Ranpirnase (Frog RNase) Targeted with a Humanized, Internalizing, Anti–Trop-2 Antibody Has Potent Cytotoxicity against Diverse Epithelial Cancer Cells

Chang, Chien-Hsing; Gupta, Pankaj; Michel, Rosana B.; Loo, Meiyu; Wang, Yang; Cardillo, Thomas M.; Goldenberg, David M.

doi:10.1158/1535-7163.mct-10-0338

Cited by 52 publications

(41 citation statements)

References 48 publications

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“…1). Ranpirnase is the smallest member of the ribonuclease (RNase A) superfamily, and appears to be a promising drug with broad clinical application in tumor treatment due to its moderate cytotoxicity, unique synergy, low immunogenicity and few side effects (1)(2)(3)(4)(5)(6)(7)(8)(9)(10). Between 1996 and 2004, Tamir Biotechnology, Inc. (formerly Alfacell Corporation) successively conducted clinical investigations regarding the effects of ranpirnase on breast cancer, pancreatic cancer, renal cell carcinoma, non-small cell lung cancer and malignant mesothelioma, for which the therapeutic effect was the most significant with few side effects.…”

Section: Introductionmentioning

confidence: 99%

Recombinant expression, different downstream processing of the disulfide-rich anti-tumor peptide Ranpirnase and its effect on the growth of human glioma cell line SHG-44

Wang

Guo

2013

Biomedical Reports

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Abstract. Ranpirnase (Onconase) is a frogspawn-derived disulfide-rich peptide with ribonuclease activity that may be used for tumor treatment. In the present study, we established an efficient approach for preparing mature ranpirnase which may be used for research and therapeutic purposes. The designed ranpirnase precursors carried a 6xHis-tag and were recombinantly expressed in Escherichia coli. After S-sulfonation, the precursors were purified by immobilized metal-ion affinity chromatography. Following removal of the tag by aminopeptidase cleavage, cyclization and in vitro oxidative refolding, the mature ranpirnase was obtained with considerable yield, and the yield of mature ranpirnase was ~50-60 mg per liter cultures. In addition, ranpirnase inhibited the growth of human glioma cells SHG-44 in a dose-dependent manner. Thus the present study has provided an efficient approach for the preparation of active ranpirnase and its analogues for future studies.

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Section: Introductionmentioning

confidence: 99%

Recombinant expression, different downstream processing of the disulfide-rich anti-tumor peptide Ranpirnase and its effect on the growth of human glioma cell line SHG-44

Wang

Guo

2013

Biomedical Reports

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“…Onconase, which is derived from Rana pipiens, and RC-RNase, which is derived from Rana catesbeiana, each belong to the RNase A superfamily (9,10). RC-RNase and Onconase have been revealed to demonstrate antitumor activity (10)(11)(12)(13). Previous studies have reported that RC-RNase is able to exert cytotoxic effects in various tumor cells, including cervical cancer, leukemia, hepatoma and breast cancer cells (11,(14)(15)(16).…”

Section: Introductionmentioning

confidence: 99%

“…In addition, numerous studies have indicated that RC-RNase is able to trigger distinct cell death mechanisms in various tumor cell types (10,11,14,17). By contrast, previous studies have also revealed that Onconase can exert antitumor activities in numerous tumor cells, including cervical, breast, colon, pancreatic and prostate cancer cells (12,(18)(19)(20)(21)(22).…”

Section: Introductionmentioning

confidence: 99%

Rana catesbeiana ribonuclease induces cell apoptosis via the caspase-9/-3 signaling pathway in human glioblastoma DBTRG, GBM8901 and GBM8401 cell lines

