Your search keyword '"Disoma, Cyrollah"' showing total 7 results

1. Wnt/β-catenin signaling in colorectal cancer: Is therapeutic targeting even possible?

Author

Disoma, Cyrollah, Zhou, Yuzheng, Li, Shanni, Peng, Jian, and Xia, Zanxian

Subjects

*COLORECTAL cancer, *ADENOMATOUS polyposis coli, *DRUG target, *WNT signal transduction, *CANCER stem cells, *WNT genes

Abstract

The Wnt/β-catenin signaling pathway has been implicated as the central mechanism that drives colorectal carcinogenesis. Its activation is historically due to mutation on APC (adenomatous polyposis coli), resulting to nuclear localization of β-catenin and expression of Wnt target genes that promote tumor progression. Although this pathway seems to be a pivotal therapeutic target because of its critical role in colorectal cancer, there has been no clinically approved therapies targeting Wnt/β-catenin signaling pathway to this date. Here, we reviewed the recent progress of this signal transduction pathway in colorectal tumorigenesis. Apart from their roles in cancer initiation, the new pathway modulators (activators and repressors) also participate in chemoresistance, epithelial-mesenchymal transition and cancer stem cell renewal. Of the proteins reported to modulate this pathway, CDX2 (Caudal-related homeobox transcription factor 2) showed potentials as promising molecular target. CDX2 warrants further studies to determine its significance as molecular target for colorectal cancer therapeutics. Overall, the regulation of Wnt/β-catenin signaling pathway remains intriguingly complex and is not fully understood in spite of the widespread research efforts. Its intricacy remains a major barrier in the development of chemotherapeutic agent that specifically targets it. • New activators and repressors of Wnt pathway direct CRC initiation and progression. • Several protein families activate Wnt pathway to render CRC to be chemoresistant. • The transcription factor CDX2 is a promising molecular target. [ABSTRACT FROM AUTHOR]

Published

2022

2. Protein interactome of the deamidase phosphoribosylformylglycinamidine synthetase (PFAS) by LC-MS/MS.

Author

Lu, Ai, Disoma, Cyrollah, Zhou, Yuzheng, Chen, Zongpeng, Zhang, Liming, Shen, Yilun, Zhou, Mei, Du, Ashuai, Zheng, Rong, Li, Sijia, Alsaadawe, Moyed, Li, Shiqin, Li, Jiada, Wang, Weilan, Jiang, Taijiao, Peng, Jian, and Xia, Zanxian

Subjects

*POST-translational modification, *AMIDASES, *PROTEIN-protein interactions, *ISOELECTRIC point, *PROTEINS, *PURINE synthesis

Abstract

Phosphoribosylformylglycinamidine synthase (PFAS) is an essential enzyme in de novo synthesis of purine. Previously, PFAS has been reported to modulate RIG-I activation during viral infection via deamidation. In this study, we sought to identify potential substrates that PFAS can deamidate. Flag-PFAS was transfected into HEK-293T cells and PFAS associated proteins were purified with anti-Flag M2 magnetic beads. PFAS associated proteins were identified using mass spectrometry and were analyzed using bioinformatics tools including KEGG pathway analysis, gene ontology annotation, and protein interaction network analysis. A total of 441 proteins is suggested to potentially interact with PFAS. Of this number, 12 were previously identified and 429 are newly identified. The interactions of PFAS with CAD, CCT2, PRDX1, and PHGDH were confirmed by co-immunoprecipitation and western blotting. This study is first to report the interaction of PFAS with several proteins which play physiological roles in tumor development including CAD, CCT2, PRDX1, and PHGDH. Furthermore, we show here that PFAS is able to deamidate PHGDH, and induce other posttranslational modification into CAD, CCT2 and PRDX1. The present data provide insight on the biological function of PFAS. Further study to explore the role of these protein interactions in tumorigenesis and other diseases is recommended. • Expression of PFAS can cause shifting of isoelectric point of some proteins. • A total of 429 proteins are newly identified to interact with PFAS. • PFAS interacts with CAD, CCT2, PRDX1, and PHGDH. • PFAS can induce deamidation of PHGDH and other PTM on CAD, CCT2, and PRDX1. [ABSTRACT FROM AUTHOR]

Published

2019

3. Epigallocatechin-3-gallate, an active ingredient of Traditional Chinese Medicines, inhibits the 3CLpro activity of SARS-CoV-2.

