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Citations to this article

Constitutive and inducible expression of SKALP/elafin provides anti-elastase defense in human epithelia.
R Pfundt, … , P E van Erp, J Schalkwijk
R Pfundt, … , P E van Erp, J Schalkwijk
Published September 15, 1996
Citation Information: J Clin Invest. 1996;98(6):1389-1399. https://doi.org/10.1172/JCI118926.
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Constitutive and inducible expression of SKALP/elafin provides anti-elastase defense in human epithelia.

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Abstract

Skin-derived antileukoproteinase (SKALP), also known as elafin, is a serine proteinase inhibitor first discovered in keratinocytes from hyperproliferative human epidermis. In addition to the proteinase inhibiting domain which is directed against polymorphonuclear leukocyte (PMN) derived enzymes such as elastase and proteinase 3, SKALP contains multiple transglutaminase (TGase) substrate domains which enable crosslinking to extracellular and cell envelope proteins. Here we show that SKALP is constitutively expressed in several epithelia that are continuously subjected to inflammatory stimuli, such as the oral cavity and the vagina where it co-localizes with type 1 TGase. All epithelia from sterile body cavities are negative for SKALP. In general, stratified squamous epithelia are positive, whereas pseudostratified epithelia, simple/glandular epithelia and normal epidermis are negative. SKALP was found in fetal tissues of the oral cavity from 17 wk gestation onwards where it continued to be expressed up to adult life. Remarkably, in fetal epidermis SKALP was found from week 28 onwards, but was downregulated to undetectable levels in neonatal skin within three months, suggesting a role during pregnancy in feto-maternal interactions or in the early maturation phase of the epidermis. Immunoelectron microscopy revealed the presence of SKALP in secretory vesicles including the lamellar granules. In culture models for epidermal keratinocytes we found that expression of the endogenous SKALP gene provided protection against cell detachment caused by purified elastase or activated PMNs. Addition of exogenous recombinant SKALP fully protected the keratinocytes against PMN-dependent detachment whereas superoxide dismutase and catalase were only marginally effective. These findings strongly suggest that the constitutive expression of SKALP in squamous epithelia, and the inducible expression in epidermis participate in the control of epithelial integrity, by inhibiting PMN derived proteinases.

Authors

R Pfundt, F van Ruissen, I M van Vlijmen-Willems, H A Alkemade, P L Zeeuwen, P H Jap, H Dijkman, J Fransen, H Croes, P E van Erp, J Schalkwijk

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Journal of Investigative Dermatology 1998
Structural organization of cornified cell envelopes and alterations in inherited skin disorders
A Ishida-Yamamoto, H Iizuka
Experimental Dermatology 1998
SKALP/elafin gene polymorphisms are not associated with pustular forms of psoriasis
AL Kuijpers, R Pfundt, PL Zeeuwen, HO Molhuizen, EC Mariman, PC Kerkhof, J Schalkwijk
Clinical Genetics 1998
Epidermal cell kinetics by combining in situ hybridization and immunohistochemistry
F A Castelijns, J Ezendam, M A Latijnhouwers, I M Van Vlijmen-Willems, P L Zeeuwin, M J Gerritsen, P C Van de Kerkhof, P E Van Erp
The Histochemical Journal 1998
Human Epidermal Keratinocytes Are a Source of Tenascin-C during Wound Healing
M Latijnhouwers, M Bergers, M Ponec, H Dijkman, M Andriessen, J Schalkwijk
Journal of Investigative Dermatology 1997
Extremely low levels of epidermal skin-derived antileucoproteinase/elafin in a patient with impetigo herpetiformis
A Kuijpers, J Schalkwijk, H Rulo, J Peperkamp, P Kerkhof, E Jong
British Journal of Dermatology 1997
Identification and Sequence Analysis of Two New Members of the SKALP/elafin and SPAI-2 Gene Family: BIOCHEMICAL PROPERTIES OF THE TRANSGLUTAMINASE SUBSTRATE MOTIF AND SUGGESTIONS FOR A NEW NOMENCLATURE
PL Zeeuwen, W Hendriks, WW de Jong, J Schalkwijk
The Journal of biological chemistry 1997

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