Literature DB >> 33291073

Identification of a novel and potent small molecule inhibitor of SRPK1: mechanism of dual inhibition of SRPK1 for the inhibition of cancer progression.

Anshuman Chandra1, Hanumappa Ananda2, Nagendra Singh1, Imteyaz Qamar1.   

Abstract

Protein kinases are the family of attractive enzyme targets for drug design with relevance to cancer biology. Serine arginine protein kinase 1 (SRPK1) is responsible for the phosphorylation of serine/arginine (SR)-rich proteins. Alternative Splicing Factor/Splicing Factor 2 (ASF/SF2) involved in mRNA editing. ASF/SF2 is over expressed in many cancers and plays crucial roles in the cell survival. Phosphorylation of ASF/SF2 is decisive for its functions in cancer. In search of potential anticancer therapeutic agents for attenuating phosphorylation of ASF/SF2, we have explored specific and potential inhibitors of SRPK1 from natural and drug like compounds databases using in-silico methods. Compound ZINC02154892 (C02) was found to be the most potent inhibitor for SRPK1. In-vitro molecular and cell biology studies have shown C02 as a potent and specific inhibitor of phosphorylation of ASF/SF2 and cell survival in leukemic cell line. Structural analysis of SRPK1 with compound C02 revealed a unique pattern of binding targeting ATP binding site along with inhibiting recruitment of ASF/SF2 by SRPK1. The possibilities of compound C02 to be used as a lead compound paving way for the development of potent and specific inhibitors of SRPK1 for designing of novel potential anticancer inhibitor is inferred from the current studies.

Entities:  

Keywords:  MTT assay; flow cytometery; splicing inhibitor; structure based drug design; virtual screening

Mesh:

Substances:

Year:  2020        PMID: 33291073      PMCID: PMC7835025          DOI: 10.18632/aging.202301

Source DB:  PubMed          Journal:  Aging (Albany NY)        ISSN: 1945-4589            Impact factor:   5.682


  28 in total

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4.  SEER update of incidence and trends in pediatric malignancies: acute lymphoblastic leukemia.

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5.  Serine-arginine protein kinase 1 overexpression is associated with tumorigenic imbalance in mitogen-activated protein kinase pathways in breast, colonic, and pancreatic carcinomas.

Authors:  Gregory M Hayes; Patricia E Carrigan; Laurence J Miller
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6.  SRPKIN-1: A Covalent SRPK1/2 Inhibitor that Potently Converts VEGF from Pro-angiogenic to Anti-angiogenic Isoform.

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8.  Development of Potent, Selective SRPK1 Inhibitors as Potential Topical Therapeutics for Neovascular Eye Disease.

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Journal:  ACS Chem Biol       Date:  2017-02-06       Impact factor: 5.100

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Authors:  Raoni Pais Siqueira; Éverton de Almeida Alves Barbosa; Marcelo Depólo Polêto; Germanna Lima Righetto; Thiago Vargas Seraphim; Rafael Locatelli Salgado; Joana Gasperazzo Ferreira; Marcus Vinícius de Andrade Barros; Leandro Licursi de Oliveira; Angelo Brunelli Albertoni Laranjeira; Márcia Rogéria Almeida; Abelardo Silva Júnior; Juliana Lopes Rangel Fietto; Jörg Kobarg; Eduardo Basílio de Oliveira; Robson Ricardo Teixeira; Júlio César Borges; Jose Andrés Yunes; Gustavo Costa Bressan
Journal:  PLoS One       Date:  2015-08-05       Impact factor: 3.240

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  3 in total

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2.  SRSF protein kinase 1 modulates RAN translation and suppresses CGG repeat toxicity.

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Journal:  EMBO Mol Med       Date:  2021-09-20       Impact factor: 12.137

3.  Increased expression of SRPK1 (serine/arginine-rich protein-specific kinase 1) is associated with progression and unfavorable prognosis in cervical squamous cell carcinoma.

Authors:  Zhanfei Dong; Xuezhi Chang; Li Xie; Yina Wang; Youxiang Hou
Journal:  Bioengineered       Date:  2022-03       Impact factor: 3.269

  3 in total

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