TY - JOUR
T1 - Elucidating cellular response to treatment with viral immunotherapies in pediatric high-grade glioma and medulloblastoma
T2 - Brain tumor cellular response to viral immunotherapy
AU - Thompson, Eric M.
AU - Kang, Kyung Don
AU - Stevenson, Kevin
AU - Zhang, Hengshan
AU - Gromeier, Matthias
AU - Ashley, David
AU - Brown, Michael
AU - Friedman, Gregory K.
N1 - Publisher Copyright:
© 2024
PY - 2024/2
Y1 - 2024/2
N2 - HSV G207, a double-stranded, DNA virus, and the polio:rhinovirus chimera, PVSRIPO, a single positive-strand RNA virus, are viral immunotherapies being used to treat pediatric malignant brain tumors in clinical trials. The purpose of this work is to elucidate general response patterns and putative biomarkers of response. Multiple pediatric high-grade glioma and medulloblastoma cell lines were treated with various multiplicities of infection of G207 or PVSRIPO. There was a significant inverse correlation between expression of one HSV cellular receptor, CD111, and the lethal dose of 50% of cells (LD50) of cells treated with G207 (r = -0.985, P<0.001) but no correlation between PVSRIPO cellular receptor expression (CD155) and LD50. RNA sequencing of control cells and cells treated for 8 and 24 h revealed that there were few shared differentially expressed (DE) genes between cells treated with PVSRIPO and G207: GCLM, LANCL2, and RBM3 were enriched whilst ADAMTS1 and VEGFA were depleted. Likewise, there were few shared DE genes enriched between medulloblastoma and high-grade glioma cell lines treated with G207: GPSM2, CHECK2, SEPTIN2, EIF4G2, GCLM, GDAP1, LANCL2, and PWP1. Treatment with G207 and PVSRIPO appear to cause disparate gene enrichment and depletion suggesting disparate molecular mechanisms in malignant pediatric brain tumors.
AB - HSV G207, a double-stranded, DNA virus, and the polio:rhinovirus chimera, PVSRIPO, a single positive-strand RNA virus, are viral immunotherapies being used to treat pediatric malignant brain tumors in clinical trials. The purpose of this work is to elucidate general response patterns and putative biomarkers of response. Multiple pediatric high-grade glioma and medulloblastoma cell lines were treated with various multiplicities of infection of G207 or PVSRIPO. There was a significant inverse correlation between expression of one HSV cellular receptor, CD111, and the lethal dose of 50% of cells (LD50) of cells treated with G207 (r = -0.985, P<0.001) but no correlation between PVSRIPO cellular receptor expression (CD155) and LD50. RNA sequencing of control cells and cells treated for 8 and 24 h revealed that there were few shared differentially expressed (DE) genes between cells treated with PVSRIPO and G207: GCLM, LANCL2, and RBM3 were enriched whilst ADAMTS1 and VEGFA were depleted. Likewise, there were few shared DE genes enriched between medulloblastoma and high-grade glioma cell lines treated with G207: GPSM2, CHECK2, SEPTIN2, EIF4G2, GCLM, GDAP1, LANCL2, and PWP1. Treatment with G207 and PVSRIPO appear to cause disparate gene enrichment and depletion suggesting disparate molecular mechanisms in malignant pediatric brain tumors.
KW - Cell response
KW - G207
KW - Medulloblastoma
KW - Oncolytic virus
KW - Pediatric high-grade glioma
KW - PVSRIPO
KW - RNA sequencing
KW - Viral immunotherapy
UR - http://www.scopus.com/inward/record.url?scp=85181928695&partnerID=8YFLogxK
U2 - 10.1016/j.tranon.2024.101875
DO - 10.1016/j.tranon.2024.101875
M3 - Article
C2 - 38183802
AN - SCOPUS:85181928695
SN - 1936-5233
VL - 40
JO - Translational Oncology
JF - Translational Oncology
M1 - 101875
ER -