Potentiating Antitumor Efficacy Through Radiation and Sustained Intratumoral Delivery of Anti-CD40 and Anti-PDL1

Hsuan Chen Liu; Dixita I. Viswanath; Federica Pesaresi; Yitian Xu; Licheng Zhang; Nicola Di Trani; Jesus Paez-Mayorga; Nathanael Hernandez; Yu Wang; Donald R. Erm; Jeremy Ho; Antonia Susnjar; Xuewu Liu; Sandra Demaria; Shu Hsia Chen; Bin S. Teh; Edward Brian Butler; Corrine Ying Xuan Chua; Alessandro Grattoni

doi:10.1016/j.ijrobp.2020.07.2326

Potentiating Antitumor Efficacy Through Radiation and Sustained Intratumoral Delivery of Anti-CD40 and Anti-PDL1

Hsuan Chen Liu, Dixita I. Viswanath, Federica Pesaresi, Yitian Xu, Licheng Zhang, Nicola Di Trani, Jesus Paez-Mayorga, Nathanael Hernandez, Yu Wang, Donald R. Erm, Jeremy Ho, Antonia Susnjar, Xuewu Liu, Sandra Demaria, Shu Hsia Chen, Bin S. Teh, Edward Brian Butler, Corrine Ying Xuan Chua, Alessandro Grattoni

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35 Scopus citations

Abstract

Purpose: Mounting evidence demonstrates that combining radiation therapy (RT) with immunotherapy can reduce tumor burden in a subset of patients. However, conventional systemic delivery of immunotherapeutics is often associated with significant adverse effects, which force treatment cessation. The aim of this study was to investigate a minimally invasive therapeutics delivery approach to improve clinical response while attenuating toxicity. Methods and Materials: We used a nanofluidic drug-eluting seed (NDES) for sustained intratumoral delivery of combinational antibodies CD40 and PDL1. To enhance immune and tumor response, we combined the NDES intratumoral platform with RT to treat the 4T1 murine model of advanced triple negative breast cancer. We compared the efficacy of NDES against intraperitoneal administration, which mimics conventional systemic treatment. Tumor growth was recorded, and local and systemic immune responses were assessed via imaging mass cytometry and flow cytometry. Livers and lungs were histologically analyzed for evaluation of toxicity and metastasis, respectively. Results: The combination of RT and sustained intratumoral immunotherapy delivery of CD40 and PDL1 via NDES (NDES CD40/PDL1) showed an increase in both local and systemic immune response. In combination with RT, NDES CD40/PDL1 achieved significant tumor burden reduction and liver inflammation mitigation compared with systemic treatment. Importantly, our treatment strategy boosted the abscopal effect toward attenuating lung metastatic burden. Conclusions: Overall, our study demonstrated superior efficacy of combination treatment with RT and sustained intratumoral immunotherapy via NDES, offering promise for improving therapeutic index and clinical response.

Original language	English (US)
Pages (from-to)	492-506
Number of pages	15
Journal	International Journal of Radiation Oncology Biology Physics
Volume	110
Issue number	2
DOIs	https://doi.org/10.1016/j.ijrobp.2020.07.2326
State	Published - Jun 1 2021

ASJC Scopus subject areas

Radiation
Oncology
Radiology Nuclear Medicine and imaging
Cancer Research

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10.1016/j.ijrobp.2020.07.2326

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Liu, H. C., Viswanath, D. I., Pesaresi, F., Xu, Y., Zhang, L., Di Trani, N., Paez-Mayorga, J., Hernandez, N., Wang, Y., Erm, D. R., Ho, J., Susnjar, A., Liu, X., Demaria, S., Chen, S. H., Teh, B. S., Butler, E. B., Xuan Chua, C. Y., & Grattoni, A. (2021). Potentiating Antitumor Efficacy Through Radiation and Sustained Intratumoral Delivery of Anti-CD40 and Anti-PDL1. International Journal of Radiation Oncology Biology Physics, 110(2), 492-506. https://doi.org/10.1016/j.ijrobp.2020.07.2326