Author

Du, Ashuai, Zheng, Rong, Disoma, Cyrollah, Li, Shiqin, Chen, Zongpeng, Li, Sijia, Liu, Pinjia, Zhou, Yuzheng, Shen, Yilun, Liu, Sixu, Zhang, Yongxing, Dong, Zijun, Yang, Qinglong, Alsaadawe, Moyed, Razzaq, Aroona, Peng, Yuyang, Chen, Xuan, Hu, Liqiang, Peng, Jian, and Zhang, Qianjun

Subjects

*CHINESE medicine, *COVID-19, *SARS-CoV-2, *FLUORESCENCE resonance energy transfer, *EPIGALLOCATECHIN gallate

Abstract

SARS-CoV-2 is the etiological agent responsible for the ongoing pandemic of coronavirus disease 2019 (COVID-19). The main protease of SARS-CoV-2, 3CLpro, is an attractive target for antiviral inhibitors due to its indispensable role in viral replication and gene expression of viral proteins. The search of compounds that can effectively inhibit the crucial activity of 3CLpro, which results to interference of the virus life cycle, is now widely pursued. Here, we report that epigallocatechin-3-gallate (EGCG), an active ingredient of Chinese herbal medicine (CHM), is a potent inhibitor of 3CLpro with half-maximum inhibitory concentration (IC50) of 0.874 ± 0.005 μM. In the study, we retrospectively analyzed the clinical data of 123 cases of COVID-19 patients, and found three effective Traditional Chinese Medicines (TCM) prescriptions. Multiple strategies were performed to screen potent inhibitors of SARS-CoV-2 3CLpro from the active ingredients of TCMs, including network pharmacology, molecular docking, surface plasmon resonance (SPR) binding assay and fluorescence resonance energy transfer (FRET)-based inhibition assay. The SPR assay showed good interaction between EGCG and 3CLpro with KD ~6.17 μM, suggesting a relatively high affinity of EGCG with SARS-CoV-2 3CLpro. Our results provide critical insights into the mechanism of action of EGCG as a potential therapeutic agent against COVID-19. [ABSTRACT FROM AUTHOR]

Published

2021

4. UBR5 Acts as an Antiviral Host Factor against MERS-CoV via Promoting Ubiquitination and Degradation of ORF4b.

Author

Yuzheng Zhou, Rong Zheng, Donglan Liu, Sixu Liu, Disoma, Cyrollah, Shiqin Li, Yujie Liao, Zongpeng Chen, Ashuai Du, Zijun Dong, Yongxing Zhang, Pinjia Liu, Razzaq, Aroona, Dingbin Chen, Xuan Chen, Xiankezi Zhong, Sijie Liu, Siyi Tao, Yuxin Liu, and Lunan Xu

Subjects

*UBIQUITINATION, *SARS-CoV-2, *MERS coronavirus, *UBIQUITIN ligases, *MIDDLE East respiratory syndrome, *PROTEASOMES

Abstract

Within the past 2 decades, three highly pathogenic human coronaviruses have emerged, namely, severe acute respiratory syndrome coronavirus (SARS-CoV), Middle East respiratory syndrome coronavirus (MERS-CoV), and severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). The health threats and economic burden posed by these tremendously severe coronaviruses have paved the way for research on their etiology, pathogenesis, and treatment. Compared to SARS-CoV and SARS-CoV-2, MERS-CoV genome encoded fewer accessory proteins, among which the ORF4b protein had anti-immunity ability in both the cytoplasm and nucleus. Our work for the first time revealed that ORF4b protein was unstable in the host cells and could be degraded by the ubiquitin proteasome system. After extensive screenings, it was found that UBR5 (ubiquitin protein ligase E3 component N-recognin 5), a member of the HECT E3 ubiquitin ligases, specifically regulated the ubiquitination and degradation of ORF4b. Similar to ORF4b, UBR5 can also translocate into the nucleus through its nuclear localization signal, enabling it to regulate ORF4b stability in both the cytoplasm and nucleus. Through further experiments, lysine 36 was identified as the ubiquitination site on the ORF4b protein, and this residue was highly conserved in various MERS-CoV strains isolated from different regions. When UBR5 was knocked down, the ability of ORF4b to suppress innate immunity was enhanced and MERS-CoV replication was stronger. As an anti-MERS-CoV host protein, UBR5 targets and degrades ORF4b protein through the ubiquitin proteasome system, thereby attenuating the anti-immunity ability of ORF4b and ultimately inhibiting MERS-CoV immune escape, which is a novel antagonistic mechanism of the host against MERS-CoV infection. [ABSTRACT FROM AUTHOR]

Published

2022

5. Fringe family genes and their modulation of Notch signaling in cancer.

Author

Mugisha, Samson, Di, Xiaotang, Disoma, Cyrollah, Jiang, Hao, and Zhang, Shubing

Subjects

*NOTCH genes, *GENE families, *GLYCOSYLTRANSFERASES, *FUCOSE, *CANCER invasiveness, *TUMOR suppressor genes

Abstract

Fringes are glycosyltransferases that transfer N -acetylglucosamine to the O-linked fucose of Notch receptors. They regulate the Notch signaling activity that drives tumor formation and progression, resulting in poor prognosis. However, the specific tumor-promoting role of Fringes differs depending on the type of cancer. Although a particular Fringe member could act as a tumor suppressor in one cancer type, it may act as an oncogene in another. This review discusses the tumorigenic role of the Fringe family (lunatic fringe, manic fringe, and radical fringe) in modulating Notch signaling in various cancers. Although the crucial functions of Fringes continue to emerge as more mechanistic studies are being pursued, further translational research is needed to explore their roles and therapeutic benefits in various malignancies. [ABSTRACT FROM AUTHOR]

Published

2022

6. M6A-mediated upregulation of circMDK promotes tumorigenesis and acts as a nanotherapeutic target in hepatocellular carcinoma.

