Your search keyword '"Wilhelmus S"' showing total 6 results

1. Increased microchimerism in peripheral blood of women with systemic lupus erythematosus: relation with pregnancy

Author

Bos, E.M., Rijnink, E.C., Zandbergen, M., Pool, J.D.N. Diaz de, Almekinders, M.M., Berden, J.H., Bijl, M. de, Hagen, E.C., Kolster-Bijdevaate, C., Steup-Beekman, G.M., Wolterbeek, R.., Bloemenkamp, K.W.M., Baelde, H.J., Bruijn, J.A., Bajema, I.M., Wilhelmus, S., Bos, E.M., Rijnink, E.C., Zandbergen, M., Pool, J.D.N. Diaz de, Almekinders, M.M., Berden, J.H., Bijl, M. de, Hagen, E.C., Kolster-Bijdevaate, C., Steup-Beekman, G.M., Wolterbeek, R.., Bloemenkamp, K.W.M., Baelde, H.J., Bruijn, J.A., Bajema, I.M., and Wilhelmus, S.

Abstract

Item does not contain fulltext, OBJECTIVES: We aimed to determine the presence, amount and origin of microchimerism in peripheral blood of pregnant and non-pregnant parous women with systemic lupus erythematosus (SLE) as compared to control subjects. METHODS: We performed a comparative study in which peripheral blood was drawn from eleven female non-pregnant SLE-patients and 22 control subjects, and from six pregnant SLE-patients and eleven control subjects during gestation and up to six months postpartum. Quantitative PCR for insertion-deletion polymorphisms and null alleles was used to detect microchimerism in peripheral blood mononuclear cells and granulocytes. RESULTS: Microchimerism was detected more often in non-pregnant SLE-patients than control subjects (54.4% vs. 13.6%, respectively; p=0.03). When present, the median total number of foetal chimeric cells was 5 gEq/106 in patients and 2.5gEq/106 in control subjects (p=0.048). Microchimerism was mostly foetal in origin; maternal microchimerism was detected in one patient and one control subject. In control subjects, microchimerism was always derived from only one source whereas in 50% of patients it originated from multiple sources. The pregnant patients had a significantly higher median number of foetal chimeric cells in the granulocyte fraction just after delivery than control subjects (7.5 gEq/106 vs. 0 gEq/106, respectively; p=0.02). CONCLUSIONS: Just after delivery, SLE-patients had more microchimerism than control subjects. Three months post-partum, microchimerism was no longer detectable, only to reappear many years after the last pregnancy, more often and at higher levels in SLE-patients than in control subjects. This suggests that these chimeric cells may originate from non-circulating foetal chimeric stem cells.

Published

2022

2. Increased microchimerism in peripheral blood of women with systemic lupus erythematosus: relation with pregnancy

Author

Bos, E.M., Rijnink, E.C., Zandbergen, M., Pool, J.D.N. Diaz de, Almekinders, M.M., Berden, J.H., Bijl, M. de, Hagen, E.C., Kolster-Bijdevaate, C., Steup-Beekman, G.M., Wolterbeek, R.., Bloemenkamp, K.W.M., Baelde, H.J., Bruijn, J.A., Bajema, I.M., Wilhelmus, S., Bos, E.M., Rijnink, E.C., Zandbergen, M., Pool, J.D.N. Diaz de, Almekinders, M.M., Berden, J.H., Bijl, M. de, Hagen, E.C., Kolster-Bijdevaate, C., Steup-Beekman, G.M., Wolterbeek, R.., Bloemenkamp, K.W.M., Baelde, H.J., Bruijn, J.A., Bajema, I.M., and Wilhelmus, S.

Abstract

Item does not contain fulltext, OBJECTIVES: We aimed to determine the presence, amount and origin of microchimerism in peripheral blood of pregnant and non-pregnant parous women with systemic lupus erythematosus (SLE) as compared to control subjects. METHODS: We performed a comparative study in which peripheral blood was drawn from eleven female non-pregnant SLE-patients and 22 control subjects, and from six pregnant SLE-patients and eleven control subjects during gestation and up to six months postpartum. Quantitative PCR for insertion-deletion polymorphisms and null alleles was used to detect microchimerism in peripheral blood mononuclear cells and granulocytes. RESULTS: Microchimerism was detected more often in non-pregnant SLE-patients than control subjects (54.4% vs. 13.6%, respectively; p=0.03). When present, the median total number of foetal chimeric cells was 5 gEq/106 in patients and 2.5gEq/106 in control subjects (p=0.048). Microchimerism was mostly foetal in origin; maternal microchimerism was detected in one patient and one control subject. In control subjects, microchimerism was always derived from only one source whereas in 50% of patients it originated from multiple sources. The pregnant patients had a significantly higher median number of foetal chimeric cells in the granulocyte fraction just after delivery than control subjects (7.5 gEq/106 vs. 0 gEq/106, respectively; p=0.02). CONCLUSIONS: Just after delivery, SLE-patients had more microchimerism than control subjects. Three months post-partum, microchimerism was no longer detectable, only to reappear many years after the last pregnancy, more often and at higher levels in SLE-patients than in control subjects. This suggests that these chimeric cells may originate from non-circulating foetal chimeric stem cells.

Published

2022

3. The efficient market hypothesis and insider trading during the recent financial crisis

Author

Wilhelmus, S., Wilhelmus, S., Wilhelmus, S., and Wilhelmus, S.

Published

2011

4. The efficient market hypothesis and insider trading during the recent financial crisis

Author

Wilhelmus, S., Wilhelmus, S., Wilhelmus, S., and Wilhelmus, S.

Published

2011

5. The recent crisis vs. the Scandinavian crisis: a comparison of the causes

Author

Wilhelmus, S., Wilhelmus, S., Wilhelmus, S., and Wilhelmus, S.

Published

2009

6. The recent crisis vs. the Scandinavian crisis: a comparison of the causes

Author

Wilhelmus, S., Wilhelmus, S., Wilhelmus, S., and Wilhelmus, S.

Published

2009