Collagen XVII (BP180) modulates keratinocyte expression of the proinflammatory chemokine, IL-8.

[junctional epidermolysis bullosa]

Collagen XVII (COL 17 ), a transmembrane protein expressed in epidermal keratinocytes (EK ), is targeted by pathogenic autoantibodies in bullous pemphigoid . Treatment of EK with anti-COL 17 autoantibodies triggers the production of proinflammatory cytokines . In this study , we test the hypothesis that COL 17 is involved in the regulation of the EK proinflammatory response , using IL -8 expression as the primary readout . The absence of COL 17 in EK derived from a junctional epidermolysis bullosa patient or shRNA-mediated knockdown of COL 17 in normal EK resulted in a dysregulation of IL -8 responses under various conditions . The COL 17 -deficient cells showed an abnormally high IL -8 response after treatment with lipopolysaccharide (LPS ), ultraviolet-B radiation or tumor necrosis factor , but exhibited a blunted IL -8 response to phorbol 12 -myristate 13 -acetate exposure . Induction of COL 17 expression in COL 17 -negative EK led to a normalization of the LPS-induced proinflammatory response . Although α 6 β 4 integrin was found to be up-regulated in COL 17 -deficient EK , siRNA-mediated knockdown of the α 6 and β 4 subunits revealed that COL 17 's effects on the LPS IL -8 response are not dependent on this integrin . In LPS-treated cells , inhibition of NF-kappa B activity in COL 17 -negative EK resulted in a normalization of their IL -8 response , and expression of an NF-kappa B-driven reporter was shown to be higher in COL 17 -deficient , compared with normal EK . These findings support the hypothesis that COL 17 plays an important regulatory role in the EK proinflammatory response , acting largely via NF-kappa B . Future investigations will focus on further defining the molecular basis of this novel control network .