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  • Nilsson, GunnarUppsala universitet,Institutionen för genetik och patologi,Mast Cell Biology (author)

C3a and C5a are chemotaxins for human mast cells and act through distinct receptors via a pertussis toxin-sensitive signal transduction pathway

  • Article/chapterEnglish1996

Publisher, publication year, extent ...

  • 1996
  • printrdacarrier

Numbers

  • LIBRIS-ID:oai:DiVA.org:uu-51797
  • https://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-51797URI

Supplementary language notes

  • Language:English
  • Summary in:English

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  • Subject category:ref swepub-contenttype
  • Subject category:art swepub-publicationtype

Notes

  • Mast cells are known to accumulate at sites of inflammation, however, the chemotaxins involved are undefined. Since most natural leukocyte secretagogues also induce cell migration, and since the anaphylatoxins C3a and C5a are mast cell secretagogues, we hypothesized that both C3a and C5a are also mast cell chemotaxins. Here we report that C3a and C5a are, in fact, potent chemotaxins for the human mast cell line HMC-1. The optimal concentrations, half-maximal effective concentrations (a measure of agonist potency) and the efficacy (response at the optimal concentration) compared with medium control were, for C3a: 10 nM, 0.5 nM, and 256%, respectively; for C5a: 1 nM, 10 pM and 145%. Chemotaxis of HMC-1 cells to both C3a and C5a was blocked by pertussis toxin, suggesting that Gi-coupled receptors are involved in signal transduction. C3a and C5a also induced transient pertussis toxin-inhibitable increases in [Ca2+]i (ED50 = 1 nM for both) that could be homologously but not heterologously desensitized, suggesting that the receptors for C3a and C5a are distinct. These results make C3a the most effective mast cell chemotaxin identified to date. The chemotactic potency described here for C3a is also 100- to 1000-fold greater than for all of its previously described cellular actions. Direct chemoattraction of mast cells by C3a and C5a may help explain the rapid accumulation of mast cells at sites of inflammation.

Subject headings and genre

  • MEDICINE
  • MEDICIN

Added entries (persons, corporate bodies, meetings, titles ...)

  • Johnell, MatildaUppsala universitet,Institutionen för medicinska vetenskaper,Coagulation research (author)
  • Hammer, Carl H. (author)
  • Tiffany, H. Lee (author)
  • Nilsson, KennethUppsala universitet,Institutionen för genetik och patologi (author)
  • Metcalfe, Dean D. (author)
  • Siegbahn, AgnetaUppsala universitet,Institutionen för medicinska vetenskaper,Coagulation Research (author)
  • Murphy, Phil M. (author)
  • Uppsala universitetInstitutionen för genetik och patologi (creator_code:org_t)

Related titles

  • In:Journal of Immunology157:4, s. 1693-16980022-17671550-6606

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