Role of ADAM-9 Disintegrin-Cysteine-rich Domains in Human Keratinocyte Migration

Zigrino, Paola; Steiger, Julia; Fox, Jay W.; Löffek, Stefanie; Schild, Alexander; Nischt, Roswitha; Mauch, Cornelia

doi:10.1074/jbc.m701658200

Cited by 52 publications

(57 citation statements)

References 41 publications

(39 reference statements)

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“…Further evidence of the adhesive function of cysteine has been found in many cell adhesion proteins, since they can promote cell adhesion through their cysteine-rich domains. [19][20][21][22][23] Cysteine is assumed to play a role in maintaining the topology of charged amino acids on the molecular surface by the formation of intramolecular disulfidebonds.…”

Section: Discussionmentioning

confidence: 99%

Characterization of a Cysteine-Rich Protein Specifically Expressed in the Silk Gland of CaddisflyStenopsyche marmorata(Trichoptera; Stenopsychidae)

Wang

Zhao

et al. 2010

Bioscience, Biotechnology, and Biochemistry

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Section: Discussionmentioning

confidence: 99%

Characterization of a Cysteine-Rich Protein Specifically Expressed in the Silk Gland of CaddisflyStenopsyche marmorata(Trichoptera; Stenopsychidae)

Wang

Zhao

et al. 2010

Bioscience, Biotechnology, and Biochemistry

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“…The cells were resuspended in HEPES buffer (1 mM Hepes, 0.5% BSA, 1 mM of each CaCl 2 and MnCl 2 ). Adhesion assays were performed as described before (10). Briefly, 96-well tissue culture plates were coated with recombinant DC-9 and His 6 peptide (0.6 M) at 4°C overnight.…”

Section: Methodsmentioning

confidence: 99%

“…We have recently shown that ADAM-9 is expressed in both human and mouse epidermis. In keratinocytes, the adhesive activity of ADAM-9 leads to modulation of MMP-9 expression and cell migration (10). Further, proteolysis via ADAM-9 in keratinocytes has been shown to be important for the constitutive shedding of collagen XVII (11).…”

mentioning

confidence: 99%

The Disintegrin-like and Cysteine-rich domains of ADAM-9 Mediate Interactions between Melanoma Cells and Fibroblasts

Zigrino

Nischt

Mauch

2011

Journal of Biological Chemistry

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A characteristic of malignant cells is their capacity to invade their surrounding and to metastasize to distant organs. During these processes, proteolytic activities of tumor and stromal cells modify the extracellular matrix to produce a microenvironment suitable for their growth and migration. In recent years the family of ADAM proteases has been ascribed important roles in these processes. ADAM-9 is expressed in human melanoma at the tumor-stroma border where direct or indirect interactions between tumor cells and fibroblasts occur. To analyze the role of ADAM-9 for the interaction between melanoma cells and stromal fibroblasts, we produced the recombinant disintegrin-like and cysteine-rich domain of ADAM-9 (DC-9). Melanoma cells and human fibroblasts adhered to immobilized DC-9 in a Mn 2؉ -dependent fashion suggesting an integrin-mediated process. Inhibition studies showed that adhesion of fibroblasts was mediated by several ␤1 integrin receptors independent of the RGD and ECD recognition motif. Furthermore, interaction of fibroblasts and high invasive melanoma cells with soluble recombinant DC-9 resulted in enhanced expression of MMP-1 and MMP-2. Silencing of ADAM-9 in melanoma cells significantly reduced cell adhesion to fibroblasts. Ablation of ADAM-9 in fibroblasts almost completely abolished these cellular interactions and melanoma cell invasion in vitro. In summary, these results suggest that ADAM-9 expression plays an important role in mediating cell-cell contacts between fibroblasts and melanoma cells and that these interactions contribute to proteolytic activities required during invasion of melanoma cells.Growth and progression of human melanoma is a process that requires a cascade of different cellular processes including cellular interactions and proteolytic cleavage of growth factors and extracellular matrix proteins. ADAMs (a disintegrin and metalloproteinase) 2 with both their proteolytic and adhesive functions play a pivotal role in these processes (1).Most of the members of the ADAM family share a general phylogenetically well-conserved domain structure including a pro-, metalloprotease-, disintegrin-like-, cysteine rich-, EGFlike-, and cytoplasmic domain (reviewed by Refs. 2, 3). Apart from their proteolytic activity, ADAMs exert also adhesive functions, which are mediated for example in ADAM-15 by the RGD motif in the disintegrin-like domain (4). For other ADAMs, as ADAM-2 and ADAM-9, an electron capture detection motif (ECD) also located within the disintegrin-like domain has been reported to be responsible for this event (5, 6). In vitro studies have shown that ADAM-15 interacts with ␣ ␤ 3 and ␣ 5 ␤ 1 integrins (7), whereas ADAM-2 binds to ␣ 6 ␤ 1 integrin and ADAM-9 to ␣ 6 ␤ 1, ␣ ␤ 5 and ␣ 3 ␤ 1 integrins (6,8,9). The interactions of ADAM proteases with cellular receptors have been proven to be of major importance in cell adhesion and fusion processes as for instance during spermatogenesis (ADAM-1, -16, -20) and myo-and osteogenesis (ADAM-9, -12, -19) (1). We have recently shown that AD...

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“…Although studies have often focused on the proteolytic activity of members of this family, there is increasing evidence that they play a role in cell adhesion through direct interaction with integrins. ADAM9 is a widely expressed non-Arg-Gly-Asp-containing molecule, which has been shown to bind to αvβ5 on myeloma cells, α3β1 on keratinocytes, and α6β1 on fibroblasts (28,29,(31)(32)(33)(34). These studies raise the possibility that ADAM9 could mediate cell-platelet interactions to regulate dissemination of cancer cells.…”

Section: Introductionmentioning

confidence: 99%

“…Recombinant DC-9 was produced as previously described (33). Briefly, HEK293-EBNA cells were transfected by JetPei (Polyplus) with pCEP-pu BM40-cHis-Dis-Cys plasmid giving rise to a fusion protein with a His6 tag placed in frame with disintegrin-cysteine-rich coding regions of ADAM9.…”

Section: Methodsmentioning

confidence: 99%

Platelet integrin α6β1 controls lung metastasis through direct binding to cancer cell–derived ADAM9

Mammadova‐Bach¹,

Zigrino²,

Brucker³

et al. 2016

JCI Insight

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Role of ADAM-9 Disintegrin-Cysteine-rich Domains in Human Keratinocyte Migration

Cited by 52 publications

References 41 publications

Characterization of a Cysteine-Rich Protein Specifically Expressed in the Silk Gland of CaddisflyStenopsyche marmorata(Trichoptera; Stenopsychidae)

Characterization of a Cysteine-Rich Protein Specifically Expressed in the Silk Gland of CaddisflyStenopsyche marmorata(Trichoptera; Stenopsychidae)

The Disintegrin-like and Cysteine-rich domains of ADAM-9 Mediate Interactions between Melanoma Cells and Fibroblasts

Platelet integrin α6β1 controls lung metastasis through direct binding to cancer cell–derived ADAM9

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