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Dive into the research topics where Marina I. Nelen is active.

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Featured researches published by Marina I. Nelen.


Journal of The Chemical Society-perkin Transactions 1 | 1997

Electrostatic molecular recognition in rigid frameworks

Marina I. Nelen; Alexey V. Eliseev

Complexation of six organic dianionic hosts (1cc–2tt) with methylguanidinium, tetramethylammonium and ammonium salts in various protic solvents has been studied by NMR spectroscopy. Stability of the 1∶1 electrostatic complexes is shown to decrease with increasing distances between the carboxylate groups in the host compounds. Spectroscopic data and the results of molecular modelling support non-symmetrical structures of some of the complexes which contain one tight and one loose ion pair. The difference between the contributions of the tight and loose ion pair formation into the binding free energy can be predicted by the Fuoss theory of ion pairing on the basis of interionic distances calculated by molecular modelling.


PLOS ONE | 2017

RORγt and RORα signature genes in human Th17 cells

Glenda Castro; Xuejun Liu; Karen Ngo; Aimee De Leon-Tabaldo; Shanrong Zhao; Rosa Luna-Roman; Jingxue Yu; Tinghua Cao; Robert Kuhn; Patrick Wilkinson; Krystal Herman; Marina I. Nelen; Jonathan M. Blevitt; Xiaohua Xue; Anne M. Fourie; Wai-Ping Fung-Leung; Yeonseok Chung

RORγt and RORα are transcription factors of the RAR-related orphan nuclear receptor (ROR) family. They are expressed in Th17 cells and have been suggested to play a role in Th17 differentiation. Although RORγt signature genes have been characterized in mouse Th17 cells, detailed information on its transcriptional control in human Th17 cells is limited and even less is known about RORα signature genes which have not been reported in either human or mouse T cells. In this study, global gene expression of human CD4 T cells activated under Th17 skewing conditions was profiled by RNA sequencing. RORγt and RORα signature genes were identified in these Th17 cells treated with specific siRNAs to knock down RORγt or RORα expression. We have generated selective small molecule RORγt modulators and they were also utilized as pharmacological tools in RORγt signature gene identification. Our results showed that RORγt controlled the expression of a very selective number of genes in Th17 cells and most of them were regulated by RORα as well albeit a weaker influence. Key Th17 genes including IL-17A, IL-17F, IL-23R, CCL20 and CCR6 were shown to be regulated by both RORγt and RORα. Our results demonstrated an overlapping role of RORγt and RORα in human Th17 cell differentiation through regulation of a defined common set of Th17 genes. RORγt as a drug target for treatment of Th17 mediated autoimmune diseases such as psoriasis has been demonstrated recently in clinical trials. Our results suggest that RORα could be involved in same disease mechanisms and gene signatures identified in this report could be valuable biomarkers for tracking the pharmacodynamic effects of compounds that modulate RORγt or RORα activities in patients.


Journal of Medicinal Chemistry | 2017

Structural Basis of Small-Molecule Aggregate Induced Inhibition of a Protein-Protein Interaction.

Jonathan M. Blevitt; Michael D. Hack; Krystal Herman; Paul F. Jackson; Paul J. Krawczuk; Alec D. Lebsack; Annie X. Liu; Taraneh Mirzadegan; Marina I. Nelen; Aaron N. Patrick; Stefan Steinbacher; Marcos E. Milla; Kevin J. Lumb

A prevalent observation in high-throughput screening and drug discovery programs is the inhibition of protein function by small-molecule compound aggregation. Here, we present the X-ray structural description of aggregation-based inhibition of a protein-protein interaction involving tumor necrosis factor α (TNFα). An ordered conglomerate of an aggregating small-molecule inhibitor (JNJ525) induces a quaternary structure switch of TNFα that inhibits the protein-protein interaction between TNFα and TNFα receptors. SPD-304 may employ a similar mechanism of inhibition.


Journal of the American Chemical Society | 1997

Use of Molecular Recognition To Drive Chemical Evolution. 1. Controlling the Composition of an Equilibrating Mixture of Simple Arginine Receptors

Alexey V. Eliseev; Marina I. Nelen


Journal of Medicinal Chemistry | 2002

Water-soluble, core-modified porphyrins as novel, longer-wavelength-absorbing sensitizers for photodynamic therapy. II. Effects of core heteroatoms and meso-substituents on biological activity.

David G. Hilmey; Masako Abe; Marina I. Nelen; Corey E. Stilts; Gary A. Baker; Sheila N. Baker; Frank V. Bright; Sherry R. Davies; Sandra O. Gollnick; Allan R. Oseroff; Scott L. Gibson; and Russell Hilf; Michael R. Detty


Journal of Physical Organic Chemistry | 1999

Imine exchange in O-aryl and O-alkyl oximes as a base reaction for aqueous ‘dynamic’ combinatorial libraries. A kinetic and thermodynamic study

Vladimir A. Polyakov; Marina I. Nelen; Noureddin Nazarpack-Kandlousy; Alexander D. Ryabov; Alexey V. Eliseev


Journal of Medicinal Chemistry | 2000

Water-Soluble, Core-Modified Porphyrins as Novel, Longer-Wavelength-Absorbing Sensitizers for Photodynamic Therapy

Corey E. Stilts; Marina I. Nelen; David G. Hilmey; Sherry R. Davies; Sandra O. Gollnick; Allan R. Oseroff; Scott L. Gibson; Russell Hilf; Michael R. Detty


Chemistry: A European Journal | 1998

Use of Molecular Recognition To Drive Chemical Evolution: Mechanisms of an Automated Genetic Algorithm Implementation

Alexey V. Eliseev; Marina I. Nelen


Journal of Medicinal Chemistry | 2000

A selenopyrylium photosensitizer for photodynamic therapy related in structure to the antitumor agent aa1 with potent in vivo activity and no long-term skin photosensitization

Kristi A. Leonard; Jonathan Hall; Marina I. Nelen; Sherry R. Davies; Sandra O. Gollnick; Sue Camacho; Allan R. Oseroff; Scott L. Gibson; Russell Hilf; Michael R. Detty


Journal of Medicinal Chemistry | 1999

Synthesis and Evaluation of Chalcogenopyrylium Dyes as Potential Sensitizers for the Photodynamic Therapy of Cancer

Kristi A. Leonard; Marina I. Nelen; Todd P. Simard; Sherry R. Davies; Sandra O. Gollnick; Allan R. Oseroff; Scott L. Gibson; Russell Hilf; and Lan Bo Chen; Michael R. Detty

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Michael R. Detty

State University of New York System

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Allan R. Oseroff

Roswell Park Cancer Institute

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Russell Hilf

University of Rochester

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Sandra O. Gollnick

Roswell Park Cancer Institute

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Sherry R. Davies

Roswell Park Cancer Institute

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