Sertraline/chloroquine combination therapy to target hypoxic and immunosuppressive serine/glycine synthesis-dependent glioblastomas

Anais Sanchez-Castillo; Kim G. Savelkouls; Alessandra Baldini; Judith Hounjet; Pierre Sonveaux; Paulien Verstraete; Kim De Keersmaecker; Barbara Dewaele; Benny Bjorkblom; Beatrice Melin; Wendy Y. Wu; Rickard L. Sjoberg; Kasper M. A. Rouschop; Martijn P. G. Broen; Marc Vooijs; Kim R. Kampen

doi:10.1038/s41389-024-00540-3

Sertraline/chloroquine combination therapy to target hypoxic and immunosuppressive serine/glycine synthesis-dependent glioblastomas

Anais Sanchez-Castillo, Kim G. Savelkouls, Alessandra Baldini, Judith Hounjet, Pierre Sonveaux, Paulien Verstraete, Kim De Keersmaecker, Barbara Dewaele, Benny Bjorkblom, Beatrice Melin, Wendy Y. Wu, Rickard L. Sjoberg, Kasper M. A. Rouschop, Martijn P. G. Broen, Marc Vooijs, Kim R. Kampen^*

^*Corresponding author for this work

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

Abstract

The serine/glycine (ser/gly) synthesis pathway branches from glycolysis and is hyperactivated in approximately 30% of cancers. In similar to 13% of glioblastoma cases, we observed frequent amplifications and rare mutations in the gene encoding the enzyme PSPH, which catalyzes the last step in the synthesis of serine. This urged us to unveil the relevance of PSPH genetic alterations and subsequent ser/gly metabolism deregulation in the pathogenesis of glioblastoma. Primary glioblastoma cells overexpressing PSPH and PSPHV116I showed an increased clonogenic capacity, cell proliferation, and migration, supported by elevated nucleotide synthesis and utilization of reductive NAD(P). We previously identified sertraline as an inhibitor of ser/gly synthesis and explored its efficacy at suboptimal dosages in combination with the clinically pretested chloroquine to target ser/gly(high) glioblastoma models. Interestingly, ser/gly(high) glioblastomas, including PSPHamp and PSPHV116I, displayed selective synergistic inhibition of proliferation in response to combination therapy. PSPH knockdown severely affected ser/gly(high) glioblastoma clonogenicity and proliferation, while simultaneously increasing its sensitivity to chloroquine treatment. Metabolite landscaping revealed that sertraline/chloroquine combination treatment blocks NADH and ATP generation and restricts nucleotide synthesis, thereby inhibiting glioblastoma proliferation. Our previous studies highlight ser/gly(high) cancer cell modulation of its microenvironment at the level of immune suppression. To this end, high PSPH expression predicts poor immune checkpoint therapy responses in glioblastoma patients. Interestingly, we show that PSPH amplifications in glioblastoma facilitate the expression of immune suppressor galectin-1, which can be inhibited by sertraline treatment. Collectively, we revealed that ser/gly(high) glioblastomas are characterized by enhanced clonogenicity, migration, and suppression of the immune system, which could be tackled using combined sertraline/chloroquine treatment, revealing novel therapeutic opportunities for this subgroup of GBM patients.

Original language	English
Article number	39
Number of pages	18
Journal	Oncogenesis
Volume	13
Issue number	1
DOIs	https://doi.org/10.1038/s41389-024-00540-3
Publication status	Published - 13 Nov 2024

Keywords

ELECTRON-TRANSPORT CHAIN
GLIOMA STEM-CELLS
SERINE SYNTHESIS
ROS GENERATION
CULTURE-SYSTEM
BRAIN
GALECTIN-1
HETEROGENEITY
RESPIRATION
METABOLISM

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Sanchez-Castillo, A., Savelkouls, K. G., Baldini, A., Hounjet, J., Sonveaux, P., Verstraete, P., De Keersmaecker, K., Dewaele, B., Bjorkblom, B., Melin, B., Wu, W. Y., Sjoberg, R. L., Rouschop, K. M. A., Broen, M. P. G., Vooijs, M., & Kampen, K. R. (2024). Sertraline/chloroquine combination therapy to target hypoxic and immunosuppressive serine/glycine synthesis-dependent glioblastomas. Oncogenesis, 13(1), Article 39. https://doi.org/10.1038/s41389-024-00540-3

