Pemphigus autoantibodies generated through somatic mutations target the desmoglein-3 cis-interface
Giovanni Di Zenzo, Giulia Di Lullo, Davide Corti, Valentina Calabresi, Anna Sinistro, Fabrizia Vanzetta, Biagio Didona, Giuseppe Cianchini, Michael Hertl, Rudiger Eming, Masayuki Amagai, Bungo Ohyama, Takashi Hashimoto, Jerry Sloostra, Federica Sallusto, Giovanna Zambruno, Antonio Lanzavecchia
Giovanni Di Zenzo, Giulia Di Lullo, Davide Corti, Valentina Calabresi, Anna Sinistro, Fabrizia Vanzetta, Biagio Didona, Giuseppe Cianchini, Michael Hertl, Rudiger Eming, Masayuki Amagai, Bungo Ohyama, Takashi Hashimoto, Jerry Sloostra, Federica Sallusto, Giovanna Zambruno, Antonio Lanzavecchia
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Research Article Autoimmunity

Pemphigus autoantibodies generated through somatic mutations target the desmoglein-3 cis-interface

Abstract

Pemphigus vulgaris (PV) is an autoimmune blistering disease of skin and mucous membranes caused by autoantibodies to the desmoglein (DSG) family proteins DSG3 and DSG1, leading to loss of keratinocyte cell adhesion. To learn more about pathogenic PV autoantibodies, we isolated 15 IgG antibodies specific for DSG3 from 2 PV patients. Three antibodies disrupted keratinocyte monolayers in vitro, and 2 were pathogenic in a passive transfer model in neonatal mice. The epitopes recognized by the pathogenic antibodies were mapped to the DSG3 extracellular 1 (EC1) and EC2 subdomains, regions involved in cis-adhesive interactions. Using a site-specific serological assay, we found that the cis-adhesive interface on EC1 recognized by the pathogenic antibody PVA224 is the primary target of the autoantibodies present in the serum of PV patients. The autoantibodies isolated used different heavy- and light-chain variable region genes and carried high levels of somatic mutations in complementary-determining regions, consistent with antigenic selection. Remarkably, binding to DSG3 was lost when somatic mutations were reverted to the germline sequence. These findings identify the cis-adhesive interface of DSG3 as the immunodominant region targeted by pathogenic antibodies in PV and indicate that autoreactivity relies on somatic mutations generated in the response to an antigen unrelated to DSG3.

Authors

Giovanni Di Zenzo, Giulia Di Lullo, Davide Corti, Valentina Calabresi, Anna Sinistro, Fabrizia Vanzetta, Biagio Didona, Giuseppe Cianchini, Michael Hertl, Rudiger Eming, Masayuki Amagai, Bungo Ohyama, Takashi Hashimoto, Jerry Sloostra, Federica Sallusto, Giovanna Zambruno, Antonio Lanzavecchia

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Figure 4

Epitope mapping of 3 pathogenic antibodies.

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Epitope mapping of 3 pathogenic antibodies. (A) Alignment of DSG3 amino ...
(A) Alignment of DSG3 amino acid sequence 1–232 with C-cadherin, DSG1, DSG2, and DSG4. EC1, EC2, and EC3 subdomains are highlighted with red, blue, and orange boxes, respectively. Peptides recognized by PVA224 are highlighted in blue and pink, peptides recognized by PVB28 in green, and peptides recognized by PVB124 in light blue, red, and green. The reported amino acid residues bound by AK23 (13) are highlighted in yellow. (B) Location of peptides recognized by PVA224, PVB28, PVB124, and AK23 on the structure of C-cadherin ectodomain as determined in ref. 8. Color code is as above. The trans-adhesive interface is indicated by a gray double arrow. The cis-adhesive interfaces are indicated by orange double arrows.