Author

Du, Ashuai, Li, Shiqin, Zhou, Yuzheng, Disoma, Cyrollah, Liao, Yujie, Zhang, Yongxing, Chen, Zongpeng, Yang, Qinglong, Liu, Pinjia, Liu, Sixu, Dong, Zijun, Razzaq, Aroona, Tao, Siyi, Chen, Xuan, Liu, Yuxin, Xu, Lunan, Zhang, Qianjun, Li, Shanni, Peng, Jian, and Xia, Zanxian

Subjects

*HEPATOCELLULAR carcinoma, *SMALL interfering RNA, *CIRCULAR RNA, *GENE silencing, *CANCER invasiveness, *ADENOSINES

Abstract

Background: Emerging evidence suggest the critical role of circular RNAs (circRNAs) in disease development especially in various cancers. However, the oncogenic role of circRNAs in hepatocellular carcinoma (HCC) is still largely unknown. Methods: RNA sequencing was performed to identify significantly upregulated circRNAs in paired HCC tissues and non-tumor tissues. CCK-8 assay, colony formation, transwell, and xenograft mouse models were used to investigate the role of circRNAs in HCC proliferation and metastasis. Small interfering RNA (siRNA) was used to silence gene expression. RNA immunoprecipitation, biotin pull-down, RNA pull-down, luciferase reporter assay and western blot were used to explore the underlying molecular mechanisms. Results: Hsa_circ_0095868, derived from exon 5 of the MDK gene (named circMDK), was identified as a new oncogenic circRNA that was significantly upregulated in HCC. The upregulation of circMDK was associated with the modification of N6-methyladenosine (m6A) and poor survival in HCC patients. Mechanistically, circMDK sponged miR-346 and miR-874-3p to upregulate ATG16L1 (Autophagy Related 16 Like 1), resulting to the activation of PI3K/AKT/mTOR signaling pathway to promote cell proliferation, migration and invasion. Poly (β-amino esters) (PAEs) were synthesized to assist the delivery of circMDK siRNA (PAE-siRNA), which effectively inhibited tumor progression without obvious adverse effects in four liver tumor models including subcutaneous, metastatic, orthotopic and patient-derived xenograft (PDX) models. Conclusions: CircMDK could serve as a potential tumor biomarker that promotes the progression of HCC via the miR-346/874-3p-ATG16L1 axis. The PAE-based delivery of siRNA improved the stability and efficiency of siRNA targeting circMDK. The PAE-siRNA nanoparticles effectively inhibited HCC proliferation and metastasis in vivo. Our current findings offer a promising nanotherapeutic strategy for the treatment of HCC. [ABSTRACT FROM AUTHOR]

Published

2022

7. Host E3 ligase HUWE1 attenuates the proapoptotic activity of the MERS-CoV accessory protein ORF3 by promoting its ubiquitin-dependent degradation.

Author

Yuzheng Zhou, Rong Zheng, Sixu Liu, Disoma, Cyrollah, Ashuai Du, Shiqin Li, Zongpeng Chen, Zijun Dong, Yongxing Zhang, Sijia Li, Pinjia Liu, Razzaq, Aroona, Xuan Chen, Yujie Liao, Siyi Tao, Yuxin Liu, Lunan Xu, Qianjun Zhang, Jian Peng, and Xu Deng

Subjects

*SARS-CoV-2, *MERS coronavirus, *SARS Epidemic, 2002-2003, *SARS disease, *VIRAL nonstructural proteins, *UBIQUITIN ligases, *CYTOSKELETAL proteins

Abstract

With the outbreak of severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2), coronaviruses have begun to attract great attention across the world. Of the known human coronaviruses, however, Middle East respiratory syndrome coronavirus (MERS-CoV) is the most lethal. Coronavirus proteins can be divided into three groups: nonstructural proteins, structural proteins, and accessory proteins. While the number of each of these proteins varies greatly among different coronaviruses, accessory proteins are most closely related to the pathogenicity of the virus. We found for the first time that the ORF3 accessory protein of MERS-CoV, which closely resembles the ORF3a proteins of severe acute respiratory syndrome coronavirus and SARS-CoV-2, has the ability to induce apoptosis in cells in a dose-dependent manner. Through bioinformatics analysis and validation, we revealed that ORF3 is an unstable protein and has a shorter half-life in cells compared to that of severe acute respiratory syndrome coronavirus and SARS-CoV-2 ORF3a proteins. After screening, we identified a host E3 ligase, HUWE1, that specifically induces MERS-CoV ORF3 protein ubiquitination and degradation through the ubiquitin-proteasome system. This results in the diminished ability of ORF3 to induce apoptosis, which might partially explain the lower spread of MERS-CoV compared to other coronaviruses. In summary, this study reveals a pathological function of MERS-CoV ORF3 protein and identifies a potential host antiviral protein, HUWE1, with an ability to antagonize MERS-CoV pathogenesis by inducing ORF3 degradation, thus enriching our knowledge of the pathogenesis of MERS-CoV and suggesting new targets and strategies for clinical development of drugs for MERS-CoV treatment. [ABSTRACT FROM AUTHOR]

Published

2022