Liu, HC, Viswanath, DI, Pesaresi, F, Xu, Y, Zhang, L, Di Trani, N, Paez-Mayorga, J, Hernandez, N, Wang, Y, Erm, DR, Ho, J, Susnjar, A, Liu, X, Demaria, S, Chen, SH , Teh, BS , Butler, EB , Xuan Chua, CY & Grattoni, A 2021, 'Potentiating Antitumor Efficacy Through Radiation and Sustained Intratumoral Delivery of Anti-CD40 and Anti-PDL1', International Journal of Radiation Oncology Biology Physics, vol. 110, no. 2, pp. 492-506. https://doi.org/10.1016/j.ijrobp.2020.07.2326

@article{04636e35f4b54aa4a0087885190bdcf5,

title = "Potentiating Antitumor Efficacy Through Radiation and Sustained Intratumoral Delivery of Anti-CD40 and Anti-PDL1",

abstract = "Purpose: Mounting evidence demonstrates that combining radiation therapy (RT) with immunotherapy can reduce tumor burden in a subset of patients. However, conventional systemic delivery of immunotherapeutics is often associated with significant adverse effects, which force treatment cessation. The aim of this study was to investigate a minimally invasive therapeutics delivery approach to improve clinical response while attenuating toxicity. Methods and Materials: We used a nanofluidic drug-eluting seed (NDES) for sustained intratumoral delivery of combinational antibodies CD40 and PDL1. To enhance immune and tumor response, we combined the NDES intratumoral platform with RT to treat the 4T1 murine model of advanced triple negative breast cancer. We compared the efficacy of NDES against intraperitoneal administration, which mimics conventional systemic treatment. Tumor growth was recorded, and local and systemic immune responses were assessed via imaging mass cytometry and flow cytometry. Livers and lungs were histologically analyzed for evaluation of toxicity and metastasis, respectively. Results: The combination of RT and sustained intratumoral immunotherapy delivery of CD40 and PDL1 via NDES (NDES CD40/PDL1) showed an increase in both local and systemic immune response. In combination with RT, NDES CD40/PDL1 achieved significant tumor burden reduction and liver inflammation mitigation compared with systemic treatment. Importantly, our treatment strategy boosted the abscopal effect toward attenuating lung metastatic burden. Conclusions: Overall, our study demonstrated superior efficacy of combination treatment with RT and sustained intratumoral immunotherapy via NDES, offering promise for improving therapeutic index and clinical response.",

author = "Liu, {Hsuan Chen} and Viswanath, {Dixita I.} and Federica Pesaresi and Yitian Xu and Licheng Zhang and {Di Trani}, Nicola and Jesus Paez-Mayorga and Nathanael Hernandez and Yu Wang and Erm, {Donald R.} and Jeremy Ho and Antonia Susnjar and Xuewu Liu and Sandra Demaria and Chen, {Shu Hsia} and Teh, {Bin S.} and Butler, {Edward Brian} and {Xuan Chua}, {Corrine Ying} and Alessandro Grattoni",