Chen¹,

Yiang²,

Lin³

et al. 2015

Oncology Letters

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Abstract. Human glioblastoma multiforme is one of the most aggressive malignant brain tumor types, and the mean survival time of patients with a brain tumor is <2 years when traditional therapies are administered. Thus, numerous studies have focused on the development of novel treatments for brain tumors. Frog ribonucleases, such as Onconase and Rana catesbeiana ribonuclease (RC-RNase), exert antitumor effects on various tumor cells, including cervical cancer, breast cancer, hepatoma, leukemia, pancreatic cancer and prostate cancer cells. In addition, frog Onconase has been applied as a treatment in clinical trials. However, the antitumor effects of frog ribonucleases on brain tumors are unclear. Previous studies have indicated that RC-RNase demonstrates a decreased cytotoxic effect in normal cells compared with Onconase. Therefore, the present study investigated the ability of RC-RNase to exert antitumor activities on human glioblastoma.It was found that RC-RNase inhibits the growth of the human glioblastoma DBTRG, GBM8901 and GBM8401 cells. In addition, the present study revealed that RC-RNase induces caspase-9/-3 activity and triggers the apoptotic cell death pathway in human glioblastoma cells. Notably, it was also demonstrated that RC-RNase effectively inhibits the growth of human glioblastoma tumors in a nude mouse model. Overall, the present study indicates that RC-RNase may be a potential agent for the treatment of human glioblastoma.

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“…ONC is the smallest member of the ribonuclease A (RNase A) family (Porta et al, 2008) and is considered unique since it has entered clinical trials (Darzynkiewicz et al, 1988;Ardelt et al, 1991). Once ONC is internalized and sorted to the cytosol, it could degrade the target tRNA to inhibit protein synthesis (Chang et al, 2010); however, the mechanism of its cytotoxicity is not completely understood. The company Timair (formerly known as Alfacell) has successively carried out I-III phase clinical trials of ONC on breast cancer, pancreatic cancer, non-small cell lung cancer, and malignant melanoma (Tian et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

Linker length affects expression and bioactivity of the onconase fusion protein in Pichia pastoris

Xu¹,

Ding²,

Cui³

et al. 2015

Genet. Mol. Res.

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ABSTRACT. The aim of this study was to analyze the effect of linker length on the expression and biological activity of recombinant protein onconase (ONC) in fusion with human serum albumin (HSA) in Pichia pastoris. Four flexible linkers with different lengths namely Linker L0, L1: (GGGGS) 1 , L2: (GGGGS) 2 , and L3:(GGGGS) 3 were inserted into the fusion gene and referred to as HSA-n-ONC, where N = 0, 5, 10, or 15. The sequence of the fusion gene HSA-ONC was designed based on the GC content and codon bias in P. pastoris; the signal peptide of albumin was used as the secretion signal. Gene sequences coding for the fusion protein with different linkers were inserted into pPICZα-A to form recombinant plasmids pPICZα-A/HSA-n-ONC, which were then transformed into P. pastoris X-33 for protein expression. Ideal conditions for expression of the fusion proteins were optimized at a small scale, using shake flasks before proceeding to mass production in 10-L fermenters. The recombinant fusion proteins 19361Linker length affects HSA-fused ONC in P. pastoris ©FUNPEC-RP www.funpecrp.com.br Genetics and Molecular Research 14 (4): 19360-19370 (2015) were purified by aqueous two-phase extraction coupled with DEAE anion exchange chromatography, and their cytotoxic effect on the tumor cell was evaluated by the sulforhodamine B assay. The results showed that the expressed amount of fusion proteins had no significant relationship with the length of different linkers and rHSA-0-ONC had no cytotoxic effect on the tumor cells. While rHSA-5-ONC and rHSA-10-ONC had a weak cytotoxic effect, rHSA-15-ONC could kill various tumor cells in vitro. In summary, the biological activity of the fusion protein gradually improved with increasing length of the linker.

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Ranpirnase (Frog RNase) Targeted with a Humanized, Internalizing, Anti–Trop-2 Antibody Has Potent Cytotoxicity against Diverse Epithelial Cancer Cells

Cited by 52 publications

References 48 publications

Recombinant expression, different downstream processing of the disulfide-rich anti-tumor peptide Ranpirnase and its effect on the growth of human glioma cell line SHG-44

Recombinant expression, different downstream processing of the disulfide-rich anti-tumor peptide Ranpirnase and its effect on the growth of human glioma cell line SHG-44

Rana catesbeiana ribonuclease induces cell apoptosis via the caspase-9/-3 signaling pathway in human glioblastoma DBTRG, GBM8901 and GBM8401 cell lines

Linker length affects expression and bioactivity of the onconase fusion protein in Pichia pastoris

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