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Dive into the research topics where Hening Lin is active.

Publication


Featured researches published by Hening Lin.


Proceedings of the National Academy of Sciences of the United States of America | 2006

The pathogen-associated iroA gene cluster mediates bacterial evasion of lipocalin 2

Michael A. Fischbach; Hening Lin; Lu Zhou; Yang Yu; Rebecca J. Abergel; David R. Liu; Kenneth N. Raymond; Barry L. Wanner; Roland K. Strong; Christopher T. Walsh; Alan Aderem; Kelly D. Smith

Numerous bacteria cope with the scarcity of iron in their microenvironment by synthesizing small iron-scavenging molecules known as siderophores. Mammals have evolved countermeasures to block siderophore-mediated iron acquisition as part of their innate immune response. Secreted lipocalin 2 (Lcn2) sequesters the Escherichia coli siderophore enterobactin (Ent), preventing E. coli from acquiring iron and protecting mammals from infection by E. coli. Here, we show that the iroA gene cluster, found in many pathogenic strains of Gram-negative enteric bacteria, including E. coli, Salmonella spp., and Klebsiella pneumoniae, allows bacteria to evade sequestration of Ent by Lcn2. We demonstrate that C-glucosylated derivatives of Ent produced by iroA-encoded enzymes do not bind purified Lcn2, and an iroA-harboring strain of E. coli is insensitive to the growth inhibitory effects of Lcn2 in vitro. Furthermore, we show that mice rapidly succumb to infection by an iroA-harboring strain of E. coli but not its wild-type counterpart, and that this increased virulence depends on evasion of host Lcn2. Our findings indicate that the iroA gene cluster allows bacteria to evade this component of the innate immune system, rejuvenating their Ent-mediated iron-acquisition pathway and playing an important role in their virulence.


Nature Chemical Biology | 2006

How pathogenic bacteria evade mammalian sabotage in the battle for iron

Michael A. Fischbach; Hening Lin; David R. Liu; Christopher T. Walsh


Proceedings of the National Academy of Sciences of the United States of America | 2005

In vitro characterization of IroB, a pathogen-associated C-glycosyltransferase

Michael A. Fischbach; Hening Lin; David R. Liu; Christopher T. Walsh


Journal of the American Chemical Society | 2005

In vitro characterization of salmochelin and enterobactin trilactone hydrolases IroD, IroE, and Fes.

Hening Lin; Michael A. Fischbach; David R. Liu; Christopher T. Walsh


Journal of the American Chemical Society | 2004

A Chemoenzymatic Approach to Glycopeptide Antibiotics

Hening Lin; Christopher T. Walsh


Chemistry & Biology | 2004

Macrolactamization of Glycosylated Peptide Thioesters by the Thioesterase Domain of Tyrocidine Synthetase

Hening Lin; Desiree A. Thayer; Chi-Huey Wong; Christopher T. Walsh


ACS Chemical Biology | 2006

Enzymatic Tailoring of Enterobactin Alters Membrane Partitioning and Iron Acquisition

Minkui Luo; Hening Lin; Michael A. Fischbach; David R. Liu; Christopher T. Walsh; John T. Groves


Biochemistry | 2006

Structural characterization of enterobactin hydrolase IroE.

Nicholas A. Larsen; Hening Lin; Wei R; Michael A. Fischbach; Christopher T. Walsh


Chemistry & Biology | 2004

Enhanced Macrocyclizing Activity of the Thioesterase from Tyrocidine Synthetase in Presence of Nonionic Detergent

Ellen Yeh; Hening Lin; Susan L. Clugston; Rahul M. Kohli; Christopher T. Walsh


Journal of the American Chemical Society | 2006

Bromoenterobactins as Potent Inhibitors of a Pathogen-Associated, Siderophore-Modifying C-Glycosyltransferase

Hening Lin; Michael A. Fischbach; Gregory J. Gatto; David R. Liu; Christopher T. Walsh

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Michael A. Fischbach

California Institute for Quantitative Biosciences

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Desiree A. Thayer

Scripps Research Institute

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Kelly D. Smith

University of Washington

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