Identification in Collagen Type I of an Integrin α2β1-binding Site Containing an Essential GER Sequence

Knight, Christopher G.; Morton, L F; Onley, David J.; Peachey, Anthony R.; Messent, Anthea J.; Smethurst, Peter A.; Tuckwell, Danny S.; Farndale, Richard W.; Barnes, Michael J.

doi:10.1074/jbc.273.50.33287

Cited by 263 publications

(242 citation statements)

References 33 publications

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“…Similar to α 1 β 1 , a conformational-dependent binding to collagen I and IV has been shown for α 2 β 1 integrin (Knight et al, 1998). The α 2 β 1 integrin plays an important role in platelet adhesion to collagens and hemostasis in the blood vessel wall (Sixma et al, 1997).…”

Section: Integrin Receptorsmentioning

confidence: 99%

Mammalian collagen IV

Khoshnoodi

Pedchenko

Hudson

2008

Microscopy Res & Technique

538

470

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Four decades have passed since the first discovery of collagen IV by Kefalides in 1966. Since then collagen IV has been investigated extensively by a large number of research laboratories around the world. Advances in molecular genetics have resulted in identification of six evolutionary related mammalian genes encoding six different polypeptide chains of collagen IV. The genes are differentially expressed during the embryonic development, providing different tissues with specific collagen IV networks each having unique biochemical properties. Newly translated α-chains interact and assemble in the endoplasmic reticulum in a chain-specific fashion and form unique heterotrimers. Unlike most collagens, type IV collagen is an exclusive member of the basement membranes and through a complex inter-and intramolecular interactions form supramolecular networks that influence cell adhesion, migration, and differentiation. Collagen IV is directly involved in a number of genetic and acquired disease such as Alport's and Goodpasture's syndromes. Recent discoveries have also highlighted a new and direct role for collagen IV in the development of rare genetic diseases such as cerebral hemorrhage and porencephaly in infants and hemorrhagic stroke in adults. Years of intensive investigations have resulted in a vast body of information about the structure, function, and biology of collagen IV. In this review article, we will summarize essential findings on the structural and functional relationships of different collagen IV chains and their roles in health and disease.

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Section: Integrin Receptorsmentioning

confidence: 99%

Mammalian collagen IV

Khoshnoodi

Pedchenko

Hudson

2008

Microscopy Res & Technique

538

470

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“…Of the integrin receptors, a number of interactive sites have been mapped. The site at residue positions 435-438 was proposed to mediate platelet ␣ 2 ␤ 1 integrin-collagen binding (24,25); however, this was not subsequently confirmed (18,26). Another site at residues 567-569 was implicated in RGD-dependent cell adhesion (27) but was later shown relevant only for denatured collagen (28).…”

Section: Distribution Of Ligand-binding Sites and Functional Domains mentioning

confidence: 99%

“…Integrin-binding Sites-Type I collagen is considered an important substrate for cell adhesion, and receptors reported to mediate cell-type I collagen interactions include the ␣ 1 ␤ 1 and ␣ 2 ␤ 1 integrins (18,19), cell surface HSPGs (20), and the discoidin domain receptors 1 and 2 (DDR1 and DDR2) (21)(22)(23). Of the integrin receptors, a number of interactive sites have been mapped.…”

Section: Distribution Of Ligand-binding Sites and Functional Domains mentioning

confidence: 99%

Mapping the Ligand-binding Sites and Disease-associated Mutations on the Most Abundant Protein in the Human, Type I Collagen

