Oncolytic Adenovirus ORCA-010 Activates Proinflammatory Myeloid Cells and Facilitates T Cell Recruitment and Activation by PD-1 Blockade in Melanoma | Zendy

Ioanna Milenova | Zendy; Marta López González | Zendy; Dafne C.A. Quixabeira | Zendy; João M. Santos | Zendy; Víctor Cervera-Carrascón | Zendy; WenLiang Dong | Zendy; Akseli Hemminki | Zendy; Victor W. van Beusechem | Zendy; Rieneke van de Ven | Zendy; Tanja D. de Gruijl | Zendy

Open Access

Oncolytic Adenovirus ORCA-010 Activates Proinflammatory Myeloid Cells and Facilitates T Cell Recruitment and Activation by PD-1 Blockade in Melanoma

Author(s) -

Ioanna Milenova,

Marta López González,

Dafne C.A. Quixabeira,

João M. Santos,

Víctor Cervera-Carrascón,

WenLiang Dong,

Akseli Hemminki,

Victor W. van Beusechem,

Rieneke van de Ven,

Tanja D. de Gruijl

Publication year - 2021

Publication title -

human gene therapy

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.633

H-Index - 149

eISSN - 1557-7422

pISSN - 1043-0342

DOI - 10.1089/hum.2020.277

Subject(s) - cd80 , cd86 , oncolytic virus , cancer research , melanoma , immune checkpoint , t cell , tumor microenvironment , biology , myeloid , proinflammatory cytokine , immune system , cytotoxic t cell , immunology , immunotherapy , cd40 , in vitro , inflammation , biochemistry

Immune checkpoint inhibitors have advanced the treatment of melanoma. Nevertheless, a majority of patients are resistant, or develop resistance, to immune checkpoint blockade, which may be related to prevailing immune suppression by myeloid regulatory cells in the tumor microenvironment (TME). ORCA-010 is a novel oncolytic adenovirus that selectively replicates in, and lyses, cancer cells. We previously showed that ORCA-010 can activate melanoma-exposed conventional dendritic cells (cDCs). To study the effect of ORCA-010 on melanoma-conditioned macrophage development, we used an in vitro co-culture model of human monocytes with melanoma cell lines. We observed a selective survival and polarization of monocytes into M2-like macrophages (CD14 + CD80 - CD163 + ) in co-cultures with cell lines that expressed macrophage colony-stimulating factor. Oncolysis of these melanoma cell lines, effected by ORCA-010, activated the resulting macrophages and converted them to a more proinflammatory state, evidenced by higher levels of PD-L1, CD80, and CD86 and an enhanced capacity to prime allogenic T cells and induce a type-1 T cell response. To assess the effect of ORCA-010 on myeloid subset distribution and activation in vivo , ORCA-010 was intratumorally injected and tested for T cell activation and recruitment in the human adenovirus nonpermissive B16-OVA mouse melanoma model. While systemic PD-1 blockade in this model in itself did not modulate myeloid or T cell subset distribution and activation, when it was preceded by i.t. injection of ORCA-010, this induced an increased rate and activation state of CD8α + cDC1, both in the TME and in the spleen. Observed increased rates of activated CD8 + T cells, expressing CD69 and PD-1, were related to both increased CD8α + cDC1 rates and M1/M2 shifts in tumor and spleen. In conclusion, the myeloid modulatory properties of ORCA-010 in melanoma, resulting in recruitment and activation of T cells, could enhance the antitumor efficacy of PD-1 blockade.

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