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4 research outputs found

Structure and function of the complex formed by the tuberculosis virulence factors CFP-10 and ESAT-6

Author: Alderson MR
Bartels C
Behr MA
Bernard Burke
Berthet F-X
Brosch R
Carr MD
Cole ST
Cornilescu G
Delaglio F
Fred W Muskett
Geoff Kelly
Gey van Pittius NC
Guinn KM
Herrmann T
Hsu T
Jim Norman
Kirsty L Lightbody
Koradi R
Kwiatkowska K
Laskowski RA
Lemercinier X
Lightbody KL
Mahairas GG
Mark D Carr
Muskett FW
Philip S Renshaw
Pym AS
Pym AS
R Glyn Hewinson
Renshaw PS
Renshaw PS
Richard A Williamson
Rosenkrands I
Sassetti CM
Schnappinger D
Skj&oslash
Skj&oslash
Stanley SA
Stephen V Gordon
Thomas A Frenkiel
Thompson JD
Vaclav Veverka
Volkman HE
Wards BJ
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Calcium-Calmodulin Regulation of hEAG1 Channel Gating is also Important for the Enhanced Proliferation of hEAG1 Expressing cells

Author: Alina Finch
Fred W. Muskett
John S. Mitcheson
Raj Patel
Publication venue: 'Elsevier BV'
Publication date
Field of study

Crossref

Role of Dimerization in KH/RNA Complexes: The Example of Nova KH3

Author: Andres Ramos
Annalisa Pastore
David Hollingworth
Fred W. Muskett
Geoff Kelly
Salvatore Adinolfi
Sarah A. Major
Publication venue: 'American Chemical Society (ACS)'
Publication date
Field of study

Crossref

Structure and function of the complex formed by the tuberculosis virulence factors CFP-10 and ESAT-6

Author: Burke Bernard
Carr Mark D.
Frenkiel Thomas A.
Gordon Stephen V.
Hewinson R. Glyn
Kelly Geoff
Lightbody Kirsty L.
Muskett Fred W.
Norman Jim
Renshaw Philip S.
Veverka Vaclav
Williamson Richard A.
Publication venue
Publication date: 01/01/2005
Field of study

The secreted Mycobacterium tuberculosis complex proteins CFP-10 and ESAT-6 have recently been shown to play an essential role in tuberculosis pathogenesis. We have determined the solution structure of the tight, 1:1 complex formed by CFP-10 and ESAT-6, and employed fluorescence microscopy to demonstrate specific binding of the complex to the surface of macrophage and monocyte cells. A striking feature of the complex is the long flexible arm formed by the C-terminus of CFP-10, which was found to be essential for binding to the surface of cells. The surface features of the CFP-10.ESAT-6 complex, together with observed binding to specific host cells, strongly suggest a key signalling role for the complex, in which binding to cell surface receptors leads to modulation of host cell behaviour to the advantage of the pathogen

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