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title = "Sertraline/chloroquine combination therapy to target hypoxic and immunosuppressive serine/glycine synthesis-dependent glioblastomas",

abstract = "The serine/glycine (ser/gly) synthesis pathway branches from glycolysis and is hyperactivated in approximately 30% of cancers. In similar to 13% of glioblastoma cases, we observed frequent amplifications and rare mutations in the gene encoding the enzyme PSPH, which catalyzes the last step in the synthesis of serine. This urged us to unveil the relevance of PSPH genetic alterations and subsequent ser/gly metabolism deregulation in the pathogenesis of glioblastoma. Primary glioblastoma cells overexpressing PSPH and PSPHV116I showed an increased clonogenic capacity, cell proliferation, and migration, supported by elevated nucleotide synthesis and utilization of reductive NAD(P). We previously identified sertraline as an inhibitor of ser/gly synthesis and explored its efficacy at suboptimal dosages in combination with the clinically pretested chloroquine to target ser/gly(high) glioblastoma models. Interestingly, ser/gly(high) glioblastomas, including PSPHamp and PSPHV116I, displayed selective synergistic inhibition of proliferation in response to combination therapy. PSPH knockdown severely affected ser/gly(high) glioblastoma clonogenicity and proliferation, while simultaneously increasing its sensitivity to chloroquine treatment. Metabolite landscaping revealed that sertraline/chloroquine combination treatment blocks NADH and ATP generation and restricts nucleotide synthesis, thereby inhibiting glioblastoma proliferation. Our previous studies highlight ser/gly(high) cancer cell modulation of its microenvironment at the level of immune suppression. To this end, high PSPH expression predicts poor immune checkpoint therapy responses in glioblastoma patients. Interestingly, we show that PSPH amplifications in glioblastoma facilitate the expression of immune suppressor galectin-1, which can be inhibited by sertraline treatment. Collectively, we revealed that ser/gly(high) glioblastomas are characterized by enhanced clonogenicity, migration, and suppression of the immune system, which could be tackled using combined sertraline/chloroquine treatment, revealing novel therapeutic opportunities for this subgroup of GBM patients.",

keywords = "ELECTRON-TRANSPORT CHAIN, GLIOMA STEM-CELLS, SERINE SYNTHESIS, ROS GENERATION, CULTURE-SYSTEM, BRAIN, GALECTIN-1, HETEROGENEITY, RESPIRATION, METABOLISM",

author = "Anais Sanchez-Castillo and Savelkouls, {Kim G.} and Alessandra Baldini and Judith Hounjet and Pierre Sonveaux and Paulien Verstraete and {De Keersmaecker}, Kim and Barbara Dewaele and Benny Bjorkblom and Beatrice Melin and Wu, {Wendy Y.} and Sjoberg, {Rickard L.} and Rouschop, {Kasper M. A.} and Broen, {Martijn P. G.} and Marc Vooijs and Kampen, {Kim R.}",

year = "2024",

month = nov,

day = "13",

doi = "10.1038/s41389-024-00540-3",

language = "English",

volume = "13",

journal = "Oncogenesis",

issn = "2157-9024",

publisher = "Nature Publishing Group",

number = "1",

}

Sanchez-Castillo, A, Savelkouls, KG, Baldini, A, Hounjet, J, Sonveaux, P, Verstraete, P, De Keersmaecker, K, Dewaele, B, Bjorkblom, B, Melin, B, Wu, WY, Sjoberg, RL, Rouschop, KMA , Broen, MPG , Vooijs, M & Kampen, KR 2024, 'Sertraline/chloroquine combination therapy to target hypoxic and immunosuppressive serine/glycine synthesis-dependent glioblastomas', Oncogenesis, vol. 13, no. 1, 39. https://doi.org/10.1038/s41389-024-00540-3

TY - JOUR

T1 - Sertraline/chloroquine combination therapy to target hypoxic and immunosuppressive serine/glycine synthesis-dependent glioblastomas

AU - Sanchez-Castillo, Anais

AU - Savelkouls, Kim G.

AU - Baldini, Alessandra

AU - Hounjet, Judith

AU - Sonveaux, Pierre

AU - Verstraete, Paulien

AU - De Keersmaecker, Kim

AU - Dewaele, Barbara

AU - Bjorkblom, Benny

AU - Melin, Beatrice

AU - Wu, Wendy Y.

AU - Sjoberg, Rickard L.

AU - Rouschop, Kasper M. A.

AU - Broen, Martijn P. G.

AU - Vooijs, Marc

AU - Kampen, Kim R.

