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Author Report for: Love J

Title: Structures of human acetylcholinesterase in complex with pharmacologically important ligands
Cheung J, Rudolph MJ, Burshteyn F, Cassidy MS, Gary EN, Love J, Franklin MC, Height JJ
Ref: Journal of Medicinal Chemistry, 55:10282, 2012 : PubMed
Abstract


ESTHER: Cheung_2012_J.Med.Chem_55_10282
PubMedSearch: Cheung 2012 J.Med.Chem 55 10282
PubMedID: 23035744
Gene_locus related to this paper: human-ACHE

Abstract

Human acetylcholinesterase (AChE) is a significant target for therapeutic drugs. Here we present high resolution crystal structures of human AChE, alone and in complexes with drug ligands; donepezil, an Alzheimer's disease drug, binds differently to human AChE than it does to Torpedo AChE. These crystals of human AChE provide a more accurate platform for further drug development than previously available.



        

Title: Complete genome sequence of a free-living Vibrio furnissii sp. nov. strain (NCTC 11218)
Lux TM, Lee R, Love J
Ref: Journal of Bacteriology, 193:1487, 2011 : PubMed
Abstract


ESTHER: Lux_2011_J.Bacteriol_193_1487
PubMedSearch: Lux 2011 J.Bacteriol 193 1487
PubMedID: 21217006
Gene_locus related to this paper: vibfn-f0lr02, vibfn-f0lug8, vibfu-c9pbt2, vibfu-c9pdm3, vibfu-c9pfx8, vibfu-c9p9p8, vibfu-c9pl22, vibfu-c9pet6



        

Title: Coccolithophores: functional biodiversity, enzymes and bioprospecting
Reid EL, Worthy CA, Probert I, Ali ST, Love J, Napier J, Littlechild JA, Somerfield PJ, Allen MJ
Ref: Mar Drugs, 9:586, 2011 : PubMed
Abstract


ESTHER: Reid_2011_Mar.Drugs_9_586
PubMedSearch: Reid 2011 Mar.Drugs 9 586
PubMedID: 21731551

Abstract

Emiliania huxleyi is a single celled, marine phytoplankton with global distribution. As a key species for global biogeochemical cycling, a variety of strains have been amassed in various culture collections. Using a library consisting of 52 strains of E. huxleyi and an 'in house' enzyme screening program, we have assessed the functional biodiversity within this species of fundamental importance to global biogeochemical cycling, whilst at the same time determining their potential for exploitation in biocatalytic applications. Here, we describe the screening of E. huxleyi strains, as well as a coccolithovirus infected strain, for commercially relevant biocatalytic enzymes such as acid/alkali phosphodiesterase, acid/alkali phosphomonoesterase, EC1.1.1-type dehydrogenase, EC1.3.1-type dehydrogenase and carboxylesterase.



        

Title: Adhesion molecules in the nervous system: structural insights into function and diversity
Shapiro L, Love J, Colman DR
Ref: Annual Review of Neuroscience, 30:451, 2007 : PubMed
Abstract


ESTHER: Shapiro_2007_Annu.Rev.Neurosci_30_451
PubMedSearch: Shapiro 2007 Annu.Rev.Neurosci 30 451
PubMedID: 17600523
Gene_locus related to this paper: human-NLGN3, human-NLGN4X

Abstract

The unparalleled complexity of intercellular connections in the nervous system presents requirements for high levels of both specificity and diversity for the proteins that mediate cell adhesion. Here we describe recent advances toward understanding the molecular mechanisms that underlie adhesive binding, specificity, and diversity for several well-characterized families of adhesion molecules in the nervous system. Although many families of adhesion proteins, including cadherins and immunoglobulin superfamily members, are utilized in neural and nonneural contexts, nervous system-specific diversification mechanisms, such as precisely regulated alternative splicing, provide an important means to enable their function in the complex context of the nervous system.