Lullo¹,

Sweeney²,

Körkkö³

et al. 2002

Journal of Biological Chemistry

795

533

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Type I collagen is the most abundant protein in humans, and it helps to maintain the integrity of many tissues via its interactions with cell surfaces, other extracellular matrix molecules, and growth and differentiation factors. Nearly 50 molecules have been found to interact with type I collagen, and for about half of them, binding sites on this collagen have been elucidated. In addition, over 300 mutations in type I collagen associated with human connective tissue disorders have been described. However, the spatial relationships between the known ligand-binding sites and mutation positions have not been examined. To this end, here we have created a map of type I collagen that includes all of its ligand-binding sites and mutations. The map reveals the existence of several hot spots for ligand interactions on type I collagen and that most of the binding sites locate to its C-terminal half. Moreover, on the collagen fibril some potentially relevant relationships between binding sites were observed including the following: fibronectin-and certain integrin-binding regions are near neighbors, which may mechanistically relate to fibronectin-dependent cell-collagen attachment; proteoglycan binding may potentially impact upon collagen fibrillogenesis, cell-collagen attachment, and collagen glycation seen in diabetes and aging; and mutations associated with osteogenesis imperfecta and other disorders show apparently nonrandom distribution patterns within both the monomer and fibril, implying that mutation positions correlate with disease phenotype. These and other observations presented here may provide novel insights into evaluating type I collagen functions and the relationships between its binding partners and mutations.

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“…2B). To confirm an essential role of integrin α2 in the induction of HOTAIR, we inhibited integrin α2 using its neutralizing antibody (clone JBS2) in lrECM 3D culture of MDA‐MB‐231 and Hs578T cells (Knight et al ., 1998). The integrin α2‐neutralizing antibody (10 μg·mL −1 ) reduced the RNA levels of HOTAIR to 32% and 38% of that in the control IgG‐treated MDA‐MB‐231 and Hs578T cells, respectively (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The GAPDH‐ and BRD4‐specific antibodies were purchased from Novus Biologicals (Littleton, CO, USA) and Cell Signaling (Danvers, MA, USA), respectively. An integrin α2β1‐neutralizing antibody (clone JBS2) was purchased from Chemicon (Temecula, CA, USA) (Knight et al ., 1998). A retroviral vector expressing dominant‐negative chicken Src‐K295R mutant (dnSrc) was kindly provided by Joan Brugge at Harvard University (Thomas et al ., 1991).…”

Section: Methodsmentioning

confidence: 99%

Induction of a novel isoform of the lncRNA HOTAIR in Claudin‐low breast cancer cells attached to extracellular matrix

Zhuang

et al. 2017

Molecular Oncology

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Elevated overexpression of the lncRNA HOTAIR mediates invasion and metastasis in breast cancer. In an apparent paradox, we observed low expression of HOTAIR in the invasive Claudin‐low MDA‐MB‐231 and Hs578T cells in two‐dimensional culture (2D). However, HOTAIR expression exhibited robust induction in laminin‐rich extracellular matrix‐based three‐dimensional organotypic culture (lrECM 3D) over that in 2D culture. Induction of HOTAIR required intact ECM signaling, namely integrin α2 and SRC kinase activity. Moreover, invasive growth was suppressed by HOTAIR‐specific siRNA. Induction of HOTAIR in lrECM 3D culture resulted from the activation of a novel isoform of HOTAIR (HOTAIR‐N) whose transcription is started from the first intron of the HOXC11 gene. The HOTAIR‐N promoter exhibited increased trimethylation of histone H3 lysine 4, a histone marker of active transcription, and binding of BRD4, a reader of transcriptionally active histone markers. Inhibition of BRD4 substantially reduced the expression of HOTAIR in lrECM 3D culture. In summary, our results indicate that HOTAIR expression is activated by BRD4 binding to a novel HOTAIR‐N promoter in Claudin‐low breast cancer cells that are attached to ECM. Induction of HOTAIR is required for invasive growth of Claudin‐low breast cancer cells in lrECM 3D culture.

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Identification in Collagen Type I of an Integrin α2β1-binding Site Containing an Essential GER Sequence

Cited by 263 publications

References 33 publications

Mammalian collagen IV

Mammalian collagen IV

Mapping the Ligand-binding Sites and Disease-associated Mutations on the Most Abundant Protein in the Human, Type I Collagen

Induction of a novel isoform of the lncRNA HOTAIR in Claudin‐low breast cancer cells attached to extracellular matrix

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