Ismail M Meraz, Mourad Majidi, Renduo Song, Feng Meng, Lihui Gao, Qi Wang, Jing Wang, Elizabeth J Shpall, Jack A Roth
{"title":"NPRL2基因治疗在KRAS/STK11突变体抗pd1耐药转移性非小细胞肺癌(NSCLC)人源化小鼠模型中诱导有效的抗肿瘤免疫。","authors":"Ismail M Meraz, Mourad Majidi, Renduo Song, Feng Meng, Lihui Gao, Qi Wang, Jing Wang, Elizabeth J Shpall, Jack A Roth","doi":"10.7554/eLife.98258","DOIUrl":null,"url":null,"abstract":"<p><p>Expression of <i>NPRL2/TUSC4</i>, a tumor-suppressor gene, is reduced in many cancers including NSCLC. Restoration of <i>NPRL2</i> induces DNA damage, apoptosis, and cell-cycle arrest. We investigated <i>NPRL2</i> antitumor immune responses in aPD1<sup>R</sup>/<i>KRAS/STK11<sup>mt</sup></i> NSCLC in humanized-mice. Humanized-mice were generated by transplanting fresh human cord blood-derived CD34 stem cells into sub-lethally irradiated NSG mice. Lung-metastases were developed from <i>KRAS/STK11<sup>mt</sup></i>/aPD1<sup>R</sup> A549 cells and treated with <i>NPRL2</i> w/wo pembrolizumab. <i>NPRL2</i>-treatment reduced lung metastases significantly, whereas pembrolizumab was ineffective. Antitumor effect was greater in humanized than non-humanized-mice. <i>NPRL2</i> + pembrolizumab was not synergistic in <i>KRAS/STK11<sup>mt</sup></i>/aPD1<sup>R</sup> tumors but was synergistic in <i>KRAS<sup>wt</sup></i>/aPD1<sup>S</sup> H1299. <i>NPRL2</i> also showed a significant antitumor effect on <i>KRAS<sup>mt</sup></i>/aPD1<sup>R</sup> LLC2 syngeneic-tumors. The antitumor effect was correlated with increased infiltration of human cytotoxic-T, HLA-DR<sup>+</sup>DC, CD11c<sup>+</sup>DC, and downregulation of myeloid and regulatory-T cells in TME. Antitumor effect was abolished upon in-vivo depletion of CD8-T, macrophages, and CD4-T cells whereas remained unaffected upon NK-cell depletion. A distinctive protein-expression profile was found after <i>NPRL2</i> treatment. <i>IFNγ, CD8b</i>, and <i>TBX21</i> associated with T-cell functions were significantly increased, whereas <i>FOXP3, TGFB1/B2</i>, and <i>IL-10RA</i> were strongly inhibited by <i>NPRL2</i>. A list of T-cell co-inhibitory molecules was also downregulated. Restoration of <i>NPRL2</i> exhibited significantly slower tumor growth in humanized-mice, which was associated with increased presence of human cytotoxic-T, and DC and decreased percentage of Treg, MDSC, and TAM in TME. <i>NPRL2</i>-stable cells showed a substantial increase in colony-formation inhibition and heightened sensitivity to carboplatin. Stable-expression of <i>NPRL2</i> resulted in the downregulation of MAPK and AKT-mTOR signaling. Taken-together, <i>NPRL2</i> gene-therapy induces antitumor activity on <i>KRAS/STK11<sup>mt</sup></i>/aPD1<sup>R</sup> tumors through DC-mediated antigen-presentation and cytotoxic immune-cell activation.</p>","PeriodicalId":11640,"journal":{"name":"eLife","volume":"13 ","pages":""},"PeriodicalIF":6.4000,"publicationDate":"2025-02-11","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11813225/pdf/","citationCount":"0","resultStr":"{\"title\":\"<i>NPRL2</i> gene therapy induces effective antitumor immunity in <i>KRAS/STK11</i> mutant anti-PD1 resistant metastatic non-small cell lung cancer (NSCLC) in a humanized mouse model.\",\"authors\":\"Ismail M Meraz, Mourad Majidi, Renduo Song, Feng Meng, Lihui Gao, Qi Wang, Jing Wang, Elizabeth J Shpall, Jack A Roth\",\"doi\":\"10.7554/eLife.98258\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>Expression of <i>NPRL2/TUSC4</i>, a tumor-suppressor gene, is reduced in many cancers including NSCLC. Restoration of <i>NPRL2</i> induces DNA damage, apoptosis, and cell-cycle arrest. We investigated <i>NPRL2</i> antitumor immune responses in aPD1<sup>R</sup>/<i>KRAS/STK11<sup>mt</sup></i> NSCLC in humanized-mice. Humanized-mice were generated by transplanting fresh human cord blood-derived CD34 stem cells into sub-lethally irradiated NSG mice. Lung-metastases were developed from <i>KRAS/STK11<sup>mt</sup></i>/aPD1<sup>R</sup> A549 cells and treated with <i>NPRL2</i> w/wo pembrolizumab. <i>NPRL2</i>-treatment reduced lung metastases significantly, whereas pembrolizumab was ineffective. Antitumor effect was greater in humanized than non-humanized-mice. <i>NPRL2</i> + pembrolizumab was not synergistic in <i>KRAS/STK11<sup>mt</sup></i>/aPD1<sup>R</sup> tumors but was synergistic in <i>KRAS<sup>wt</sup></i>/aPD1<sup>S</sup> H1299. <i>NPRL2</i> also showed a significant antitumor effect on <i>KRAS<sup>mt</sup></i>/aPD1<sup>R</sup> LLC2 syngeneic-tumors. The antitumor effect was correlated with increased infiltration of human