Male microchimerism and HLA compatibility in French women with sclerodema: a different profile in limited and diffuse subset.

نویسندگان

  • Justyna M Rak
  • Philippe P Pagni
  • Kiet Tiev
  • Yannick Allanore
  • Dominique Farge
  • Jean-Robert Harlé
  • David Launay
  • Eric Hachulla
  • Rémi Didelot
  • Jean Cabane
  • André Kahan
  • Marielle Martin
  • Brigitte Granel
  • Jean Roudier
  • Nathalie C Lambert
چکیده

OBJECTIVES Male microchimerism (Mc) persisting from pregnancy has been found at greater frequencies and/or higher quantities in women with scleroderma (SSc) compared with controls, suggesting a possible role in disease development. Moreover, women with an HLA-compatible child have a higher risk to develop SSc. We tested the hypothesis, on our French SSc cohort, that women with lcSSc and dcSSc, two distinct clinical subsets, have a different profile in terms of Mc and HLA compatibility in families. METHODS We studied 98 women (52 lcSSc and 46 dcSSc) for male Mc, by real-time PCR, in their whole blood and/or peripheral blood mononuclear cells (PBMC). Similarly, 91 matched healthy women were analysed. Complete HLA-DRB1 typing was obtained for 58 SSc and 68 control families (proband/children). RESULTS Women with lcSSc (N = 50) had male Mc more often in their whole blood than women with dcSSc (N = 40, 20 vs 5%, P = 0.038), but not significantly more than controls. By contrast, women with dcSSc (N = 36) hold Mc more often in PBMC (25 vs 9%), but not significantly and have greater quantities than controls (N = 82, P = 0.048). This contrast is also visible in feto-maternal HLA-DRB1 compatibility, which was increased only among women with lcSSc (N = 33) compared with controls (N = 68, P = 0.003). CONCLUSION For the first time, we showed that women with lcSSc and dcSSc hold male Mc in different blood compartments. Furthermore, a distinct pattern between the two SSc subtypes is observed for feto-maternal HLA-DRB1 compatibility. These results suggest a different mechanism behind each type of disease.

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عنوان ژورنال:
  • Rheumatology

دوره 48 4  شماره 

صفحات  -

تاریخ انتشار 2009