Alternative splicing of the inhibitory immune checkpoint receptor SLAMF6 generates a dominant positive form, boosting T-cell effector functions

Emma Hajaj; Elad Zisman; Shay Tzaban; Sharon Merims; Cohen Jonathan; Shiri Klein; Shoshana Frankenburg; Moshe Sade-Feldman; Yuval Tabach; Keren Yizhak; Ami Navon; Polina Stepensky; Nir Hacohen; Tamar Peretz; Andre Veillette; Rotem Karni; Galit Eisenberg; Michal Lotem

doi:10.1158/2326-6066.CIR-20-0800

Alternative splicing of the inhibitory immune checkpoint receptor SLAMF6 generates a dominant positive form, boosting T-cell effector functions

Emma Hajaj, Elad Zisman, Shay Tzaban, Sharon Merims, Cohen Jonathan, Shiri Klein, Shoshana Frankenburg, Moshe Sade-Feldman, Yuval Tabach, Keren Yizhak, Ami Navon, Polina Stepensky, Nir Hacohen, Tamar Peretz, Andre Veillette, Rotem Karni, Galit Eisenberg, Michal Lotem

Technion - Israel Institute of Technology, The Hebrew University of Jerusalem, Weizmann Institute of Science

Research output: Contribution to journal › Article › peer-review

Abstract

SLAMF6 is a homotypic receptor of the Ig-superfamily associated with progenitor-exhausted T cells. Here we show that in humans, SLAMF6 has three splice isoforms involving its V-domain. Although the canonical receptor inhibited T-cell activation through SAP recruitment, the short isoform SLAMF6^D17–⁶⁵ had a strong agonistic effect. The costimulatory action depended on protein phosphatase SHP1 and led to a cytotoxic molecular profile mediated by the expression of TBX21 and RUNX3. Patients treated with immune checkpoint blockade showed a shift toward SLAMF6^D17–65 in peripheral blood T cells. We developed splice-switching antisense oligonucleotides (ASO) designed to target the relevant SLAMF6 splice junction. Our ASOs enhanced SLAMF6^D17–⁶⁵ expression in human tumor-infiltrating lymphocytes and improved their capacity to inhibit human melanoma in mice. The yin-yang relationship of SLAMF6 splice isoforms may represent a balancing mechanism that could be exploited to improve cancer immunotherapy.

Original language	English
Pages (from-to)	637-650
Number of pages	14
Journal	Cancer Immunology Research
Volume	9
Issue number	6
DOIs	https://doi.org/10.1158/2326-6066.CIR-20-0800
State	Published - Jun 2021

All Science Journal Classification (ASJC) codes

General Medicine
Immunology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1158/2326-6066.CIR-20-0800

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Hajaj, E., Zisman, E., Tzaban, S., Merims, S., Jonathan, C., Klein, S., Frankenburg, S., Sade-Feldman, M., Tabach, Y., Yizhak, K., Navon, A., Stepensky, P., Hacohen, N., Peretz, T., Veillette, A., Karni, R., Eisenberg, G., & Lotem, M. (2021). Alternative splicing of the inhibitory immune checkpoint receptor SLAMF6 generates a dominant positive form, boosting T-cell effector functions. Cancer Immunology Research, 9(6), 637-650. https://doi.org/10.1158/2326-6066.CIR-20-0800

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title = "Alternative splicing of the inhibitory immune checkpoint receptor SLAMF6 generates a dominant positive form, boosting T-cell effector functions",

abstract = "SLAMF6 is a homotypic receptor of the Ig-superfamily associated with progenitor-exhausted T cells. Here we show that in humans, SLAMF6 has three splice isoforms involving its V-domain. Although the canonical receptor inhibited T-cell activation through SAP recruitment, the short isoform SLAMF6D17–65 had a strong agonistic effect. The costimulatory action depended on protein phosphatase SHP1 and led to a cytotoxic molecular profile mediated by the expression of TBX21 and RUNX3. Patients treated with immune checkpoint blockade showed a shift toward SLAMF6D17–65 in peripheral blood T cells. We developed splice-switching antisense oligonucleotides (ASO) designed to target the relevant SLAMF6 splice junction. Our ASOs enhanced SLAMF6D17–65 expression in human tumor-infiltrating lymphocytes and improved their capacity to inhibit human melanoma in mice. The yin-yang relationship of SLAMF6 splice isoforms may represent a balancing mechanism that could be exploited to improve cancer immunotherapy.",