note = "Funding Information: We thank Dr Jianhua (James) Gu from the electron microscopy core; Dr Andreana L. Rivera, Yulan Ren, and Sandra Steptoe from the research pathology core of HMRI; Dr David L. Haviland and Nicole Vaughn from the Flow Cytometry Core of HMRI; and ImmunoMonitoring Core at the Immunotherapy Center and Cancer Center, HMRI. Funding support from the Nancy Owens Breast Cancer Foundation (A.G.), Golfers Against Cancer (A.G.), and the development of the nanochannel membrane was funded by NIH-NIGMS R01GM127558 (A.G.). A.G. and his research group received support through the Frank J. and Jean Raymond Centennial Chair Endowment. This study was partially supported by Emily Hermann endowed chair fund to S.-H.C., and the following grants to SHC (NIH grant nos. R01CA127483, R01CA204191, R01CA208703, Houston Methodist Cancer Center 2019 High Impact in Cancer Research Grant Award) and DoD grant no. BC191397P1 (S.-H.C. & A.G.). Disclosures: X.L. reports a patent null pending. S.D. reports grants from Nanobiotix, grants and other from Lytix Biopharma, other from EMD Serono, and other from Mersana Therapeutics, outside the submitted work. A.G. reports a U.S. patent application no. 62/161,986 pending. Funding Information: Funding support from the Nancy Owens Breast Cancer Foundation (A.G.), Golfers Against Cancer (A.G.), and the development of the nanochannel membrane was funded by NIH-NIGMS R01GM127558 (A.G.). A.G. and his research group received support through the Frank J. and Jean Raymond Centennial Chair Endowment. This study was partially supported by Emily Hermann endowed chair fund to S.-H.C., and the following grants to SHC (NIH grant nos. R01CA127483, R01CA204191, R01CA208703, Houston Methodist Cancer Center 2019 High Impact in Cancer Research Grant Award) and DoD grant no. BC191397P1 (S.-H.C. & A.G.). Publisher Copyright: {\textcopyright} 2020 Elsevier Inc.",

year = "2021",

month = jun,

day = "1",

doi = "10.1016/j.ijrobp.2020.07.2326",

language = "English (US)",

volume = "110",

pages = "492--506",

journal = "International Journal of Radiation Oncology Biology Physics",

issn = "0360-3016",

publisher = "Elsevier",

number = "2",

}

TY - JOUR

T1 - Potentiating Antitumor Efficacy Through Radiation and Sustained Intratumoral Delivery of Anti-CD40 and Anti-PDL1

AU - Liu, Hsuan Chen

AU - Viswanath, Dixita I.

AU - Pesaresi, Federica

AU - Xu, Yitian

AU - Zhang, Licheng

AU - Di Trani, Nicola

AU - Paez-Mayorga, Jesus

AU - Hernandez, Nathanael

AU - Wang, Yu

AU - Erm, Donald R.

AU - Ho, Jeremy

AU - Susnjar, Antonia

AU - Liu, Xuewu

AU - Demaria, Sandra

AU - Chen, Shu Hsia

AU - Teh, Bin S.

AU - Butler, Edward Brian

AU - Xuan Chua, Corrine Ying

AU - Grattoni, Alessandro

N1 - Funding Information: We thank Dr Jianhua (James) Gu from the electron microscopy core; Dr Andreana L. Rivera, Yulan Ren, and Sandra Steptoe from the research pathology core of HMRI; Dr David L. Haviland and Nicole Vaughn from the Flow Cytometry Core of HMRI; and ImmunoMonitoring Core at the Immunotherapy Center and Cancer Center, HMRI. Funding support from the Nancy Owens Breast Cancer Foundation (A.G.), Golfers Against Cancer (A.G.), and the development of the nanochannel membrane was funded by NIH-NIGMS R01GM127558 (A.G.). A.G. and his research group received support through the Frank J. and Jean Raymond Centennial Chair Endowment. This study was partially supported by Emily Hermann endowed chair fund to S.-H.C., and the following grants to SHC (NIH grant nos. R01CA127483, R01CA204191, R01CA208703, Houston Methodist Cancer Center 2019 High Impact in Cancer Research Grant Award) and DoD grant no. BC191397P1 (S.-H.C. & A.G.). Disclosures: X.L. reports a patent null pending. S.D. reports grants from Nanobiotix, grants and other from Lytix Biopharma, other from EMD Serono, and other from Mersana Therapeutics, outside the submitted work. A.G. reports a U.S. patent application no. 62/161,986 pending. Funding Information: Funding support from the Nancy Owens Breast Cancer Foundation (A.G.), Golfers Against Cancer (A.G.), and the development of the nanochannel membrane was funded by NIH-NIGMS R01GM127558 (A.G.). A.G. and his research group received support through the Frank J. and Jean Raymond Centennial Chair Endowment. This study was partially supported by Emily Hermann endowed chair fund to S.-H.C., and the following grants to SHC (NIH grant nos. R01CA127483, R01CA204191, R01CA208703, Houston Methodist Cancer Center 2019 High Impact in Cancer Research Grant Award) and DoD grant no. BC191397P1 (S.-H.C. & A.G.). Publisher Copyright: © 2020 Elsevier Inc.

