scp=85104743516&partnerID=8YFLogxK
U2 - 10.1136/jitc-2020-001955
DO - 10.1136/jitc-2020-001955
M3 - Article
C2 - 33883256
AN - SCOPUS:85104743516
SN - 2051-1426
VL - 9
JO - Journal for ImmunoTherapy of Cancer
JF - Journal for ImmunoTherapy of Cancer
IS - 4
M1 - e001955
ER -