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Featured researches published by Charlotte Mobarak.


Nucleic Acids Research | 2008

The SET and transposase domain protein Metnase enhances chromosome decatenation: regulation by automethylation

Elizabeth A. Williamson; Kanwaldeep Kaur Rasila; Lori Kwan Corwin; Justin Wray; Brian D. Beck; Virginia Severns; Charlotte Mobarak; Suk Hee Lee; Jac A. Nickoloff; Robert Hromas

Metnase is a human SET and transposase domain protein that methylates histone H3 and promotes DNA double-strand break repair. We now show that Metnase physically interacts and co-localizes with Topoisomerase IIα (Topo IIα), the key chromosome decatenating enzyme. Metnase promotes progression through decatenation and increases resistance to the Topo IIα inhibitors ICRF-193 and VP-16. Purified Metnase greatly enhanced Topo IIα decatenation of kinetoplast DNA to relaxed circular forms. Nuclear extracts containing Metnase decatenated kDNA more rapidly than those without Metnase, and neutralizing anti-sera against Metnase reversed that enhancement of decatenation. Metnase automethylates at K485, and the presence of a methyl donor blocked the enhancement of Topo IIα decatenation by Metnase, implying an internal regulatory inhibition. Thus, Metnase enhances Topo IIα decatenation, and this activity is repressed by automethylation. These results suggest that cancer cells could subvert Metnase to mediate clinically relevant resistance to Topo IIα inhibitors.


Chemical Research in Toxicology | 2014

Differential binding of monomethylarsonous acid compared to arsenite and arsenic trioxide with zinc finger peptides and proteins

Xixi Zhou; Xi Sun; Charlotte Mobarak; A. Jay Gandolfi; Scott W. Burchiel; Laurie G. Hudson; Ke Jian Liu

Arsenic is an environmental toxin that enhances the carcinogenic effect of DNA-damaging agents, such as ultraviolet radiation and benzo[a]pyrene. Interaction with zinc finger proteins has been shown to be an important molecular mechanism for arsenic toxicity and cocarcinogenesis. Arsenicals such as arsenite, arsenic trioxide (ATO), and monomethylarsonous acid (MMA(III)) have been reported to interact with cysteine residues of zinc finger domains, but little is known about potential differences in their selectivity of interaction. Herein we analyzed the interaction of arsenite, MMA(III), and ATO with C2H2, C3H1, and C4 configurations of zinc fingers using UV–vis, cobalt, fluorescence, and mass spectrometry. We observed that arsenite and ATO both selectively bound to C3H1 and C4 zinc fingers, while MMA(III) interacted with all three configurations of zinc finger peptides. Structurally and functionally, arsenite and ATO caused conformational changes and zinc loss on C3H1 and C4 zinc finger peptide and protein, respectively, whereas MMA(III) changed conformation and displaced zinc on all three types of zinc fingers. The differential selectivity was also demonstrated in zinc finger proteins isolated from cells treated with these arsenicals. Our results show that trivalent inorganic arsenic compounds, arsenite and ATO, have the same selectivity and behavior when interacting with zinc finger proteins, while methylation removes the selectivity. These findings provide insights on the molecular mechanisms underlying the differential effects of inorganic versus methylated arsenicals, as well as the role of in vivo arsenic methylation in arsenic toxicity and carcinogenesis.


Developmental and Comparative Immunology | 2010

Identification of protein components of egg masses indicates parental investment in immunoprotection of offspring by Biomphalaria glabrata (gastropoda, mollusca).

Jennifer J.M. Hathaway; Coen M. Adema; Barbara A. Stout; Charlotte Mobarak; Eric S. Loker


American Journal of Obstetrics and Gynecology | 2007

Identification of proteins within the nuclear factor-κ B transcriptional complex including estrogen receptor-α

Irv Feldman; Gerald M. Feldman; Charlotte Mobarak; Jeffrey C. Dunkelberg; Kimberly K. Leslie


Journal of Biological Chemistry | 2001

New Roles for the Snp1 and Exo84 Proteins in Yeast Pre-mRNA Splicing

Sita Awasthi; Rachel Palmer; Marygrace Castro; Charlotte Mobarak; Stephanie W. Ruby


Chemical Research in Toxicology | 2002

Determining the site of spin trapping of the equine myoglobin radical by combined use of EPR, electrophoretic purification, and mass spectrometry.

Michael N. Harris; Scott W. Burchiel; Paul G. Winyard; John R. Engen; Charlotte Mobarak; Graham S. Timmins


Archive | 2004

Detection of endometrial pathology

Kimberly K. Leslie; Charlotte Mobarak; Harriet O. Smith


American Journal of Obstetrics and Gynecology | 2006

Proteomic screening using SELDI-TOF to detect biomarkers for preterm labor in serum

Suzy Davies; Jay Bolnick; Charlotte Mobarak; Sang-Joon Lee; Kimberly K. Leslie


Clinical Proteomics | 2010

Proteomic Analysis of the Systemic Response to Radiographic Contrast Media

Juan Martinez; Warren K. Laskey; Cheri Wells; Armin Foghi; Sarah Rohde; Mark J. Ricciardi; Charlotte Mobarak


American Journal of Obstetrics and Gynecology | 2007

469: Unique serum fragments of fibrinopeptide A and kininogen I are identified as potential biomarkers of preeclampsia

Sunanda Sadanandan; Eliza Berkley; Suzy Davies; Jennifer L. Mitchell; Charlotte Mobarak; Maria Velasquez; Sang-Joon Lee; Gene La Monica; Adanna Amanze; Kimberly K. Leslie

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Kimberly K. Leslie

University of Iowa Hospitals and Clinics

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Suzy Davies

University of New Mexico

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Eliza Berkley

University of New Mexico

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Jay Bolnick

University of New Mexico

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Sang-Joon Lee

University of New Mexico

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Adanna Amanze

University of New Mexico

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