PY - 2021/6/1

Y1 - 2021/6/1

N2 - Purpose: Mounting evidence demonstrates that combining radiation therapy (RT) with immunotherapy can reduce tumor burden in a subset of patients. However, conventional systemic delivery of immunotherapeutics is often associated with significant adverse effects, which force treatment cessation. The aim of this study was to investigate a minimally invasive therapeutics delivery approach to improve clinical response while attenuating toxicity. Methods and Materials: We used a nanofluidic drug-eluting seed (NDES) for sustained intratumoral delivery of combinational antibodies CD40 and PDL1. To enhance immune and tumor response, we combined the NDES intratumoral platform with RT to treat the 4T1 murine model of advanced triple negative breast cancer. We compared the efficacy of NDES against intraperitoneal administration, which mimics conventional systemic treatment. Tumor growth was recorded, and local and systemic immune responses were assessed via imaging mass cytometry and flow cytometry. Livers and lungs were histologically analyzed for evaluation of toxicity and metastasis, respectively. Results: The combination of RT and sustained intratumoral immunotherapy delivery of CD40 and PDL1 via NDES (NDES CD40/PDL1) showed an increase in both local and systemic immune response. In combination with RT, NDES CD40/PDL1 achieved significant tumor burden reduction and liver inflammation mitigation compared with systemic treatment. Importantly, our treatment strategy boosted the abscopal effect toward attenuating lung metastatic burden. Conclusions: Overall, our study demonstrated superior efficacy of combination treatment with RT and sustained intratumoral immunotherapy via NDES, offering promise for improving therapeutic index and clinical response.

AB - Purpose: Mounting evidence demonstrates that combining radiation therapy (RT) with immunotherapy can reduce tumor burden in a subset of patients. However, conventional systemic delivery of immunotherapeutics is often associated with significant adverse effects, which force treatment cessation. The aim of this study was to investigate a minimally invasive therapeutics delivery approach to improve clinical response while attenuating toxicity. Methods and Materials: We used a nanofluidic drug-eluting seed (NDES) for sustained intratumoral delivery of combinational antibodies CD40 and PDL1. To enhance immune and tumor response, we combined the NDES intratumoral platform with RT to treat the 4T1 murine model of advanced triple negative breast cancer. We compared the efficacy of NDES against intraperitoneal administration, which mimics conventional systemic treatment. Tumor growth was recorded, and local and systemic immune responses were assessed via imaging mass cytometry and flow cytometry. Livers and lungs were histologically analyzed for evaluation of toxicity and metastasis, respectively. Results: The combination of RT and sustained intratumoral immunotherapy delivery of CD40 and PDL1 via NDES (NDES CD40/PDL1) showed an increase in both local and systemic immune response. In combination with RT, NDES CD40/PDL1 achieved significant tumor burden reduction and liver inflammation mitigation compared with systemic treatment. Importantly, our treatment strategy boosted the abscopal effect toward attenuating lung metastatic burden. Conclusions: Overall, our study demonstrated superior efficacy of combination treatment with RT and sustained intratumoral immunotherapy via NDES, offering promise for improving therapeutic index and clinical response.

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AN - SCOPUS:85090158115

SN - 0360-3016

VL - 110

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JO - International Journal of Radiation Oncology Biology Physics

JF - International Journal of Radiation Oncology Biology Physics

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ER -

Potentiating Antitumor Efficacy Through Radiation and Sustained Intratumoral Delivery of Anti-CD40 and Anti-PDL1

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