Immunotherapy Converts Nonimmunogenic Pancreatic Tumors into Immunogenic Foci of Immune Regulation

Eric R. Lutz; Annie A. Wu; Elaine Bigelow; Rajni Sharma; Guanglan Mo; Kevin C. Soares; Sara Solt; Alvin Dorman; Anthony Wamwea; Allison Yager; Daniel A. Laheru; Christopher L. Wolfgang; Jiang Wang; Ralph H. Hruban; Robert A. Anders; Elizabeth M. Jaffee; Lei Zheng

doi:10.1158/2326-6066.cir-14-0027

Immunotherapy Converts Nonimmunogenic Pancreatic Tumors into Immunogenic Foci of Immune Regulation

Eric R. Lutz(Johns Hopkins University), Annie A. Wu(Sidney Kimmel Cancer Center), Elaine Bigelow(Sidney Kimmel Cancer Center), Rajni Sharma, Guanglan Mo(Sidney Kimmel Cancer Center), Kevin C. Soares(Johns Hopkins University), Sara Solt(Sidney Kimmel Cancer Center), Alvin Dorman(Sidney Kimmel Cancer Center), Anthony Wamwea(Sidney Kimmel Cancer Center), Allison Yager(Sidney Kimmel Cancer Center), Daniel A. Laheru(Sidney Kimmel Cancer Center), Christopher L. Wolfgang(Johns Hopkins University), Jiang Wang(University of Cincinnati Medical Center), Ralph H. Hruban(Johns Hopkins University), Robert A. Anders(Johns Hopkins University), Elizabeth M. Jaffee(Johns Hopkins University), Lei Zheng(Johns Hopkins University)

Cancer Immunology Research

June 18, 2014

10.1158/2326-6066.cir-14-0027

Cited by 541Open Access

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Abstract

Pancreatic ductal adenocarcinoma (PDAC) is considered a "nonimmunogenic" neoplasm. Single-agent immunotherapies have failed to demonstrate significant clinical activity in PDAC and other "nonimmunogenic" tumors, in part due to a complex tumor microenvironment (TME) that provides a formidable barrier to immune infiltration and function. We designed a neoadjuvant and adjuvant clinical trial comparing an irradiated, granulocyte-macrophage colony-stimulating factor (GM-CSF)-secreting, allogeneic PDAC vaccine (GVAX) given as a single agent or in combination with low-dose cyclophosphamide to deplete regulatory T cells (Treg) as a means to study how the TME is altered by immunotherapy. Examination of resected PDACs revealed the formation of vaccine-induced intratumoral tertiary lymphoid aggregates in 33 of 39 patients 2 weeks after vaccine treatment. Immunohistochemical analysis showed these aggregates to be regulatory structures of adaptive immunity. Microarray analysis of microdissected aggregates identified gene-expression signatures in five signaling pathways involved in regulating immune-cell activation and trafficking that were associated with improved postvaccination responses. A suppressed Treg pathway and an enhanced Th17 pathway within these aggregates were associated with improved survival, enhanced postvaccination mesothelin-specific T-cell responses, and increased intratumoral Teff:Treg ratios. This study provides the first example of immune-based therapy converting a "nonimmunogenic" neoplasm into an "immunogenic" neoplasm by inducing infiltration of T cells and development of tertiary lymphoid structures in the TME. Post-GVAX T-cell infiltration and aggregate formation resulted in the upregulation of immunosuppressive regulatory mechanisms, including the PD-1-PD-L1 pathway, suggesting that patients with vaccine-primed PDAC may be better candidates than vaccine-naïve patients for immune checkpoint and other immunomodulatory therapies.

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