Transcriptionally Targeted In Vivo Gene Therapy for Carcinoembrionic Antigen-Producing Adenocarcinoma

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タイトル ( eng )
Transcriptionally Targeted In Vivo Gene Therapy for Carcinoembrionic Antigen-Producing Adenocarcinoma
作成者
Konishi Futoshi
Maeda Hiroyuki
Yamanishi Yuji
Hiyama Keiko
Ishioka Shinichi
Yamakido Michio
収録物名
Hiroshima Journal of Medical Sciences
48
3
開始ページ 79
終了ページ 89
収録物識別子
[PISSN] 0018-2052
[EISSN] 2433-7668
[NCID] AA00664312
抄録
Inoperable adenocarcinoma in colon or lung shows resistance to conventional anti-cancer therapy. For these cancers, the feasibility of transcriptionally targeted killing of carcinoembryonic antigen (CEA)-producing adenocarcinoma cells was investigated.  

Adenovirus vectors carrying a CEA promoter to express E. coli lacZ (AdCEALacZ) or herpes simplex thymidine kinase (AdCEATK) were made and their in vitro and in vivo tumoricidal effects on CEA-producing or non-producing colon and lung cancer cells were evaluated.  

In vitro infection with AdCEALacZ showed significantly higher CEA promoter-driven lacZ expression in CEA-producing adenocarcinoma cells including VMRC-LCD and LoVo than in CEA-non-producing cells. AdCEATK-infected LoVo showed higher sensitivity to ganciclovir than control vector-infected LoVo or AdCEATK-infected HeLa both in vitro and in subcutaneously implanted tumors of nude mice. Moreover, total tumor elimination in vivo was achieved by either pre-infection of as few as 30% of cells comprising tumors or by direct in vivo injection of AdCEATK to pre-established LoVo tumors. In addition, CEA promoter-driven lacZ expression in Lo Vo cells was enhanced by the addition ofinterleukin-6 (IL-6) in vitro.  

These results provide a rationale for CEA-promoter-driven, adenovirus-mediated gene therapy for CEA-producing adenocarcinomas in colon and lung with reduced toxicity to normal cells.
著者キーワード
Adenovirus-vector
HSV-TK
Interleukin-6
Cell-type-specific gene therapy
NDC分類
医学 [ 490 ]
言語
英語
資源タイプ 紀要論文
出版者
Hiroshima University Medical Press
発行日 1999-09
出版タイプ Version of Record(出版社版。早期公開を含む)
アクセス権 オープンアクセス
収録物識別子
[ISSN] 0018-2052
[NCID] AA00664312