Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic Cancer
Antiangiogenesis has been exploited as an effective approach to inhibit the growth of solid tumors. This technique has been evaluated using various vectors in several xenograft animal models to demonstrate the efficacy of endostatin gene therapy against cancer growth. However, previous studies have...
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SAGE Publishing
2008-08-01
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| Series: | Cell Transplantation |
| Online Access: | https://doi.org/10.3727/096368908786576525 |
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doaj-5e3f7c9aed4a4257a7975ab24f38a87f2020-11-25T01:25:47ZengSAGE PublishingCell Transplantation0963-68971555-38922008-08-011710.3727/096368908786576525Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic CancerZao Jiang0Gao-Jun Teng1Bao-An Chen2Zheng-Feng Xu3Jie Hu4Ze-Ye Shao5Department of Oncology, Zhongda Hospital, Southeast University, Nanjing, ChinaJiangsu Provincial Key Laboratory of Molecular Imaging, Zhongda Hospital, Southeast University, Nanjing, ChinaLaboratory of Hematology, Clinical Medical Collage, Southeast University, Nanjing, ChinaThe Center of Prenatal Diagnosis, Nanjing Maternity and Child Health Hospital, Nanjing Medical University, Nanjing, ChinaDepartment of Oncology, Zhongda Hospital, Southeast University, Nanjing, ChinaLaboratory of Hematology, Clinical Medical Collage, Southeast University, Nanjing, ChinaAntiangiogenesis has been exploited as an effective approach to inhibit the growth of solid tumors. This technique has been evaluated using various vectors in several xenograft animal models to demonstrate the efficacy of endostatin gene therapy against cancer growth. However, previous studies have not examined the use of cord blood CD34+ cells as endostatin-producing cells for gene therapy against hepatoma. This exploratory study was done to investigate the local effects of CD34+ cells transduced with the endostatin gene on a mouse xenograft tumor model. The human endostatin gene was transferred into CD34+ cells using the recombinant retrovirus plasmid, pLncx/endo. Expression was verified by RT-PCR and Western blot analyses, confirming the stable expression and secretion of endostatin from the transferred CD34+ cells. The proliferation of vascular endothelial cells was evaluated by MTT assay and found to decrease by about 59.9% when treated with the supernatant of cultured transfected CD34+ cells in vitro. These genetically modified cord blood CD34+ cells were implanted intratumorally and tumor regression was evaluated after 2 weeks. The average size of a xenograft tumor in the CD34+/endo group was reduced 31.39% compared to that in the untreated mice or those transplanted with CD34+ cells transduced with a control vector. The microvascular density of the tumor decreased 62.45% in the treated group. The expression of proliferation cell nuclear antigen (PCNA) also decreased significantly in the treated group. Moreover, the apoptotic index (AI) of tumors, as evaluated by TUNEL staining, was significantly enhanced in the treatment group. Our findings indicate that angiogenesis of the xenograft tumor in mice may be inhibited by local administration of genetically modified CD34+ cells expressing the endostatin gene. This novel approach may lead to a new direction of cell-based gene therapy for malignancy.https://doi.org/10.3727/096368908786576525 |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Zao Jiang Gao-Jun Teng Bao-An Chen Zheng-Feng Xu Jie Hu Ze-Ye Shao |
| spellingShingle |
Zao Jiang Gao-Jun Teng Bao-An Chen Zheng-Feng Xu Jie Hu Ze-Ye Shao Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic Cancer Cell Transplantation |
| author_facet |
Zao Jiang Gao-Jun Teng Bao-An Chen Zheng-Feng Xu Jie Hu Ze-Ye Shao |
| author_sort |
Zao Jiang |
| title |
Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic Cancer |
| title_short |
Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic Cancer |
| title_full |
Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic Cancer |
| title_fullStr |
Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic Cancer |
| title_full_unstemmed |
Local Effects of Retrovirally Transduced Endostatin-Expressing Human Umbilical Cord Blood CD34+ Cells on Transplanted Malignancy in a Mouse Model of Hepatic Cancer |
| title_sort |
local effects of retrovirally transduced endostatin-expressing human umbilical cord blood cd34+ cells on transplanted malignancy in a mouse model of hepatic cancer |
| publisher |
SAGE Publishing |
| series |
Cell Transplantation |
| issn |
0963-6897 1555-3892 |
| publishDate |
2008-08-01 |
| description |
Antiangiogenesis has been exploited as an effective approach to inhibit the growth of solid tumors. This technique has been evaluated using various vectors in several xenograft animal models to demonstrate the efficacy of endostatin gene therapy against cancer growth. However, previous studies have not examined the use of cord blood CD34+ cells as endostatin-producing cells for gene therapy against hepatoma. This exploratory study was done to investigate the local effects of CD34+ cells transduced with the endostatin gene on a mouse xenograft tumor model. The human endostatin gene was transferred into CD34+ cells using the recombinant retrovirus plasmid, pLncx/endo. Expression was verified by RT-PCR and Western blot analyses, confirming the stable expression and secretion of endostatin from the transferred CD34+ cells. The proliferation of vascular endothelial cells was evaluated by MTT assay and found to decrease by about 59.9% when treated with the supernatant of cultured transfected CD34+ cells in vitro. These genetically modified cord blood CD34+ cells were implanted intratumorally and tumor regression was evaluated after 2 weeks. The average size of a xenograft tumor in the CD34+/endo group was reduced 31.39% compared to that in the untreated mice or those transplanted with CD34+ cells transduced with a control vector. The microvascular density of the tumor decreased 62.45% in the treated group. The expression of proliferation cell nuclear antigen (PCNA) also decreased significantly in the treated group. Moreover, the apoptotic index (AI) of tumors, as evaluated by TUNEL staining, was significantly enhanced in the treatment group. Our findings indicate that angiogenesis of the xenograft tumor in mice may be inhibited by local administration of genetically modified CD34+ cells expressing the endostatin gene. This novel approach may lead to a new direction of cell-based gene therapy for malignancy. |
| url |
https://doi.org/10.3727/096368908786576525 |
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