CIGB-300, a novel proapoptotic peptide that impairs the CK2 phosphorylation and exhibits anticancer properties both in vitro and in vivo

Perea, Silvio E.; Reyes, Osvaldo; Baladrón, Idania; Perera, Yasser; Fariña, Hernán G.; Gil, Jeovanis; Rodriguez, Arielis; Bacardí, Dania; Marcelo, José; Cosme, Karelia; Cruz, M. Meira e; Valenzuela, Carmen; López-Saura, Pedro; Puchades, Yaquelín; Serrano, Joem M.; Mendoza, Osmani; Castellanos, Lila; Sánchez, Aniel; Betancourt, Lázaro; Besada, Vladimir; Ricardo, Silva; López, Ernesto; Falcón, Viviana; Hernández, Ignacio; Solares, Margarita; Santana, Agueda; Díaz, Alina; Ramos, Thelvia; Lopez, Carlos M; Ariosa, Juan; González, Luis Javier; Garay, Hilda; Gómez, Daniel E.; Gómez, Roberto; Alonso, Daniel F.; Sigman, Hugo; Herrera, Luís; Acevedo, Boris

doi:10.1007/s11010-008-9814-5

Cited by 82 publications

(81 citation statements)

References 15 publications

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“…In this article, we uncovered the putative mechanism of action for the novel proapoptotic peptide CIGB-300 (5,6,12). This peptide was developed to impair the tumor-exacerbated CK2 pathway by targeting the phosphoaceptor site on the substrate rather than the enzyme per se (3,4).…”

Section: Discussionmentioning

confidence: 99%

Anticancer peptide CIGB-300 binds to nucleophosmin/B23, impairs its CK2-mediated phosphorylation, and leads to apoptosis through its nucleolar disassembly activity

Perera

Fariña

Gil

et al. 2009

Molecular Cancer Therapeutics

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CIGB-300, formerly known as P15-tat, is a proapoptotic peptide with established antiproliferative activity in vitro and antitumoral activity in vivo. This hypothesis-driven peptide was initially selected for its ability to impair the in vitro CK2-mediated phosphorylation in one of its substrates through direct binding to the conserved acidic phosphoaceptor domain. However, the actual in vivo target(s) on human cancer cells among the hundreds of CK2 substrates as well as the subsequent events that lead to apoptosis on tumor cells remains to be determined. In this work, we identified the multifunctional oncoprotein nucleophosmin/B23 as a major target for CIGB-300. In vivo, the CIGB-300-B23 interaction was shown by pull-down experiments and confirmed by the early in situ colocalization of both molecules in the cell nucleolus. Moreover, CIGB-300 inhibits the CK2-mediated phosphorylation of B23 in a dose-dependent fashion both in vitro and in vivo as shown using the recombinant GST fusion protein and the metabolic labeling approach, respectively. Such phosphorylation impairment was correlated with the ability of CIGB-300 to induce nucleolar disassembly as documented by the use of established markers for nucleolar structure. Finally, we showed that such a sequence of events leads to the rapid and massive onset of apoptosis both at the molecular and cellular levels. Collectively, these findings provide important clues by which the CIGB-300 peptide exerts its proapoptotic effect on tumor cells and highlights the suitability of the B23/CK2 pathway for cancer-targeted therapy.

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Section: Discussionmentioning

confidence: 99%

Anticancer peptide CIGB-300 binds to nucleophosmin/B23, impairs its CK2-mediated phosphorylation, and leads to apoptosis through its nucleolar disassembly activity

Perera

Fariña

Gil

et al. 2009

Molecular Cancer Therapeutics

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“…As a molecular targeted agent, CIGB-300 inhibits the CK2-mediated phosphorylation of the B23/ NPM nucleolar protein and this event lead to apoptosis in tumor cells. Furthermore, degradation of B23/NPM on CIGB-300-treated cells has been also documented in nonsmall cell lung cancer cells with great sensitivity toward CIGB-300 [10,11]. Therefore, the decrease on the B23/ NPM might be indicative of some clinical activity at the molecular level.…”

