Lista de obras - Matthew B. McNeil - Dominio Público Uruguay

CRISPR-Cas gene-editing reveals RsmA and RsmC act through FlhDC to repress the SdhE flavinylation factor and control motility and prodigiosin production in Serratia.

artículo científico publicado en 2016

Cell wall inhibitors increase the accumulation of rifampicin in Mycobacterium tuberculosis

artículo científico publicado en 2019

Characterisation of the conserved hypothetical proteins SdhE and YgfX in Serratia 39006

2012 doctoral thesis by Matthew Brad McNeil at University of Otago

Corrigendum to "Mechanisms of resistance against NITD-916, a direct inhibitor of Mycobacterium tuberculosis InhA" [Tuberculosis 107 (December 2017) 133-136].

artículo científico publicado en 2018

Discovery of a cofactor-independent inhibitor of Mycobacterium tuberculosis InhA

scientific article published on 01 June 2018

Draft Genome Sequence of Serratia sp. Strain ATCC 39006, a Model Bacterium for Analysis of the Biosynthesis and Regulation of Prodigiosin, a Carbapenem, and Gas Vesicles.

artículo científico publicado en 2013

Efficacy and Improved Resistance Potential of a Cofactor-Independent InhA Inhibitor of Mycobacterium tuberculosis in the C3HeB/FeJ Mouse Model

scientific article published on 27 March 2019

In vitro isolation and characterization of oxazolidinone resistant Mycobacterium tuberculosis.

artículo científico publicado en 2017

Mechanisms of resistance against NITD-916, a direct inhibitor of Mycobacterium tuberculosis InhA.

artículo científico publicado en 2017

MmpL3 inhibitors as antituberculosis drugs

scientific article published on 04 May 2020

Mutations in MmpL3 alter membrane potential, hydrophobicity and antibiotic susceptibility in Mycobacterium smegmatis.

artículo científico publicado en 2017

Novel chemical entities inhibiting Mycobacterium tuberculosis growth identified by phenotypic high-throughput screening

artículo científico publicado en 2022

PigS and PigP regulate prodigiosin biosynthesis in Serratia via differential control of divergent operons, which include predicted transporters of sulfur-containing molecules.

artículo científico publicado en 2010

Priming in the Type I-F CRISPR-Cas system triggers strand-independent spacer acquisition, bi-directionally from the primed protospacer.

artículo científico publicado en 2014

SdhE is a conserved protein required for flavinylation of succinate dehydrogenase in bacteria

artículo científico publicado en 2012

The conserved RGxxE motif of the bacterial FAD assembly factor SdhE is required for succinate dehydrogenase flavinylation and activity

artículo científico publicado en 2013

The succinate dehydrogenase assembly factor, SdhE, is required for the flavinylation and activation of fumarate reductase in bacteria.

artículo científico publicado en 2013

Two for the price of one: Attacking the energetic-metabolic hub of mycobacteria to produce new chemotherapeutic agents

artículo científico publicado en 2019

Utilization of CRISPR Interference To Validate MmpL3 as a Drug Target in Mycobacterium tuberculosis

scientific article published on 25 July 2019

YgfX (CptA) is a multimeric membrane protein that interacts with the succinate dehydrogenase assembly factor SdhE (YgfY).

artículo científico publicado en 2013

Lista de obras de Matthew B. McNeil

CRISPR-Cas gene-editing reveals RsmA and RsmC act through FlhDC to repress the SdhE flavinylation factor and control motility and prodigiosin production in Serratia.

Cell wall inhibitors increase the accumulation of rifampicin in Mycobacterium tuberculosis

Characterisation of the conserved hypothetical proteins SdhE and YgfX in Serratia 39006

Corrigendum to "Mechanisms of resistance against NITD-916, a direct inhibitor of Mycobacterium tuberculosis InhA" [Tuberculosis 107 (December 2017) 133-136].

Discovery of a cofactor-independent inhibitor of Mycobacterium tuberculosis InhA

Draft Genome Sequence of Serratia sp. Strain ATCC 39006, a Model Bacterium for Analysis of the Biosynthesis and Regulation of Prodigiosin, a Carbapenem, and Gas Vesicles.

Efficacy and Improved Resistance Potential of a Cofactor-Independent InhA Inhibitor of Mycobacterium tuberculosis in the C3HeB/FeJ Mouse Model

In vitro isolation and characterization of oxazolidinone resistant Mycobacterium tuberculosis.

Mechanisms of resistance against NITD-916, a direct inhibitor of Mycobacterium tuberculosis InhA.

MmpL3 inhibitors as antituberculosis drugs

Mutations in MmpL3 alter membrane potential, hydrophobicity and antibiotic susceptibility in Mycobacterium smegmatis.

Novel chemical entities inhibiting Mycobacterium tuberculosis growth identified by phenotypic high-throughput screening

PigS and PigP regulate prodigiosin biosynthesis in Serratia via differential control of divergent operons, which include predicted transporters of sulfur-containing molecules.

Priming in the Type I-F CRISPR-Cas system triggers strand-independent spacer acquisition, bi-directionally from the primed protospacer.

SdhE is a conserved protein required for flavinylation of succinate dehydrogenase in bacteria

The conserved RGxxE motif of the bacterial FAD assembly factor SdhE is required for succinate dehydrogenase flavinylation and activity

The succinate dehydrogenase assembly factor, SdhE, is required for the flavinylation and activation of fumarate reductase in bacteria.

Two for the price of one: Attacking the energetic-metabolic hub of mycobacteria to produce new chemotherapeutic agents

Utilization of CRISPR Interference To Validate MmpL3 as a Drug Target in Mycobacterium tuberculosis

YgfX (CptA) is a multimeric membrane protein that interacts with the succinate dehydrogenase assembly factor SdhE (YgfY).