Intratracheal Delivery of CX3CL1-Expressing Mesenchymal Stem Cells to Multiple Lung Tumors

被引:1
|
作者
Hong Xin
Ruowen Sun
Masahiko Kanehira
Takenori Takahata
Jugoh Itoh
Hiroyuki Mizuguchi
Yasuo Saijo
机构
[1] Tohoku University Graduate School of Medicine,Department of Molecular Medicine
[2] National Institute of Biomedical Innovation,Laboratory of Gene Transfer and Regulation
[3] Hirosaki University Graduate School of Medicine,Department of Medical Oncology
来源
Molecular Medicine | 2009年 / 15卷
关键词
Mesenchymal Stem Cells (MSCs); Multiple Lung Tumors; Intratracheal Administration; Intratracheal Injection; Mouse MSCs;
D O I
暂无
中图分类号
学科分类号
摘要
The lung is one of the organs to which cancers from solid tumors frequently metastasize. Multiple tumors in the lung are usually treated by systemic chemotherapy because of the lack of efficient methods of targeting antitumor agents to the lung. Although intratracheal administration is an ideal route for targeting multiple lung tumors, antitumor agents are often harmful to the organ or induce inflammation. Mesenchymal stem cells (MSCs), nonhematopoietic stem cells capable of differentiating into various mesoderm-type cells, have a propensity to migrate to and proliferate in tumor tissues after systemic administration. We intratracheally injected MSCs expressing CX3CL1 (MSC/RGDFKN) into the lung of lung tumor-bearing mice with multiple metastases of C26 or Lewis lung carcinoma (LLC). Antitumor effects were evaluated by counting the number of lung metastases and survival. We demonstrated the tropism of mouse MSCs to lung tumor tissues after intratracheal administration of GFP-positive MSCs. Intratracheal injection of MSC/RGDFKN strongly inhibited growth of lung metastases of C26 or LLC, and thus prolonged survival. Intratracheal injection of MSC/RGDFKN did not induce an inflammatory reaction in the lung. These results suggest that MSCs expressing antitumor agents can be delivered intratracheally into multiple lung tumor tissues without causing inflammation.
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页码:321 / 327
页数:6
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