cytotoxic-T, HLA-DR<sup>+</sup>DC, CD11c<sup>+</sup>DC, and downregulation of myeloid and regulatory-T cells in TME. Antitumor effect was abolished upon in-vivo depletion of CD8-T, macrophages, and CD4-T cells whereas remained unaffected upon NK-cell depletion. A distinctive protein-expression profile was found after <i>NPRL2</i> treatment. <i>IFNγ, CD8b</i>, and <i>TBX21</i> associated with T-cell functions were significantly increased, whereas <i>FOXP3, TGFB1/B2</i>, and <i>IL-10RA</i> were strongly inhibited by <i>NPRL2</i>. A list of T-cell co-inhibitory molecules was also downregulated. Restoration of <i>NPRL2</i> exhibited significantly slower tumor growth in humanized-mice, which was associated with increased presence of human cytotoxic-T, and DC and decreased percentage of Treg, MDSC, and TAM in TME. <i>NPRL2</i>-stable cells showed a substantial increase in colony-formation inhibition and heightened sensitivity to carboplatin. Stable-expression of <i>NPRL2</i> resulted in the downregulation of MAPK and AKT-mTOR signaling. Taken-together, <i>NPRL2</i> gene-therapy induces antitumor activity on <i>KRAS/STK11<sup>mt</sup></i>/aPD1<sup>R</sup> tumors through DC-mediated antigen-presentation and cytotoxic immune-cell activation.</p>\",\"PeriodicalId\":11640,\"journal\":{\"name\":\"eLife\",\"volume\":\"13 \",\"pages\":\"\"},\"PeriodicalIF\":6.4000,\"publicationDate\":\"2025-02-11\",\"publicationTypes\":\"Journal Article\",\"fieldsOfStudy\":null,\"isOpenAccess\":false,\"openAccessPdf\":\"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11813225/pdf/\",\"citationCount\":\"0\",\"resultStr\":null,\"platform\":\"Semanticscholar\",\"paperid\":null,\"PeriodicalName\":\"eLife\",\"FirstCategoryId\":\"99\",\"ListUrlMain\":\"https://doi.org/10.7554/eLife.98258\",\"RegionNum\":1,\"RegionCategory\":\"生物学\",\"ArticlePicture\":[],\"TitleCN\":null,\"AbstractTextCN\":null,\"PMCID\":null,\"EPubDate\":\"\",\"PubModel\":\"\",\"JCR\":\"Q1\",\"JCRName\":\"BIOLOGY\",\"Score\":null,\"Total\":0}","platform":"Semanticscholar","paperid":null,"PeriodicalName":"eLife","FirstCategoryId":"99","ListUrlMain":"https://doi.org/10.7554/eLife.98258","RegionNum":1,"RegionCategory":"生物学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q1","JCRName":"BIOLOGY","Score":null,"Total":0}
NPRL2 gene therapy induces effective antitumor immunity in KRAS/STK11 mutant anti-PD1 resistant metastatic non-small cell lung cancer (NSCLC) in a humanized mouse model.
Expression of NPRL2/TUSC4, a tumor-suppressor gene, is reduced in many cancers including NSCLC. Restoration of NPRL2 induces DNA damage, apoptosis, and cell-cycle arrest. We investigated NPRL2 antitumor immune responses in aPD1R/KRAS/STK11mt NSCLC in humanized-mice. Humanized-mice were generated by transplanting fresh human cord blood-derived CD34 stem cells into sub-lethally irradiated NSG mice. Lung-metastases were developed from KRAS/STK11mt/aPD1R A549 cells and treated with NPRL2 w/wo pembrolizumab. NPRL2-treatment reduced lung metastases significantly, whereas pembrolizumab was ineffective. Antitumor effect was greater in humanized than non-humanized-mice. NPRL2 + pembrolizumab was not synergistic in KRAS/STK11mt/aPD1R tumors but was synergistic in KRASwt/aPD1S H1299. NPRL2 also showed a significant antitumor effect on KRASmt/aPD1R LLC2 syngeneic-tumors. The antitumor effect was correlated with increased infiltration of human cytotoxic-T, HLA-DR+DC, CD11c+DC, and downregulation of myeloid and regulatory-T cells in TME. Antitumor effect was abolished upon in-vivo depletion of CD8-T, macrophages, and CD4-T cells whereas remained unaffected upon NK-cell depletion. A distinctive protein-expression profile was found after NPRL2 treatment. IFNγ, CD8b, and TBX21 associated with T-cell functions were significantly increased, whereas FOXP3, TGFB1/B2, and IL-10RA were strongly inhibited by NPRL2. A list of T-cell co-inhibitory molecules was also downregulated. Restoration of NPRL2 exhibited significantly slower tumor growth in humanized-mice, which was associated with increased presence of human cytotoxic-T, and DC and decreased percentage of Treg, MDSC, and TAM in TME. NPRL2-stable cells showed a substantial increase in colony-formation inhibition and heightened sensitivity to carboplatin. Stable-expression of NPRL2 resulted in the downregulation of MAPK and AKT-mTOR signaling. Taken-together, NPRL2 gene-therapy induces antitumor activity on KRAS/STK11mt/aPD1R tumors through DC-mediated antigen-presentation and cytotoxic immune-cell activation.
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