Local delivery of cell surface-targeted immunocytokines programs systemic antitumor immunity

局部递送靶向细胞表面的免疫细胞因子可诱导全身抗肿瘤免疫。

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作者:Luciano Santollani ,Laura Maiorino ,Yiming J Zhang ,Joseph R Palmeri ,Jordan A Stinson ,Lauren R Duhamel ,Kashif Qureshi ,Jack R Suggs ,Owen T Porth ,William Pinney 3rd ,Riyam Al Msari ,Agnes A Walsh ,K Dane Wittrup ,Darrell J Irvine

Abstract

Systemically administered cytokines are potent immunotherapeutics but can cause severe dose-limiting toxicities. To overcome this challenge, cytokines have been engineered for intratumoral retention after local delivery. However, despite inducing regression of treated lesions, tumor-localized cytokines often elicit only modest responses at distal untreated tumors. In the present study, we report a localized cytokine therapy that safely elicits systemic antitumor immunity by targeting the ubiquitous leukocyte receptor CD45. CD45-targeted immunocytokines have lower internalization rates relative to wild-type counterparts, leading to sustained downstream cis and trans signaling between lymphocytes. A single intratumoral dose of αCD45-interleukin (IL)-12 followed by a single dose of αCD45-IL-15 eradicated treated tumors and untreated distal lesions in multiple syngeneic mouse tumor models without toxicity. Mechanistically, CD45-targeted cytokines reprogrammed tumor-specific CD8+ T cells in the tumor-draining lymph nodes to have an antiviral transcriptional signature. CD45 anchoring represents a broad platform for protein retention by host immune cells for use in immunotherapy.

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