Evaluation of tumor-specific promoter activities in melanoma

Lu, Baogen; Makhija, Sonia K.; Nettelbeck, Dirk M.; Rivera, Angel A.; Wang, M.; Komarova, Svetlana V.; Zhou, Fen; Yamamoto, Masato; Haisma, Hidde J.; Alvarez, Ronald D.; Curiel, David T.; Zhu, Zeng B.

doi:10.1038/sj.gt.3302385

Cited by 46 publications

(43 citation statements)

References 55 publications

(57 reference statements)

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“…A second approach involved the use of the survivin gene to express a ''payload'' cytotoxic gene in tumor cells. This ''suicidal'' strategy (41) relies on the fact that the survivin gene has virtually no transcriptional expression in normal tissues, including liver (42), as opposed to a 200-fold increased activity in tumor cells in vivo (43). When coupled to a proapoptotic protein, administration of the suicidal construct as a DNA-liposome formulation resulted in complete tumor eradication in xenograft models (43), thus offering good prospects for further clinical development.…”

Section: Molecular Antagonistsmentioning

confidence: 99%

Targeted therapy by disablingcrossroadsignaling networks: the survivin paradigm

Altieri

2006

Molecular Cancer Therapeutics

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Embedded in the concept of targeted cancer therapy is the expectation that disabling a single oncogenic pathway will eliminate the tumor cells and leave the normal tissues unscathed. Although validated by clinical responses in certain malignancies, challenges exist to generalize this approach to most tumors, as multiple genetic lesions, chromosomal instability, insensitivity of the cancer stem cell compartment, and emergence of drug resistance complicate the identification and therapeutic exploitation of a single, driving oncogenic pathway. Instead, broader therapeutic prospects may be offered by targeting crossroad signaling networks that are selectively exploited in cancer and oversee multiple aspects of tumor cell maintenance. One such pathway is centered on survivin, a cancer gene that intersects cell proliferation, cell survival, and the cellular stress response. Several clinical trials targeting survivin with a collection of approaches from immunotherapy to small-molecule antagonists are currently under way. By simultaneously disabling multiple signaling circuitries, targeting survivin may provide a novel perspective in rational cancer therapy selective for specific cancer mechanisms but broadly applicable to disparate tumors regardless of their genetic makeup. [Mol Cancer Ther 2006;5(3):478 -82]

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Section: Molecular Antagonistsmentioning

confidence: 99%

Targeted therapy by disablingcrossroadsignaling networks: the survivin paradigm

Altieri

2006

Molecular Cancer Therapeutics

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“…Numerous researches have validated the specificity and utility of survivin promoter for tumor targeting therapy [26]. Survivin is over-expressed in common cancers, but not in normal adult tissues [27][28][29]. A series of studies confirmed that survivin mRNA was expressed in 12 human hepatoma cell lines, and survivin protein was highly positive in 70% of liver cancers.…”

mentioning

confidence: 74%

Suppression of hepatoma tumor growth by systemic administration of the phytotoxin gelonin driven by the survivin promoter

Wang

Zhou²,

Li³

et al. 2013

neo

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Hepatocellular carcinoma (HCC) is one of the most common types of cancer worldwide. However, there is currently no effective therapy strategy in the clinical practice. Recombinant phytotoxin gelonin fused to other factors have been used to treat different cancers. But there have been no reports of gelonin gene therapy. In this study, we have constructed a recombinant plasmid which contained a tumor-specific survivin promoter to drive phytotoxin gelonin (pSur-Gel). And the cytotoxicity effects of pSur-Gel in HCC were also validated both in vitro and in vivo. The expression level of survivin was detetected in different liver cancer cell lines and nomal liver cell lines by western blot analysis, and a survivin promoter-driven green fluorescent protein (GFP) expression vectors (pSur-GFP) was also tested in liver cancer cell line HepG2 and normal liver cell line LO2. Moreover, phytotoxin gelonin expression experiment and cytotoxicity experiment of pSur-Gel was performed in HepG2 cells and LO2 cells in vitro. Furthermore, anti-tumor effect of pSur-Gel against HepG2 xenografts and toxicity of this gene were evaluated in the mice model. Finally, LDH release assay, apoptosis assay and immunoblot analyse LC3 conversion (LC3-I to LC3-II) were tested. We found that the expression of survivin protein was higher in liver cancer cell lines compared with the normal liver cells. Further study showed that the pSur-GFP and pSur-Gel was expressed specially in liver cancer cell other than in normal liver cells. pSur-Gel plasmid could effectively inhibit the proliferation of liver cancer cells (*P<0.05), and significantly repress the growth of HepG2 xenografts via intravenous in vivo (*P<0.05). Otherwise, compared to cytomegalovirus promoter-driven gelonin expression vectors (pCMV-Gel), no significantly systemic toxicity or organ injuries had been observed in pSur-Gel treated mice. Further studies revealed that the phytotoxin gelonin induced cell death might be mediated by apoptosis and the damage of cell membrane. Taken together, treating hepatocellular carcinoma with the pSur-Gel may be a novel and interesting cancer gene therapy protocol and is worthy of further development for future clinical trials.

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“…7 Aside from cellular targeting, transcriptional targeting has recently also been assessed in primary melanoma cells, the most important skin tumor. 8 In these experiments, the survivin promotor exhibited the highest activity in melanoma cells, while normal tissues such as liver, lung and spleen were relatively spared. Combinations of cellular targeting using RGD fiber-mutant adenovirus vectors that contain an alpha-v integrin tropism with the melanoma-specific tyrosinase promotor or human telomerase reverse transcriptase (TERT) promotor have shown increased gene expression in tumor cells with a relative quiescence in normal cells.…”

Section: Skin Gene Therapy Ur Henggementioning

confidence: 92%

Gene therapy progress and prospects: the skin – easily accessible, but still far away

Hengge

2006

Gene Ther

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Significant progress has been made in corrective gene therapy of inherited skin diseases. This includes advances in vector technology, targeted gene expression, gene replacement, and the availability of appropriate animal models for a variety of candidate diseases. In addition, an increased understanding of the uptake and trafficking mechanisms inside keratinocytes has evolved. Topical application facilitates DNA vaccination through the skin, albeit clinical benefits have not yet materialized. However, the translation into clinical trials has only been partially mastered. The latter and the control of immune responses represent challenges for the research community.

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Evaluation of tumor-specific promoter activities in melanoma

Cited by 46 publications

References 55 publications

Targeted therapy by disablingcrossroadsignaling networks: the survivin paradigm

Targeted therapy by disablingcrossroadsignaling networks: the survivin paradigm

Suppression of hepatoma tumor growth by systemic administration of the phytotoxin gelonin driven by the survivin promoter

Gene therapy progress and prospects: the skin – easily accessible, but still far away

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