Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System

Scabies is a parasitic infestation of the skin by the mite Sarcoptes scabiei that causes significant morbidity worldwide, in particular within socially disadvantaged populations. In order to identify mechanisms that enable the scabies mite to evade human immune defenses, we have studied molecules as...

Descripción completa

Detalles Bibliográficos
Autores principales: Mika, Angela, Reynolds, Simone L., Mohlin, Frida C., Willis, Charlene, Swe, Pearl M., Pickering, Darren A., Halilovic, Vanja, Wijeyewickrema, Lakshmi C., Pike, Robert N., Blom, Anna M., Kemp, David J., Fischer, Katja
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3394726/
https://www.ncbi.nlm.nih.gov/pubmed/22792350
http://dx.doi.org/10.1371/journal.pone.0040489
_version_ 1782237885361029120
author Mika, Angela
Reynolds, Simone L.
Mohlin, Frida C.
Willis, Charlene
Swe, Pearl M.
Pickering, Darren A.
Halilovic, Vanja
Wijeyewickrema, Lakshmi C.
Pike, Robert N.
Blom, Anna M.
Kemp, David J.
Fischer, Katja
author_facet Mika, Angela
Reynolds, Simone L.
Mohlin, Frida C.
Willis, Charlene
Swe, Pearl M.
Pickering, Darren A.
Halilovic, Vanja
Wijeyewickrema, Lakshmi C.
Pike, Robert N.
Blom, Anna M.
Kemp, David J.
Fischer, Katja
author_sort Mika, Angela
collection PubMed
description Scabies is a parasitic infestation of the skin by the mite Sarcoptes scabiei that causes significant morbidity worldwide, in particular within socially disadvantaged populations. In order to identify mechanisms that enable the scabies mite to evade human immune defenses, we have studied molecules associated with proteolytic systems in the mite, including two novel scabies mite serine protease inhibitors (SMSs) of the serpin superfamily. Immunohistochemical studies revealed that within mite-infected human skin SMSB4 (54 kDa) and SMSB3 (47 kDa) were both localized in the mite gut and feces. Recombinant purified SMSB3 and SMSB4 did not inhibit mite serine and cysteine proteases, but did inhibit mammalian serine proteases, such as chymotrypsin, albeit inefficiently. Detailed functional analysis revealed that both serpins interfered with all three pathways of the human complement system at different stages of their activation. SMSB4 inhibited mostly the initial and progressing steps of the cascades, while SMSB3 showed the strongest effects at the C9 level in the terminal pathway. Additive effects of both serpins were shown at the C9 level in the lectin pathway. Both SMSs were able to interfere with complement factors without protease function. A range of binding assays showed direct binding between SMSB4 and seven complement proteins (C1, properdin, MBL, C4, C3, C6 and C8), while significant binding of SMSB3 occurred exclusively to complement factors without protease function (C4, C3, C8). Direct binding was observed between SMSB4 and the complement proteases C1s and C1r. However no complex formation was observed between either mite serpin and the complement serine proteases C1r, C1s, MASP-1, MASP-2 and MASP-3. No catalytic inhibition by either serpin was observed for any of these enzymes. In summary, the SMSs were acting at several levels mediating overall inhibition of the complement system and thus we propose that they may protect scabies mites from complement-mediated gut damage.
format Online
Article
Text
id pubmed-3394726
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-33947262012-07-12 Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System Mika, Angela Reynolds, Simone L. Mohlin, Frida C. Willis, Charlene Swe, Pearl M. Pickering, Darren A. Halilovic, Vanja Wijeyewickrema, Lakshmi C. Pike, Robert N. Blom, Anna M. Kemp, David J. Fischer, Katja PLoS One Research Article Scabies is a parasitic infestation of the skin by the mite Sarcoptes scabiei that causes significant morbidity worldwide, in particular within socially disadvantaged populations. In order to identify mechanisms that enable the scabies mite to evade human immune defenses, we have studied molecules associated with proteolytic systems in the mite, including two novel scabies mite serine protease inhibitors (SMSs) of the serpin superfamily. Immunohistochemical studies revealed that within mite-infected human skin SMSB4 (54 kDa) and SMSB3 (47 kDa) were both localized in the mite gut and feces. Recombinant purified SMSB3 and SMSB4 did not inhibit mite serine and cysteine proteases, but did inhibit mammalian serine proteases, such as chymotrypsin, albeit inefficiently. Detailed functional analysis revealed that both serpins interfered with all three pathways of the human complement system at different stages of their activation. SMSB4 inhibited mostly the initial and progressing steps of the cascades, while SMSB3 showed the strongest effects at the C9 level in the terminal pathway. Additive effects of both serpins were shown at the C9 level in the lectin pathway. Both SMSs were able to interfere with complement factors without protease function. A range of binding assays showed direct binding between SMSB4 and seven complement proteins (C1, properdin, MBL, C4, C3, C6 and C8), while significant binding of SMSB3 occurred exclusively to complement factors without protease function (C4, C3, C8). Direct binding was observed between SMSB4 and the complement proteases C1s and C1r. However no complex formation was observed between either mite serpin and the complement serine proteases C1r, C1s, MASP-1, MASP-2 and MASP-3. No catalytic inhibition by either serpin was observed for any of these enzymes. In summary, the SMSs were acting at several levels mediating overall inhibition of the complement system and thus we propose that they may protect scabies mites from complement-mediated gut damage. Public Library of Science 2012-07-11 /pmc/articles/PMC3394726/ /pubmed/22792350 http://dx.doi.org/10.1371/journal.pone.0040489 Text en Mika et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Mika, Angela
Reynolds, Simone L.
Mohlin, Frida C.
Willis, Charlene
Swe, Pearl M.
Pickering, Darren A.
Halilovic, Vanja
Wijeyewickrema, Lakshmi C.
Pike, Robert N.
Blom, Anna M.
Kemp, David J.
Fischer, Katja
Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System
title Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System
title_full Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System
title_fullStr Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System
title_full_unstemmed Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System
title_short Novel Scabies Mite Serpins Inhibit the Three Pathways of the Human Complement System
title_sort novel scabies mite serpins inhibit the three pathways of the human complement system
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3394726/
https://www.ncbi.nlm.nih.gov/pubmed/22792350
http://dx.doi.org/10.1371/journal.pone.0040489
work_keys_str_mv AT mikaangela novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT reynoldssimonel novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT mohlinfridac novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT willischarlene novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT swepearlm novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT pickeringdarrena novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT halilovicvanja novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT wijeyewickremalakshmic novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT pikerobertn novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT blomannam novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT kempdavidj novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem
AT fischerkatja novelscabiesmiteserpinsinhibitthethreepathwaysofthehumancomplementsystem

Ejemplares similares