PY - 2024/11/13

Y1 - 2024/11/13

N2 - The serine/glycine (ser/gly) synthesis pathway branches from glycolysis and is hyperactivated in approximately 30% of cancers. In similar to 13% of glioblastoma cases, we observed frequent amplifications and rare mutations in the gene encoding the enzyme PSPH, which catalyzes the last step in the synthesis of serine. This urged us to unveil the relevance of PSPH genetic alterations and subsequent ser/gly metabolism deregulation in the pathogenesis of glioblastoma. Primary glioblastoma cells overexpressing PSPH and PSPHV116I showed an increased clonogenic capacity, cell proliferation, and migration, supported by elevated nucleotide synthesis and utilization of reductive NAD(P). We previously identified sertraline as an inhibitor of ser/gly synthesis and explored its efficacy at suboptimal dosages in combination with the clinically pretested chloroquine to target ser/gly(high) glioblastoma models. Interestingly, ser/gly(high) glioblastomas, including PSPHamp and PSPHV116I, displayed selective synergistic inhibition of proliferation in response to combination therapy. PSPH knockdown severely affected ser/gly(high) glioblastoma clonogenicity and proliferation, while simultaneously increasing its sensitivity to chloroquine treatment. Metabolite landscaping revealed that sertraline/chloroquine combination treatment blocks NADH and ATP generation and restricts nucleotide synthesis, thereby inhibiting glioblastoma proliferation. Our previous studies highlight ser/gly(high) cancer cell modulation of its microenvironment at the level of immune suppression. To this end, high PSPH expression predicts poor immune checkpoint therapy responses in glioblastoma patients. Interestingly, we show that PSPH amplifications in glioblastoma facilitate the expression of immune suppressor galectin-1, which can be inhibited by sertraline treatment. Collectively, we revealed that ser/gly(high) glioblastomas are characterized by enhanced clonogenicity, migration, and suppression of the immune system, which could be tackled using combined sertraline/chloroquine treatment, revealing novel therapeutic opportunities for this subgroup of GBM patients.

AB - The serine/glycine (ser/gly) synthesis pathway branches from glycolysis and is hyperactivated in approximately 30% of cancers. In similar to 13% of glioblastoma cases, we observed frequent amplifications and rare mutations in the gene encoding the enzyme PSPH, which catalyzes the last step in the synthesis of serine. This urged us to unveil the relevance of PSPH genetic alterations and subsequent ser/gly metabolism deregulation in the pathogenesis of glioblastoma. Primary glioblastoma cells overexpressing PSPH and PSPHV116I showed an increased clonogenic capacity, cell proliferation, and migration, supported by elevated nucleotide synthesis and utilization of reductive NAD(P). We previously identified sertraline as an inhibitor of ser/gly synthesis and explored its efficacy at suboptimal dosages in combination with the clinically pretested chloroquine to target ser/gly(high) glioblastoma models. Interestingly, ser/gly(high) glioblastomas, including PSPHamp and PSPHV116I, displayed selective synergistic inhibition of proliferation in response to combination therapy. PSPH knockdown severely affected ser/gly(high) glioblastoma clonogenicity and proliferation, while simultaneously increasing its sensitivity to chloroquine treatment. Metabolite landscaping revealed that sertraline/chloroquine combination treatment blocks NADH and ATP generation and restricts nucleotide synthesis, thereby inhibiting glioblastoma proliferation. Our previous studies highlight ser/gly(high) cancer cell modulation of its microenvironment at the level of immune suppression. To this end, high PSPH expression predicts poor immune checkpoint therapy responses in glioblastoma patients. Interestingly, we show that PSPH amplifications in glioblastoma facilitate the expression of immune suppressor galectin-1, which can be inhibited by sertraline treatment. Collectively, we revealed that ser/gly(high) glioblastomas are characterized by enhanced clonogenicity, migration, and suppression of the immune system, which could be tackled using combined sertraline/chloroquine treatment, revealing novel therapeutic opportunities for this subgroup of GBM patients.

KW - ELECTRON-TRANSPORT CHAIN

KW - GLIOMA STEM-CELLS

KW - SERINE SYNTHESIS

KW - ROS GENERATION

KW - CULTURE-SYSTEM

KW - BRAIN

KW - GALECTIN-1

KW - HETEROGENEITY

KW - RESPIRATION

KW - METABOLISM

U2 - 10.1038/s41389-024-00540-3

DO - 10.1038/s41389-024-00540-3

M3 - Article

SN - 2157-9024

VL - 13

JO - Oncogenesis

JF - Oncogenesis

IS - 1

M1 - 39

ER -

Sertraline/chloroquine combination therapy to target hypoxic and immunosuppressive serine/glycine synthesis-dependent glioblastomas

Abstract

Keywords

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