Homotypic fibrillin-1 interactions in microfibril assembly

Andrew Marson; Matthew J. Rock; Stuart A. Cain; Lyle J. Freeman; Amanda Morgan; Kieran Mellody; C. Adrian Shuttleworth; Clair Baldock; Cay M. Kielty

doi:10.1074/jbc.M409029200

Homotypic fibrillin-1 interactions in microfibril assembly

Andrew Marson, Matthew J. Rock, Stuart A. Cain, Lyle J. Freeman, Amanda Morgan, Kieran Mellody, C. Adrian Shuttleworth, Clair Baldock, Cay M. Kielty

Research output: Contribution to journal › Article › peer-review

Abstract

We have defined the homotypic interactions of fibrillin-1 to obtain new insights into microfibril assembly. Dose-dependent saturable high affinity binding was demonstrated between N-terminal fragments, between furin processed C-terminal fragments, and between these N- and C-terminal fragments. The N terminus also interacted with a downstream fragment. A post-furin cleavage site C-terminal sequence also interacted with the N terminus, with itself and with the furin-processed fragment. No other homotypic fibrillin-1 interactions were detected. Some terminal homotypic interactions were inhibited by other terminal sequences, and were strongly calcium-dependent. Treatment of an N-terminal fragment with N-ethylmaleimide reduced homotypic binding. Microfibril-associated glycoprotein-1 inhibited N- to C-terminal interactions but not homotypic N-terminal interactions. These fibrillin-1 interactions are likely to regulate peri-cellular fibrillin-1 microfibril assembly.

Original language	English
Pages (from-to)	5013-5021
Number of pages	8
Journal	Journal of Biological Chemistry
Volume	280
Issue number	6
DOIs	https://doi.org/10.1074/jbc.M409029200
Publication status	Published - 11 Feb 2005

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title = "Homotypic fibrillin-1 interactions in microfibril assembly",

abstract = "We have defined the homotypic interactions of fibrillin-1 to obtain new insights into microfibril assembly. Dose-dependent saturable high affinity binding was demonstrated between N-terminal fragments, between furin processed C-terminal fragments, and between these N- and C-terminal fragments. The N terminus also interacted with a downstream fragment. A post-furin cleavage site C-terminal sequence also interacted with the N terminus, with itself and with the furin-processed fragment. No other homotypic fibrillin-1 interactions were detected. Some terminal homotypic interactions were inhibited by other terminal sequences, and were strongly calcium-dependent. Treatment of an N-terminal fragment with N-ethylmaleimide reduced homotypic binding. Microfibril-associated glycoprotein-1 inhibited N- to C-terminal interactions but not homotypic N-terminal interactions. These fibrillin-1 interactions are likely to regulate peri-cellular fibrillin-1 microfibril assembly.",

author = "Andrew Marson and Rock, {Matthew J.} and Cain, {Stuart A.} and Freeman, {Lyle J.} and Amanda Morgan and Kieran Mellody and Shuttleworth, {C. Adrian} and Clair Baldock and Kielty, {Cay M.}",

year = "2005",

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day = "11",

doi = "10.1074/jbc.M409029200",

language = "English",

volume = "280",

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journal = "Journal of Biological Chemistry",

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T1 - Homotypic fibrillin-1 interactions in microfibril assembly

AU - Marson, Andrew

AU - Rock, Matthew J.

AU - Cain, Stuart A.

AU - Freeman, Lyle J.

AU - Morgan, Amanda

AU - Mellody, Kieran

AU - Shuttleworth, C. Adrian

AU - Baldock, Clair

AU - Kielty, Cay M.

PY - 2005/2/11

Y1 - 2005/2/11

N2 - We have defined the homotypic interactions of fibrillin-1 to obtain new insights into microfibril assembly. Dose-dependent saturable high affinity binding was demonstrated between N-terminal fragments, between furin processed C-terminal fragments, and between these N- and C-terminal fragments. The N terminus also interacted with a downstream fragment. A post-furin cleavage site C-terminal sequence also interacted with the N terminus, with itself and with the furin-processed fragment. No other homotypic fibrillin-1 interactions were detected. Some terminal homotypic interactions were inhibited by other terminal sequences, and were strongly calcium-dependent. Treatment of an N-terminal fragment with N-ethylmaleimide reduced homotypic binding. Microfibril-associated glycoprotein-1 inhibited N- to C-terminal interactions but not homotypic N-terminal interactions. These fibrillin-1 interactions are likely to regulate peri-cellular fibrillin-1 microfibril assembly.

AB - We have defined the homotypic interactions of fibrillin-1 to obtain new insights into microfibril assembly. Dose-dependent saturable high affinity binding was demonstrated between N-terminal fragments, between furin processed C-terminal fragments, and between these N- and C-terminal fragments. The N terminus also interacted with a downstream fragment. A post-furin cleavage site C-terminal sequence also interacted with the N terminus, with itself and with the furin-processed fragment. No other homotypic fibrillin-1 interactions were detected. Some terminal homotypic interactions were inhibited by other terminal sequences, and were strongly calcium-dependent. Treatment of an N-terminal fragment with N-ethylmaleimide reduced homotypic binding. Microfibril-associated glycoprotein-1 inhibited N- to C-terminal interactions but not homotypic N-terminal interactions. These fibrillin-1 interactions are likely to regulate peri-cellular fibrillin-1 microfibril assembly.

U2 - 10.1074/jbc.M409029200

DO - 10.1074/jbc.M409029200

M3 - Article

C2 - 15569675

SN - 1083-351X

VL - 280

SP - 5013

EP - 5021

JO - Journal of Biological Chemistry

JF - Journal of Biological Chemistry

IS - 6

ER -

Homotypic fibrillin-1 interactions in microfibril assembly

Abstract

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