Therapeutic inhibition of the SRC-kinase HCK facilitates T cell tumor infiltration and improves response to immunotherapy.

Poh, Ashleigh R; Love, Christopher G; Chisanga, David; Steer, James H; Baloyan, David; Chopin, Michaël; Nutt, Stephen; Rautela, Jai; Huntington, Nicholas D; Etemadi, Nima; O'Brien, Megan; O'Keefe, Ryan; Ellies, Lesley G; Macri, Christophe; Mintern, Justine D; Whitehead, Lachlan; Gangadhara, Gangadhara; Boon, Louis; Chand, Ashwini L; Lowell, Clifford A; Shi, Wei; Pixley, Fiona J; Ernst, Matthias

doi:10.1126/sciadv.abl7882

Title

Therapeutic inhibition of the SRC-kinase HCK facilitates T cell tumor infiltration and improves response to immunotherapy.

Publication Date

2022-06-24

Author(s)

Poh, Ashleigh R

Love, Christopher G

Chisanga, David

Steer, James H

Baloyan, David

Chopin, Michaël

Nutt, Stephen

Rautela, Jai

Huntington, Nicholas D

Etemadi, Nima

O'Brien, Megan

O'Keefe, Ryan

Ellies, Lesley G

Macri, Christophe

Mintern, Justine D

Whitehead, Lachlan

Gangadhara, Gangadhara

Boon, Louis

Chand, Ashwini L

Lowell, Clifford A

Shi, Wei

Pixley, Fiona J

Ernst, Matthias

Type of document

Journal Article

OrcId

0000-0001-8375-4753

0000-0002-0421-3957

0000-0003-0630-5027

0000-0002-9153-263X

0000-0001-8812-2763

0000-0002-0020-6637

0000-0002-4253-9966

0000-0002-5267-7211

0000-0002-7137-1373

0000-0002-9687-919X

0000-0002-8527-2165

0000-0002-3797-8577

0000-0002-4388-9642

0000-0002-0937-9171

0000-0002-1245-729X

0000-0002-0467-7073

0000-0003-1182-7735

0000-0002-1571-2532

0000-0002-6399-1177

0000-0001-7297-4128

DOI

10.1126/sciadv.abl7882

Abstract

Although immunotherapy has revolutionized cancer treatment, many immunogenic tumors remain refractory to treatment. This can be largely attributed to an immunologically "cold" tumor microenvironment characterized by an accumulation of immunosuppressive myeloid cells and exclusion of activated T cells. Here, we demonstrate that genetic ablation or therapeutic inhibition of the myeloid-specific hematopoietic cell kinase (HCK) enables activity of antagonistic anti-programmed cell death protein 1 (anti-PD1), anti-CTLA4, or agonistic anti-CD40 immunotherapies in otherwise refractory tumors and augments response in treatment-susceptible tumors. Mechanistically, HCK ablation reprograms tumor-associated macrophages and dendritic cells toward an inflammatory endotype and enhances CD8+ T cell recruitment and activation when combined with immunotherapy in mice. Meanwhile, therapeutic inhibition of HCK in humanized mice engrafted with patient-derived xenografts counteracts tumor immunosuppression, improves T cell recruitment, and impairs tumor growth. Collectively, our results suggest that therapeutic targeting of HCK activity enhances response to immunotherapy by simultaneously stimulating immune cell activation and inhibiting the immunosuppressive tumor microenvironment.

Link

link

Citation

Science advances 2022; 8(25): eabl7882

Jornal Title

Science advances

Austin Health

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