Transcriptional control of the MUC16 promoter facilitates follicle-stimulating hormone peptide-conjugated shRNA nanoparticle-mediated inhibition of ovarian carcinoma <i>in vivo</i>

Zhang, Mingxing; Hong, Shanshan; Cai, Qingsheng; Zhang, Meng; Zhang, Xiaoyan; Xu, Congjian

doi:10.1080/10717544.2018.1451934

Cited by 11 publications

(9 citation statements)

References 37 publications

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“…In particular, nanoparticles carrying the RI variant of the peptide FP21 showed to bind FSHR (Table 1). They were thus used as an ovarian cancer targeted delivery system [57][58][59], showing improved biostability compared to the parent peptide, with no degradation even after 12 h incubation with proteolytic enzymes. The data obtained on the RI peptide encouraged further developments and optimizations of the molecule for treating ovarian cancers expressing FSHR [57].…”

Section: Anticancer Applications-diagnosticmentioning

confidence: 99%

“…In another study, Zhang et al demonstrated that the RI derivative of the same peptide FP21 conjugated to nanocarriers had significantly enhanced anti-tumor effects working by reducing the tumor volumes in nude mice from 33.3% to 58.5%. This effect was likely amplified by the high resistance of the ligand to hydrolysis [57][58][59]. Another tumor promoter is the Transferrin receptor (TfR), an important transmembrane glycoprotein involved in iron transport.…”

Section: Anticancer Applications-diagnosticmentioning

confidence: 99%

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Recent Applications of Retro-Inverso Peptides

Doti

Mardirossian

Sandomenico

et al. 2021

IJMS

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Natural and de novo designed peptides are gaining an ever-growing interest as drugs against several diseases. Their use is however limited by the intrinsic low bioavailability and poor stability. To overcome these issues retro-inverso analogues have been investigated for decades as more stable surrogates of peptides composed of natural amino acids. Retro-inverso peptides possess reversed sequences and chirality compared to the parent molecules maintaining at the same time an identical array of side chains and in some cases similar structure. The inverted chirality renders them less prone to degradation by endogenous proteases conferring enhanced half-lives and an increased potential as new drugs. However, given their general incapability to adopt the 3D structure of the parent peptides their application should be careful evaluated and investigated case by case. Here, we review the application of retro-inverso peptides in anticancer therapies, in immunology, in neurodegenerative diseases, and as antimicrobials, analyzing pros and cons of this interesting subclass of molecules.

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Section: Anticancer Applications-diagnosticmentioning

confidence: 99%

Section: Anticancer Applications-diagnosticmentioning

confidence: 99%

Recent Applications of Retro-Inverso Peptides

Doti

Mardirossian

Sandomenico

et al. 2021

IJMS

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“…5A). The typical design of artificial promoters is the combination of one or more tandem transcription factor binding sites whose activity are confined only in the cell state of interest and minimal promoter sequence [195][196][197][198][199][200]. Recently, the group of Wang Yangming from Peking University used miRNAs in the cell in combination with the CRISPRa/i system to construct a sensor element that can sense the state in the cell [194] (Fig.…”

Section: Reprogramming Of Cell Fate and Cellular Behaviorsmentioning

confidence: 99%

Recent progress in research and application of engineered implanted cells for biomedical applications

Chen,

Zhang,

2021

Quant. Biol.

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Background: The core concept of cell engineering is the use of synthetic biological methods to engineer and design genetically modified cells with specific functions, which has revolutionized the biotechnology industry and cell therapy. Implanted cells play an important role in the cell therapy, but the currently used implanted cells are unable to fully meet the needs of researchers and clinicians. Therefore, the construction of engineered implanted cells has become a new research area, with many groups exploring the working principles of implanted cells, allowing them to better exert their repair function. Results: Based on the existing cell engineering platforms, this paper summarizes the main types of chassis cells used in implanted cell engineering, progress in the development of gene editing tools and delivery systems, as well as strategies for the construction of engineered implanted cells. Conclusions: The rational use of synthetic biology methods to program and control the function of implanted cells with high spatiotemporal accuracy provides new ideas for the development of cell therapy, and opens up new possibilities for exploring the mechanism of implanted cell action to allow them to better exert their role in promoting the progress of repair.

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“…An explanation for why CA-125 is highly expressed in gynecological cancer cells, especially in ovarian cancer cells, but rarely in other cancer cells remains elusive. Transcriptional regulation of MUC16 is also still poorly defined [ 16 , 17 ]. Thapi et al initially investigated the MUC16 promoter and planned to assess the putative transcriptional factor that controlled CA-125 expression, as presented in an AACR abstract in 2011 [ 16 ], but no follow-up information has been published.…”

Section: Introductionmentioning

confidence: 99%

Targeting CA-125 Transcription by Development of a Conditionally Replicative Adenovirus for Ovarian Cancer Treatment

Yue

Yang

Yao

et al. 2021

Cancers

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CA-125, encoded by the MUC16 gene, is highly expressed in most ovarian cancer cells and thus serves as a tumor marker for monitoring disease progression or treatment response in ovarian cancer patients. However, targeting MUC16/CA-125 for ovarian cancer treatment has not been successful to date. In the current study, we performed multiple steps of high-fidelity PCR and obtained a 5 kb DNA fragment upstream of the human MUC16 gene. Reporter assays indicate that this DNA fragment possesses transactivation activity in CA-125-high cancer cells, but not in CA-125-low cancer cells, indicating that the DNA fragment contains the transactivation region that controls specific expression of the MUC16 gene in ovarian cancer cells. We further refined the promoter and found a 1040 bp fragment with similar transcriptional activity and specificity. We used this refined MUC16 promoter to replace the E1A promoter in the adenovirus type 5 genome DNA, where E1A is an essential gene for adenovirus replication. We then generated a conditionally replicative oncolytic adenovirus (CRAd) that replicates in and lyses CA-125-high cancer cells, but not CA-125-low or -negative cancer cells. In vivo studies showed that intraperitoneal virus injection prolonged the survival of NSG mice inoculated intraperitoneally (ip) with selected ovarian cancer cell lines. Furthermore, the CRAd replicates in and lyses primary ovarian cancer cells, but not normal cells, collected from ovarian cancer patients. Collectively, these data indicate that targeting MUC16 transactivation utilizing CRAd is a feasible approach for ovarian cancer treatment that warrants further investigation.

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Transcriptional control of the MUC16 promoter facilitates follicle-stimulating hormone peptide-conjugated shRNA nanoparticle-mediated inhibition of ovarian carcinoma in vivo

Cited by 11 publications

References 37 publications

Recent Applications of Retro-Inverso Peptides

Recent Applications of Retro-Inverso Peptides

Recent progress in research and application of engineered implanted cells for biomedical applications

Targeting CA-125 Transcription by Development of a Conditionally Replicative Adenovirus for Ovarian Cancer Treatment

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