نتایج جستجو برای: small molecule

تعداد نتایج: 886075  

Journal: :Organic & biomolecular chemistry 2008
Cristina Lucas-Lopez John S Allingham Tomas Lebl Christopher P A T Lawson Ruth Brenk James R Sellers Ivan Rayment Nicholas J Westwood

The small molecule blebbistatin is now a front line tool in the study of myosin function. Chemical modification of the tricyclic core of blebbistatin could deliver the next generation of myosin inhibitors and to help address this we report here on the impact of structural changes in the methyl-substituted aromatic ring of blebbistatin on its biological activity. Chemical methods for the prepara...

Journal: :Molecular Systems Biology 2006
Anthony C Forster George M Church

Construction of a chemical system capable of replication and evolution, fed only by small molecule nutrients, is now conceivable. This could be achieved by stepwise integration of decades of work on the reconstitution of DNA, RNA and protein syntheses from pure components. Such a minimal cell project would initially define the components sufficient for each subsystem, allow detailed kinetic ana...

Journal: :The journal of physical chemistry. B 2008
Julien Michel Mario Orsi Jonathan W Essex

Coarse-grain models are becoming an increasingly important tool in computer simulations of a wide variety of molecular processes. In many instances it is, however, desirable to describe key portions of a molecular system at the atomic level. There is therefore a strong interest in the development of simulation methodologies that allow representations of matter with mixed granularities in a mult...

2009
Takuya Uchida Manuela Rodriquez Stuart L. Schreiber

Intermolecular couplings of simple building blocks using catalytic, stereoselective cross-Mannich reactions followed by intramolecular functional group-pairing reactions of easily accessed variants of the Mannich products are explored as a route to skeletally diverse small molecules. The synthetic pathway yields products having 12 different skeletons using only three steps and has the potential...

2014
Jessica Wagner Christina Leah Kline Richard S. Pottorf Bhaskara Rao Nallaganchu Gary L. Olson David T. Dicker Joshua E. Allen Wafik S. El-Deiry

We previously identified TRAIL-inducing compound 10 (TIC10), also known as NSC350625 or ONC201, from a NCI chemical library screen as a small molecule that has potent anti-tumor efficacy and a benign safety profile in preclinical cancer models. The chemical structure that was originally published by Stahle, et. al. in the patent literature was described as an imidazo[1,2-a]pyrido[4,3-d]pyrimidi...

Journal: :Trends in biotechnology 2008
Arthur Wuster M Madan Babu

A robust knowledge of the interactions between small molecules and specific proteins aids the development of new biotechnological tools and the identification of new drug targets, and can lead to specific biological insights. Such knowledge can be obtained through chemogenomic screens. In these screens, each small molecule from a chemical library is applied to each cell type from a library of c...

Journal: :Combinatorial chemistry & high throughput screening 2003
J C Yarrow Y Feng Z E Perlman T Kirchhausen T J Mitchison

We have developed high throughput fluorescence cell imaging methods to screen chemical libraries for compounds with effects on diverse aspects of cell physiology. We describe screens for compounds that arrest cells in mitosis, that block cell migration, and that block the secretory pathway. Each of these screens yielded specific inhibitors for research use, and the mitosis screen identified Eg5...

Journal: :Antimicrobial agents and chemotherapy 2009
Ning J Pan Michael J Brady John M Leong Jon D Goguen

Yersinia pestis, the causative agent of plague, utilizes a plasmid-encoded type III secretion system (T3SS) to aid it with its resistance to host defenses. This system injects a set of effector proteins known as Yops (Yersinia outer proteins) into the cytosol of host cells that come into contact with the bacteria. T3SS is absolutely required for the virulence of Y. pestis, making it a potential...

2013
Prakash Srinivasan Adam Yasgar Diane K. Luci Wandy L. Beatty Xin Hu John Andersen David L. Narum J. Kathleen Moch Hongmao Sun J. David Haynes David J. Maloney Ajit Jadhav Anton Simeonov Louis H. Miller

Plasmodium falciparum resistance to artemisinin derivatives, the first-line antimalarial drug, drives the search for new classes of chemotherapeutic agents. Current discovery is primarily directed against the intracellular forms of the parasite. However, late schizont-infected red blood cells (RBCs) may still rupture and cause disease by sequestration; consequently targeting invasion may reduce...

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