author = "Emma Hajaj and Elad Zisman and Shay Tzaban and Sharon Merims and Cohen Jonathan and Shiri Klein and Shoshana Frankenburg and Moshe Sade-Feldman and Yuval Tabach and Keren Yizhak and Ami Navon and Polina Stepensky and Nir Hacohen and Tamar Peretz and Andre Veillette and Rotem Karni and Galit Eisenberg and Michal Lotem",

note = "Publisher Copyright: {\textcopyright}2021 American Association for Cancer Research.",

year = "2021",

month = jun,

doi = "10.1158/2326-6066.CIR-20-0800",

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Hajaj, E, Zisman, E, Tzaban, S, Merims, S, Jonathan, C, Klein, S, Frankenburg, S, Sade-Feldman, M, Tabach, Y , Yizhak, K , Navon, A, Stepensky, P, Hacohen, N, Peretz, T, Veillette, A, Karni, R, Eisenberg, G & Lotem, M 2021, 'Alternative splicing of the inhibitory immune checkpoint receptor SLAMF6 generates a dominant positive form, boosting T-cell effector functions', Cancer Immunology Research, vol. 9, no. 6, pp. 637-650. https://doi.org/10.1158/2326-6066.CIR-20-0800

TY - JOUR

T1 - Alternative splicing of the inhibitory immune checkpoint receptor SLAMF6 generates a dominant positive form, boosting T-cell effector functions

AU - Hajaj, Emma

AU - Zisman, Elad

AU - Tzaban, Shay

AU - Merims, Sharon

AU - Jonathan, Cohen

AU - Klein, Shiri

AU - Frankenburg, Shoshana

AU - Sade-Feldman, Moshe

AU - Tabach, Yuval

AU - Yizhak, Keren

AU - Navon, Ami

AU - Stepensky, Polina

AU - Hacohen, Nir

AU - Peretz, Tamar

AU - Veillette, Andre

AU - Karni, Rotem

AU - Eisenberg, Galit

AU - Lotem, Michal

PY - 2021/6

Y1 - 2021/6

N2 - SLAMF6 is a homotypic receptor of the Ig-superfamily associated with progenitor-exhausted T cells. Here we show that in humans, SLAMF6 has three splice isoforms involving its V-domain. Although the canonical receptor inhibited T-cell activation through SAP recruitment, the short isoform SLAMF6D17–65 had a strong agonistic effect. The costimulatory action depended on protein phosphatase SHP1 and led to a cytotoxic molecular profile mediated by the expression of TBX21 and RUNX3. Patients treated with immune checkpoint blockade showed a shift toward SLAMF6D17–65 in peripheral blood T cells. We developed splice-switching antisense oligonucleotides (ASO) designed to target the relevant SLAMF6 splice junction. Our ASOs enhanced SLAMF6D17–65 expression in human tumor-infiltrating lymphocytes and improved their capacity to inhibit human melanoma in mice. The yin-yang relationship of SLAMF6 splice isoforms may represent a balancing mechanism that could be exploited to improve cancer immunotherapy.

AB - SLAMF6 is a homotypic receptor of the Ig-superfamily associated with progenitor-exhausted T cells. Here we show that in humans, SLAMF6 has three splice isoforms involving its V-domain. Although the canonical receptor inhibited T-cell activation through SAP recruitment, the short isoform SLAMF6D17–65 had a strong agonistic effect. The costimulatory action depended on protein phosphatase SHP1 and led to a cytotoxic molecular profile mediated by the expression of TBX21 and RUNX3. Patients treated with immune checkpoint blockade showed a shift toward SLAMF6D17–65 in peripheral blood T cells. We developed splice-switching antisense oligonucleotides (ASO) designed to target the relevant SLAMF6 splice junction. Our ASOs enhanced SLAMF6D17–65 expression in human tumor-infiltrating lymphocytes and improved their capacity to inhibit human melanoma in mice. The yin-yang relationship of SLAMF6 splice isoforms may represent a balancing mechanism that could be exploited to improve cancer immunotherapy.

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U2 - 10.1158/2326-6066.CIR-20-0800

DO - 10.1158/2326-6066.CIR-20-0800

M3 - مقالة

C2 - 33762352

SN - 2326-6066

VL - 9

SP - 637

EP - 650

JO - Cancer Immunology Research

JF - Cancer Immunology Research

IS - 6

ER -

Alternative splicing of the inhibitory immune checkpoint receptor SLAMF6 generates a dominant positive form, boosting T-cell effector functions

Abstract

All Science Journal Classification (ASJC) codes

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