Potentiation of E7 antisense RNA-induced antitumor immunity by co-delivery of IL-12 gene in HPV16 DNA-positive mouse tumor
Down-regulation of oncogene expression by antisense-based gene therapy has been extensively studied, and in some cases, therapeutic effects have been demonstrated. We have previously shown that down-regulation of HPV16 E6 and E7 gene expression inhibited HPV DNA-positive C3 mouse tumor growth. Altho...
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| Veröffentlicht in: | Gene therapy 1998-11, Vol.5 (11), p.1462-1471 |
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| creator | HE, Y. K LUI, V. W.-Y BAAR, J WANG, L SHURIN, M ALMONTE, C WATKINS, S. C HUANG, L |
| description | Down-regulation of oncogene expression by antisense-based gene therapy has been extensively studied, and in some cases, therapeutic effects have been demonstrated. We have previously shown that down-regulation of HPV16 E6 and E7 gene expression inhibited HPV DNA-positive C3 mouse tumor growth. Although not all of the tumor cells were transfected by pU6E7AS plasmid, complete tumor regression was achieved if the tumor size was small at the start of therapy in a syngeneic host. This suggests that some other antitumor mechanisms may be involved in addition to the direct down-regulation of HPV16 E7 oncogene expression by the antisense effect of E7AS. In the current study, we demonstrated that E7AS induces tumor cell apoptosis. More importantly, a strong antitumor immune response was elicited in the pU6E7AS-treated and tumor-regressed mice. There was no tumor growth after rechallenging the tumor-regressed mice with 1 million C3 cells. This E7AS-induced antitumor immune response was augmented by co-delivery of mIL-12 cytokine gene. The combination therapy strategy resulted in complete regression of 26 of 28 (93%) tumors. Only 12 of 31 (38%) tumors from the group treated with pU6E7AS alone and 14 of 28 (50%) tumors from the group treated with pCMVmIL-12 alone had completely regressed. Complete regression was also demonstrated in tumors located 1 cm from the treated tumors, which indicates that a systemic antitumor effect was induced by E7AS and mIL-12. Immunohistochemistry demonstrated that a significant amount of CD4+ and CD8+ cells infiltrated into tumors treated with pU6E7AS, pCMVmIL-12 and pU6E7AS+pCMVmIL-12. These data indicate that host immunity is an important factor for antisense-based gene therapy approach which can be further enhanced by combination with cytokine gene therapy. |
| doi_str_mv | 10.1038/sj.gt.3300769 |
| format | Article |
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K ; LUI, V. W.-Y ; BAAR, J ; WANG, L ; SHURIN, M ; ALMONTE, C ; WATKINS, S. C ; HUANG, L</creator><creatorcontrib>HE, Y. K ; LUI, V. W.-Y ; BAAR, J ; WANG, L ; SHURIN, M ; ALMONTE, C ; WATKINS, S. C ; HUANG, L</creatorcontrib><description>Down-regulation of oncogene expression by antisense-based gene therapy has been extensively studied, and in some cases, therapeutic effects have been demonstrated. We have previously shown that down-regulation of HPV16 E6 and E7 gene expression inhibited HPV DNA-positive C3 mouse tumor growth. Although not all of the tumor cells were transfected by pU6E7AS plasmid, complete tumor regression was achieved if the tumor size was small at the start of therapy in a syngeneic host. This suggests that some other antitumor mechanisms may be involved in addition to the direct down-regulation of HPV16 E7 oncogene expression by the antisense effect of E7AS. In the current study, we demonstrated that E7AS induces tumor cell apoptosis. More importantly, a strong antitumor immune response was elicited in the pU6E7AS-treated and tumor-regressed mice. There was no tumor growth after rechallenging the tumor-regressed mice with 1 million C3 cells. This E7AS-induced antitumor immune response was augmented by co-delivery of mIL-12 cytokine gene. The combination therapy strategy resulted in complete regression of 26 of 28 (93%) tumors. Only 12 of 31 (38%) tumors from the group treated with pU6E7AS alone and 14 of 28 (50%) tumors from the group treated with pCMVmIL-12 alone had completely regressed. Complete regression was also demonstrated in tumors located 1 cm from the treated tumors, which indicates that a systemic antitumor effect was induced by E7AS and mIL-12. Immunohistochemistry demonstrated that a significant amount of CD4+ and CD8+ cells infiltrated into tumors treated with pU6E7AS, pCMVmIL-12 and pU6E7AS+pCMVmIL-12. These data indicate that host immunity is an important factor for antisense-based gene therapy approach which can be further enhanced by combination with cytokine gene therapy.