Abstract 3792: Intratumoral CD56bright natural killer cells are associated with improved survival in bladder cancer

Mukherjee, Neelam; Ji, Niannian; Tomasini, Maggie E.; Hurez, Vincent; Curiel, Tyler J.; Montgomery, Maureen; Braun, Andrew J.; Nicolas, Marlo; Flores, Marcela A.; Liu, Qianqian; Ruan, Jianhua; Svatek, Robert S.

doi:10.1158/1538-7445.am2018-3792

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“…Surprisingly, a more recent flow cytometric analysis of fresh tissue from patients with both NMIBC and muscle invasive bladder cancer (MIBC) has suggested that improved survival may be linked to the presence of CD56 bright NK cells within the tumor which are found in much smaller numbers than their CD56 dim counterparts. These cells are functionally active compared to the reduced cytokine secreting capacities of the CD56 dim subset (64). This might explain the findings of the previous study which did not distinguish between the subsets in their analysis.…”

Section: Natural Killer Cell Subsets and γδ T Cellsmentioning

confidence: 99%

Immune Responses in Bladder Cancer-Role of Immune Cell Populations, Prognostic Factors and Therapeutic Implications

Joseph

Enting

2019

Front. Oncol.

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Immunosurveillance, which describes the immunologically mediated elimination of transformed cells, has been widely accepted in the context of bladder cancer for many decades with the successful use of Bacillus-Calmette Guerin for superficial bladder cancer since the 1970s. With the emergence of checkpoint inhibitor blockade in the treatment of urothelial cancers, there has been a resurgent interest in the immunology of bladder cancer. The theory of cancer immunoediting proposes that the immune system has both pro-tumorigenic and anti-tumor effects, the balance between the two determining the progression of an individual tumor. However, whilst there is evidence for the action of various immune cell populations in bladder cancer, a cohesive picture of the immune response to bladder cancer and its driving forces are still lacking. Additionally, little is still known about the normal immune landscape of the bladder. Future progress in bladder cancer therapeutic approaches will require a strong foundation in understanding the immunology of this disease. This review considers the evidence for the role of the main immune cell populations, both innate and adaptive, in the immune response to bladder cancer. Recent research and overarching themes in the immune response to bladder cancer are explored. The minimal evidence regarding the normal immune landscape of the human bladder is also summarized to contextualize downstream immune responses. Of specific interest are the innate and myeloid populations, some of which are resident in the human bladder and which have significant effects on downstream adaptive tumor immunity. We discuss factors which restrain the efficacy of populations known to have anti-tumor activity such as cytotoxic T cells, including the constraints on checkpoint blockade. Additionally, the effects on the immune response of tumor intrinsic factors such as the genomic subtype of bladder cancer and the effect of common therapies such as chemotherapy and intravesical Bacillus Calmette-Guerin are considered. A significant theme is the polarization of immune responses within the tumor by a heavily immunosuppressive tumor microenvironment which affects the phenotype of multiple innate and adaptive populations. Throughout, clinical implications are discussed with suggestions for future research directions and therapeutic targeting.

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Section: Natural Killer Cell Subsets and γδ T Cellsmentioning

confidence: 99%