Joanna Massacand

Publications (3)18.81 Total impact

• Source

  Available from: Patrick Merky

  Dataset: mmc1-1

  Kathy D McCoy, Maaike Stoel, Rebecca Stettler, Patrick Merky, Katja Fink, Beatrice M Senn, Corinne Schaer, Joanna Massacand, Bernhard Odermatt, Hans C Oettgen, Rolf M Zinkernagel, Nicolaas A Bos, Hans Hengartner, Andrew J Macpherson, Nicola L Harris
• Source

  Available from: Patrick Merky

  Article: Polyclonal and specific antibodies mediate protective immunity against enteric helminth infection.

  Kathy D McCoy, Maaike Stoel, Rebecca Stettler, Patrick Merky, Katja Fink, Beatrice M Senn, Corinne Schaer, Joanna Massacand, Bernhard Odermatt, Hans C Oettgen, Rolf M Zinkernagel, Nicolaas A Bos, Hans Hengartner, Andrew J Macpherson, Nicola L Harris
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  ABSTRACT: Anti-helminth immunity involves CD4+ T cells, yet the precise effector mechanisms responsible for parasite killing or expulsion remain elusive. We now report an essential role for antibodies in mediating immunity against the enteric helminth Heligmosomoides polygyrus (Hp), a natural murine parasite that establishes chronic infection. Polyclonal IgG antibodies, present in naive mice and produced following Hp infection, functioned to limit egg production by adult parasites. Comparatively, affinity-matured parasite-specific IgG and IgA antibodies that developed only after multiple infections were required to prevent adult worm development. These data reveal complementary roles for polyclonal and affinity-matured parasite-specific antibodies in preventing enteric helminth infection by limiting parasite fecundity and providing immune protection against reinfection, respectively. We propose that parasite-induced polyclonal antibodies play a dual role, whereby the parasite is allowed to establish chronicity, while parasite load and spread are limited, likely reflecting the long coevolution of helminth parasites with their hosts.
  Cell host & microbe 11/2008; 4(4):362-73. · 13.02 Impact Factor
• Source

  Available from: Patrick Merky

  Article: Mechanisms of neonatal mucosal antibody protection.

  Nicola L Harris, Iris Spoerri, Jacqueline F Schopfer, Chiara Nembrini, Patrick Merky, Joanna Massacand, Joseph F Urban, Alain Lamarre, Kurt Burki, Bernhard Odermatt, Rolf M Zinkernagel, Andrew J Macpherson
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  ABSTRACT: Following an abrupt transition at birth from the sterile uterus to an environment with abundant commensal and pathogenic microbes, neonatal mammals are protected by maternal Abs at mucosal surfaces. We show in mice that different Ab isotypes work in distinct ways to protect the neonatal mucosal surface. Secretory IgA acts to limit penetration of commensal intestinal bacteria through the neonatal intestinal epithelium: an apparently primitive process that does not require diversification of the primary natural Ab repertoire. In contrast, neonatal protection against the exclusively luminal parasite Heligmosomoides polygyrus required IgG from primed females. This immune IgG could either be delivered directly in milk or retrotransported via neonatal Fc receptor from the neonatal serum into the intestinal lumen to exert its protective effect.
  The Journal of Immunology 12/2006; 177(9):6256-62. · 5.79 Impact Factor