Construction of a novel vector expressing Survivin‑shRNA and fusion suicide gene yCDglyTK and its application in inhibiting proliferation and migration of colon cancer cells

Ye, Ling; Yang, Yuan; Ma, Xinyu; Li, Dan; Xu, Meili; Tan, Pan; Long, Ling; Wang, Haiqin; Liu, Ting; Guo, Ying

doi:10.3892/etm.2017.5154

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Gene Therapy Targeting Birc51

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2019

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“…A combined gene therapy using BIRC5 siRNA and the fusion suicide gene yCDglyTK system displayed a relevant antitumor effect, inducing apoptosis more efficiently and eradicating colon cancer cells. Furthermore, this therapeutic system was able to inhibit the migration of colon cancer cells in vitro (Ye et al, 2017).…”

Section: Gene Therapy Targeting Birc5mentioning

confidence: 96%

BIRC5 (baculoviral IAP repeat containing 5)

Branco¹,

Jimenez²,

Machado-Neto³

et al. 2019

Atlas of Genetics and Cytogenetics in Oncology and Haematology

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BIRC5, also known as survivin, has been implicated in cell cycle progression and apoptosis avoidance. BIRC5 is highly expressed in embryonic tissues, however very low or absent in adult tissues. BIRC5 overexpression has been frequently associated to cancer development, a poor prognosis and chemoresistance. Besides that, different BIRC5 isoforms has been characterized and related to better or worse chemotherapy responses depending on the isoform and the cancer type. So far, many efforts have been conducted in order to deplete BIRC5 in cancer cells, including gene therapy, pharmacological and nanotechnological approaches. In this review, we will discuss the role of BIRC5 in cancer cell biology and its clinical significance, demonstrating its DNA/RNA and protein aspects, also its relevance for diagnosis and prognosis, and advances as a target for the treatment of different cancer types.

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Section: Gene Therapy Targeting Birc5mentioning

confidence: 96%