2004
DOI: 10.1242/jcs.01310
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Globular domains 4/5 of the laminin α3 chain mediate deposition of precursor laminin 5

Abstract: In epidermal wounds, precursor laminin 5 (α3β3γ2) is deposited in the provisional basement membrane (PBM) before other BM components. Precursor laminin 5 contains G4/5 globular domains at the carboxyl terminus of the α3 chain. Here, the function of G4/5 was evaluated in deposition of laminin 5. Soluble laminin 5, secreted by keratinocytes in culture, is cleaved by an endogenous protease releasing G4/5. Thrombin, a serum protease, cleaves G4/5 indistinguishably from endogenous protease. Soluble human precursor … Show more

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Cited by 47 publications
(60 citation statements)
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“…3). Moreover, this localization is identical to that observed when skin cells are processed for indirect immunofluorescence using laminin-332 antibodies, as shown by a number of different workers (see, for example, Sehgal et al, 2006;Sigle et al, 2004)). …”
Section: Incorporation Of Tagged Laminin Subunits Into Laminin-332-risupporting
confidence: 83%
See 1 more Smart Citation
“…3). Moreover, this localization is identical to that observed when skin cells are processed for indirect immunofluorescence using laminin-332 antibodies, as shown by a number of different workers (see, for example, Sehgal et al, 2006;Sigle et al, 2004)). …”
Section: Incorporation Of Tagged Laminin Subunits Into Laminin-332-risupporting
confidence: 83%
“…First, it has been suggested that the LG4-5 domains of the α3 laminin subunit mediate deposition of laminin-332 into matrix (Sigle et al, 2004). This is not the case in HEKs and BEP2D cells since α3ΔLG4-5 is incorporated into their extracellular matrix.…”
Section: Incorporation Of Tagged Laminin Subunits Into Laminin-332-rimentioning
confidence: 99%
“…Additionally, the LM-332 contains a mix of both the precursor LM-332 as well as the cleaved LM-332. We have previously reported that Western blots indicated that the protein was primarily the cleaved LM-332 with only small amounts of precursor LM-332 (32). In normal human acute wounds, both precursor LM-332 and its mRNA have been detected in migrating KCs for up to 7 days.…”
Section: Discussionmentioning
confidence: 91%
“…Unfortunately, soluble purified precursor LM-332 is not currently available and when present even in small quantity, may be quickly cleaved (32). Sigle et al 2004 have engineered and expressed a non-cleavable LM-332 molecule by eliminating the cleavage site between the G4/ G5 segment and the remainder of the α chain (32). This approach bypasses the issue of rapid cleavage of LM-332, but this genetically engineered molecule is almost completely deposited by the KC's, precluding its release to culture medium and collection in sufficient quantities to test on experimental wounds.…”
Section: Discussionmentioning
confidence: 99%
“…The LG4,5 domain is typically cleaved and degraded immediately after LN332 secretion. However, its expression persists in keratinocytes migrating at the edge of epidermal wounds (61) and in a high percentage of squamous cell carcinomas (62), suggesting a possible connection between its expression and cell invasion, potentially by the Sdc1-dependent activation of ␣6␤4 integrin described here. Indeed, squamous carcinoma cells engineered to express the LG4,5 domain showed increased tumorigenesis in vivo (62).…”
Section: Tmentioning
confidence: 87%