Shining a LIGHT on myeloid cell targeted immunotherapy

Casey W Shuptrine; Vincent M Perez; Sara R Selitsky; Taylor H Schreiber; George Fromm

doi:10.1016/j.ejca.2023.03.040

Shining a LIGHT on myeloid cell targeted immunotherapy

Eur J Cancer. 2023 Jul:187:147-160. doi: 10.1016/j.ejca.2023.03.040. Epub 2023 Apr 5.

Authors

Casey W Shuptrine¹, Vincent M Perez², Sara R Selitsky², Taylor H Schreiber¹, George Fromm³

Affiliations

¹ Shattuck Labs Inc., Austin, TX, USA; Shattuck Labs Inc., Durham, NC, USA.
² QuantBio, Part of Tempus Labs, Durham NC, USA.
³ Shattuck Labs Inc., Austin, TX, USA; Shattuck Labs Inc., Durham, NC, USA. Electronic address: gfromm@shattucklabs.com.

PMID: 37167762
DOI: 10.1016/j.ejca.2023.03.040

Abstract

Despite over a decade of clinical trials combining inhibition of emerging checkpoints with a PD-1/L1 inhibitor backbone, meaningful survival benefits have not been shown in PD-1/L1 inhibitor resistant or refractory solid tumours, particularly tumours dominated by a myelosuppressive microenvironment. Achieving durable anti-tumour immunity will therefore likely require combination of adaptive and innate immune stimulation, myeloid repolarisation, enhanced APC activation and antigen processing/presentation, lifting of the CD47/SIRPα (Cluster of Differentiation 47/signal regulatory protein alpha) 'do not eat me' signal, provision of an apoptotic 'pro-eat me' or 'find me' signal, and blockade of immune checkpoints. The importance of effectively targeting mLILRB2 and SIRPAyeloid cells to achieve improved response rates has recently been emphasised, given myeloid cells are abundant in the tumour microenvironment of most solid tumours. TNFSF14, or LIGHT, is a tumour necrosis superfamily ligand with a broad range of adaptive and innate immune activities, including (1) myeloid cell activation through Lymphotoxin Beta Receptor (LTβR), (2) T/NK (T cell and natural killer cell) induced anti-tumour immune activity through Herpes virus entry mediator (HVEM), (3) potentiation of proinflammatory cytokine/chemokine secretion through LTβR on tumour stromal cells, (4) direct induction of tumour cell apoptosis in vitro, and (5) the reorganisation of lymphatic tissue architecture, including within the tumour microenvironment (TME), by promoting high endothelial venule (HEV) formation and induction of tertiary lymphoid structures. LTBR (Lymphotoxin beta receptor) and HVEM rank highly amongst a range of costimulatory receptors in solid tumours, which raises interest in considering how LIGHT-mediated costimulation may be distinct from a growing list of immunotherapy targets which have failed to provide survival benefit as monotherapy or in combination with PD-1 inhibitors, particularly in the checkpoint acquired resistant setting.

Keywords: Acquired resistance; Checkpoint inhibition; Co-stimulation; HVEM; LIGHT; LTβR; Myeloid therapy.

Publication types

Review
Research Support, Non-U.S. Gov't

MeSH terms

Cytokines
Humans
Immunotherapy
Lymphotoxin beta Receptor*
Myeloid Cells
Neoplasms* / drug therapy
Programmed Cell Death 1 Receptor
Tumor Microenvironment

Substances

Lymphotoxin beta Receptor
Programmed Cell Death 1 Receptor
Cytokines