Section: Discussionmentioning

confidence: 93%

“…9 Molecular Oncology Laboratory, National University of Quilmes, Buenos Aires, Argentina. 10 ELEA Laboratories, Buenos Aires, Argentina. 11 ChemoFrance Division, ChemoFrance, Paris, France.…”

Section: Conflict Of Interestmentioning

confidence: 99%

Pharmacological and safety evaluation of CIGB-300, a casein kinase 2 inhibitor peptide, administered intralesionally to patients with cervical cancer stage IB2/II

Jl¹,

Lopez-Díaz²,

Solares-Asteasuainzarra³

et al. 2013

J Cancer Res Ther

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“…The antineoplastic effect of this peptide has been well documented in the preclinical setting in vitro and in vivo (13,17,18). In 2006, the peptide entered a phase I clinical trial on patients with HSILs, where safety and efficacy signs were registered (19).…”

Section: Discussionmentioning

confidence: 99%

“…Such a multitarget effect may better explain the diverse arrays of proteins and processes that appear to be modulated by CIGB-300 and its already established antiangiogenic effect (15,16). Of note, CIGB-300 exerts a broad antiproliferative effect on cell lines derived from breast, cervical, lung, colon and prostate cancer, while a robust antitumor effect was also observed in vivo in mouse models of cervical and lung cancer (13,17,18). In the clinical setting, CIGB-300 was investigated in a phase I clinical trial on high-grade squamous intraepithelial lesions (HSILs), establishing its safety and tolerability by local injection (19).…”

Section: Introductionmentioning

confidence: 99%

Synergistic interactions of the anti-casein kinase 2 CIGB-300 peptide and chemotherapeutic agents in lung and cervical preclinical cancer models

Perera

Toro

Gorovaya

et al. 2014

Molecular and Clinical Oncology

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Abstract. CIGB-300 is a novel clinical-stage synthetic peptide that impairs the casein kinase 2 (CK2)-mediated phosphorylation of B23/nucleophosmin in different experimental settings and cancer models. As a single agent, CIGB-300 induces apoptosis in vitro and in vivo and modulates an array of proteins that are mainly involved in drug resistance, cell proliferation and apoptosis, as determined by proteomic analysis. However, the clinical oncology practice and cumulative knowledge on tumor biology suggest that drug combinations are more likely to cope with tumor complexity compared to single agents. In this study, we investigated the antiproliferative effect of CIGB-300 when combined with different anticancer drugs, such as cisplatin (alkylating), paclitaxel (antimitotic), doxorubicin (antitopoisomerase II) or 5-fluorouracil (DNA/RNA antimetabolite) in cell lines derived from lung and cervical cancer. Of note, using a Latin square design and subsequent analysis by CalcuSyn software, we observed that paclitaxel and cisplatin exhibited the best synergistic/additive profile when combined with CIGB-300, according to the combination and dose reduction indices. Such therapeutically favorable profiles may be explained by a direct cytotoxic effect and also by the observed cell cycle impairment following incubation of tumor cells with selected drug combinations. Importantly, on in vivo dose-finding schedules in human cervical tumors xenografted in nude mice, we observed that concomitant administration of CIGB-300 and cisplatin increased mice survival compared to single-agent treatment. Collectively, these findings provide a rationale for combining the anti-CK2 CIGB-300 peptide with currently available anticancer agents in the clinical setting and indicate platins and taxanes as compounds with major perspectives.

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CIGB-300, a novel proapoptotic peptide that impairs the CK2 phosphorylation and exhibits anticancer properties both in vitro and in vivo

Cited by 82 publications

References 15 publications

Anticancer peptide CIGB-300 binds to nucleophosmin/B23, impairs its CK2-mediated phosphorylation, and leads to apoptosis through its nucleolar disassembly activity

Anticancer peptide CIGB-300 binds to nucleophosmin/B23, impairs its CK2-mediated phosphorylation, and leads to apoptosis through its nucleolar disassembly activity

Pharmacological and safety evaluation of CIGB-300, a casein kinase 2 inhibitor peptide, administered intralesionally to patients with cervical cancer stage IB2/II

Synergistic interactions of the anti-casein kinase 2 CIGB-300 peptide and chemotherapeutic agents in lung and cervical preclinical cancer models

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