Pathways and bottlenecks in the web of inflammatory adhesion molecules and chemoattractants

Klaus Ley

doi:10.1385/IR:24:1:87

Pathways and bottlenecks in the web of inflammatory adhesion molecules and chemoattractants

Klaus Ley

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

47 Scopus citations

Abstract

Leukocyte recruitment requires capture, rolling, activation, adhesion, and transmigration. Adhesion molecules and chemoattractants have been identified that mediate each of these steps. Their functions often overlap, but the combined absence of some molecules can lead to severe spontaneous phenotypes, as seen in CD18-/- mice, or early lethality, as in CD18-/- E-selectin-/- mice. These groups of molecules define bottlenecks that restrict the inflammatory response. Adhesion molecules and activation mechanisms can also form groups of preferential usage, or pathways. Based on these findings, a web-like model may represent the inflammatory process better than the linear cascade model. Bottlenecks and pathways depend on the degree and nature of overlapping functions, the disease process, tissue site, and the inflammatory stimulus.

Original language	English (US)
Pages (from-to)	87-95
Number of pages	9
Journal	Immunologic Research
Volume	24
Issue number	1
DOIs	https://doi.org/10.1385/IR:24:1:87
State	Published - 2001
Externally published	Yes

Keywords

Chemokines
Inflammation
Integrins
Neutrophils
Selectins

ASJC Scopus subject areas

Immunology

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10.1385/IR:24:1:87

Cite this

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title = "Pathways and bottlenecks in the web of inflammatory adhesion molecules and chemoattractants",

abstract = "Leukocyte recruitment requires capture, rolling, activation, adhesion, and transmigration. Adhesion molecules and chemoattractants have been identified that mediate each of these steps. Their functions often overlap, but the combined absence of some molecules can lead to severe spontaneous phenotypes, as seen in CD18-/- mice, or early lethality, as in CD18-/- E-selectin-/- mice. These groups of molecules define bottlenecks that restrict the inflammatory response. Adhesion molecules and activation mechanisms can also form groups of preferential usage, or pathways. Based on these findings, a web-like model may represent the inflammatory process better than the linear cascade model. Bottlenecks and pathways depend on the degree and nature of overlapping functions, the disease process, tissue site, and the inflammatory stimulus.",

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note = "Funding Information: I would like to thank Dan C. Bullard and Geoff S. Kansas for valuable discussions that ultimately led to the development of the web model of pathways and bottlenecks. The original research underlying this review was supported by NIH R01 HL 54136 and HL 64381.",

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N2 - Leukocyte recruitment requires capture, rolling, activation, adhesion, and transmigration. Adhesion molecules and chemoattractants have been identified that mediate each of these steps. Their functions often overlap, but the combined absence of some molecules can lead to severe spontaneous phenotypes, as seen in CD18-/- mice, or early lethality, as in CD18-/- E-selectin-/- mice. These groups of molecules define bottlenecks that restrict the inflammatory response. Adhesion molecules and activation mechanisms can also form groups of preferential usage, or pathways. Based on these findings, a web-like model may represent the inflammatory process better than the linear cascade model. Bottlenecks and pathways depend on the degree and nature of overlapping functions, the disease process, tissue site, and the inflammatory stimulus.

AB - Leukocyte recruitment requires capture, rolling, activation, adhesion, and transmigration. Adhesion molecules and chemoattractants have been identified that mediate each of these steps. Their functions often overlap, but the combined absence of some molecules can lead to severe spontaneous phenotypes, as seen in CD18-/- mice, or early lethality, as in CD18-/- E-selectin-/- mice. These groups of molecules define bottlenecks that restrict the inflammatory response. Adhesion molecules and activation mechanisms can also form groups of preferential usage, or pathways. Based on these findings, a web-like model may represent the inflammatory process better than the linear cascade model. Bottlenecks and pathways depend on the degree and nature of overlapping functions, the disease process, tissue site, and the inflammatory stimulus.

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KW - Integrins

KW - Neutrophils

KW - Selectins

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Pathways and bottlenecks in the web of inflammatory adhesion molecules and chemoattractants

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

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