</description><identifier>ISSN: 0969-7128</identifier><identifier>EISSN: 1476-5462</identifier><identifier>DOI: 10.1038/sj.gt.3300769</identifier><identifier>PMID: 9930299</identifier><language>eng</language><publisher>Basingstoke: Nature Publishing Group</publisher><subject>AIDS/HIV ; Animals ; Antisense RNA ; Antisense therapy ; Antitumor activity ; Apoptosis ; Biological and medical sciences ; Biotechnology ; CD4 antigen ; CD4-Positive T-Lymphocytes - immunology ; CD8 antigen ; CD8-Positive T-Lymphocytes - immunology ; Cytokines ; Deoxyribonucleic acid ; DNA ; E7 gene ; Fundamental and applied biological sciences. Psychology ; Gene expression ; Gene Expression Regulation ; Gene therapy ; Genetic Therapy - methods ; Genetic Vectors ; Health. Pharmaceutical industry ; Human papillomavirus 16 ; Immune response ; Immunohistochemistry ; Industrial applications and implications. Economical aspects ; Interleukin 12 ; Interleukin-12 - genetics ; Mice ; Microscopy, Fluorescence ; Neoplasms, Experimental - immunology ; Neoplasms, Experimental - pathology ; Neoplasms, Experimental - therapy ; Oncogene Proteins, Viral - genetics ; Papillomaviridae - genetics ; Papillomavirus E7 Proteins ; RNA, Antisense ; Transfection - methods ; Tumor cells ; Tumor Virus Infections - immunology ; Tumor Virus Infections - pathology ; Tumor Virus Infections - therapy ; Tumors</subject><ispartof>Gene therapy, 1998-11, Vol.5 (11), p.1462-1471</ispartof><rights>1999 INIST-CNRS</rights><rights>Macmillan Publishers Limited 1998.</rights><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed><citedby>FETCH-LOGICAL-c376t-ea057b7ce6ba1f3b1200e6f7140c7f5654a9be5d22a856766ad30dbf8e5bce5e3</citedby></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,776,780,27901,27902</link.rule.ids><backlink>$$Uhttp://pascal-francis.inist.fr/vibad/index.php?action=getRecordDetail&idt=1601144$$DView record in Pascal Francis$$Hfree_for_read</backlink><backlink>$$Uhttps://www.ncbi.nlm.nih.gov/pubmed/9930299$$D View this record in MEDLINE/PubMed$$Hfree_for_read</backlink></links><search><creatorcontrib>HE, Y. K</creatorcontrib><creatorcontrib>LUI, V. W.-Y</creatorcontrib><creatorcontrib>BAAR, J</creatorcontrib><creatorcontrib>WANG, L</creatorcontrib><creatorcontrib>SHURIN, M</creatorcontrib><creatorcontrib>ALMONTE, C</creatorcontrib><creatorcontrib>WATKINS, S. C</creatorcontrib><creatorcontrib>HUANG, L</creatorcontrib><title>Potentiation of E7 antisense RNA-induced antitumor immunity by co-delivery of IL-12 gene in HPV16 DNA-positive mouse tumor</title><title>Gene therapy</title><addtitle>Gene Ther</addtitle><description>Down-regulation of oncogene expression by antisense-based gene therapy has been extensively studied, and in some cases, therapeutic effects have been demonstrated. We have previously shown that down-regulation of HPV16 E6 and E7 gene expression inhibited HPV DNA-positive C3 mouse tumor growth. Although not all of the tumor cells were transfected by pU6E7AS plasmid, complete tumor regression was achieved if the tumor size was small at the start of therapy in a syngeneic host. This suggests that some other antitumor mechanisms may be involved in addition to the direct down-regulation of HPV16 E7 oncogene expression by the antisense effect of E7AS. In the current study, we demonstrated that E7AS induces tumor cell apoptosis. More importantly, a strong antitumor immune response was elicited in the pU6E7AS-treated and tumor-regressed mice. There was no tumor growth after rechallenging the tumor-regressed mice with 1 million C3 cells. This E7AS-induced antitumor immune response was augmented by co-delivery of mIL-12 cytokine gene. The combination therapy strategy resulted in complete regression of 26 of 28 (93%) tumors. Only 12 of 31 (38%) tumors from the group treated with pU6E7AS alone and 14 of 28 (50%) tumors from the group treated with pCMVmIL-12 alone had completely regressed. Complete regression was also demonstrated in tumors located 1 cm from the treated tumors, which indicates that a systemic antitumor effect was induced by E7AS and mIL-12. Immunohistochemistry demonstrated that a significant amount of CD4+ and CD8+ cells infiltrated into tumors treated with pU6E7AS, pCMVmIL-12 and pU6E7AS+pCMVmIL-12. These data indicate that host immunity is an important factor for antisense-based gene therapy approach which can be further enhanced by combination with cytokine gene therapy.</description><subject>AIDS/HIV</subject><subject>Animals</subject><subject>Antisense RNA</subject><subject>Antisense therapy</subject><subject>Antitumor activity</subject><subject>Apoptosis</subject><subject>Biological and medical sciences</subject><subject>Biotechnology</subject><subject>CD4 antigen</subject><subject>CD4-Positive T-Lymphocytes - immunology</subject><subject>CD8 antigen</subject><subject>CD8-Positive T-Lymphocytes - immunology</subject><subject>Cytokines</subject><subject>Deoxyribonucleic acid</subject><subject>DNA</subject><subject>E7 gene</subject><subject>Fundamental and applied biological sciences. 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K</au><au>LUI, V. W.-Y</au><au>BAAR, J</au><au>WANG, L</au><au>SHURIN, M</au><au>ALMONTE, C</au><au>WATKINS, S. C</au><au>HUANG, L</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Potentiation of E7 antisense RNA-induced antitumor immunity by co-delivery of IL-12 gene in HPV16 DNA-positive mouse tumor</atitle><jtitle>Gene therapy</jtitle><addtitle>Gene Ther</addtitle><date>1998-11-01</date><risdate>1998</risdate><volume>5</volume><issue>11</issue><spage>1462</spage><epage>1471</epage><pages>1462-1471</pages><issn>0969-7128</issn><eissn>1476-5462</eissn><abstract>Down-regulation of oncogene expression by antisense-based gene therapy has been extensively studied, and in some cases, therapeutic effects have been demonstrated. We have previously shown that down-regulation of HPV16 E6 and E7 gene expression inhibited HPV DNA-positive C3 mouse tumor growth. Although not all of the tumor cells were transfected by pU6E7AS plasmid, complete tumor regression was achieved if the tumor size was small at the start of therapy in a syngeneic host. This suggests that some other antitumor mechanisms may be involved in addition to the direct down-regulation of HPV16 E7 oncogene expression by the antisense effect of E7AS. In the current study, we demonstrated that E7AS induces tumor cell apoptosis. More importantly, a strong antitumor immune response was elicited in the pU6E7AS-treated and tumor-regressed mice. There was no tumor growth after rechallenging the tumor-regressed mice with 1 million C3 cells. This E7AS-induced antitumor immune response was augmented by co-delivery of mIL-12 cytokine gene. The combination therapy strategy resulted in complete regression of 26 of 28 (93%) tumors. Only 12 of 31 (38%) tumors from the group treated with pU6E7AS alone and 14 of 28 (50%) tumors from the group treated with pCMVmIL-12 alone had completely regressed. Complete regression was also demonstrated in tumors located 1 cm from the treated tumors, which indicates that a systemic antitumor effect was induced by E7AS and mIL-12. Immunohistochemistry demonstrated that a significant amount of CD4+ and CD8+ cells infiltrated into tumors treated with pU6E7AS, pCMVmIL-12 and pU6E7AS+pCMVmIL-12. These data indicate that host immunity is an important factor for antisense-based gene therapy approach which can be further enhanced by combination with cytokine gene therapy.</abstract><cop>Basingstoke</cop><pub>Nature Publishing Group</pub><pmid>9930299</pmid><doi>10.1038/sj.gt.3300769</doi><tpages>10</tpages></addata></record> |
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| subjects | AIDS/HIV Animals Antisense RNA Antisense therapy Antitumor activity Apoptosis Biological and medical sciences Biotechnology CD4 antigen CD4-Positive T-Lymphocytes - immunology CD8 antigen CD8-Positive T-Lymphocytes - immunology Cytokines Deoxyribonucleic acid DNA E7 gene Fundamental and applied biological sciences. Psychology Gene expression Gene Expression Regulation Gene therapy Genetic Therapy - methods Genetic Vectors Health. Pharmaceutical industry Human papillomavirus 16 Immune response Immunohistochemistry Industrial applications and implications. Economical aspects Interleukin 12 Interleukin-12 - genetics Mice Microscopy, Fluorescence Neoplasms, Experimental - immunology Neoplasms, Experimental - pathology Neoplasms, Experimental - therapy Oncogene Proteins, Viral - genetics Papillomaviridae - genetics Papillomavirus E7 Proteins RNA, Antisense Transfection - methods Tumor cells Tumor Virus Infections - immunology Tumor Virus Infections - pathology Tumor Virus Infections - therapy Tumors |
| title | Potentiation of E7 antisense RNA-induced antitumor immunity by co-delivery of IL-12 gene in HPV16 DNA-positive mouse tumor |
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