Anna Sławek scite author profile

Anna Sławek

3Publications

47Citation Statements Received

62Citation Statements Given

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Ludwik Hirszfeld Institute of Immunology and Experimental Therapy, Polish Academy of Sciences

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Tregitopes regulate the tolerogenic immune response and decrease the foetal death rate in abortion-prone mouse matings

Kędzierska

Lorek

Sławek

et al. 2020

Sci Rep

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The imbalance in immune tolerance may cause the variety of reproductive failures. An intravenous immunoglobulin infusion (IVIg) therapy is used to improve the live birth rate in women suffering from recurrent pregnancy loss, recurrent spontaneous abortions and recurrent implantation failures. However, the results of IVIg studies are still inconclusive as IVIg infusion in women suffering from pregnancy loss is sometimes ineffective. One of the mechanisms of action of this treatment is inhibition of B cells differentiation and expansion of Tregs and secretion of interleukin 10. It was proposed that immunomodulatory effects of IVIg may be attributed to tregitopes - self-IgG-derived epitopes present in the structure of immunoglobulins. Similarly to IVIg, tregitopes cause the expansion of Tregs and secretion of antigen-specific effector cytokine response. Here, we studied whether the administration of mouse tregitope 167 and/or 289 can prevent abortions in mouse abortion-prone mouse matings. We revealed that tregitopes reduce the foetal death rate. This may be driven by observed higher pool of peripheral Tregs, increased production of IL-10 by Tregs and Bregs and/or maintaining the tolerogenic phenotype of antigen-presenting cells. We believe that our findings may indicate a potential alternative to IVIg for therapeutic intervention in case of pregnancy failures.

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CD40, CD80, and CD86 Costimulatory Molecules are Differentially Expressed on Murine Splenic Antigen‐presenting Cells During the Pre‐implantation Period of Pregnancy, and they Modulate Regulatory T‐cell Abundance, Peripheral Cytokine Response, and Pregnancy Outcome

Sławek

Maj

Chełmońska-Soyta

2013

American J Rep Immunol

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CD80 and CD86 Costimulatory Molecules Differentially Regulate OT-II CD4⁺T Lymphocyte Proliferation and Cytokine Response in Cocultures with Antigen-Presenting Cells Derived from Pregnant and Pseudopregnant Mice

Maj

Sławek

Chełmońska-Soyta

2014

Mediators of Inflammation

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Immune phenomena during the preimplantation period of pregnancy are poorly understood. The aim of our study was to assess the capacity for antigen presentation of splenic antigen-presenting cells (APCs) derived from pregnant and pseudopregnant mice in in vitro conditions. Therefore, sorted CD11c+ dendritic cells and macrophages F4/80+ and CD11b+ presenting ovalbumin (OVA) were cocultured with CD4+ T cells derived from OT-II mice's (C57BL6/J-Tg(TcraTcrb)1100Mjb/J) spleen. After 132 hours of cell culture, proliferation of lymphocytes (ELISA-BrdU), activation of these cells (flow cytometry), cytokine profile (ELISA), and influence of costimulatory molecules blocking on these parameters were measured. We did not detect any differences in regulation of Th1/Th2 cytokine balance. CD86 seems to be the main costimulatory molecule involved in the proliferation response but CD80 is the main costimulatory molecule influencing cytokine secretion in pregnant mice. In conclusion, this study showed that CD80 and CD86 costimulatory molecules regulate OT-II CD4+ T lymphocyte proliferation and cytokine response in cocultures with antigen-presenting cells derived from pregnant and pseudopregnant mice. The implications of these changes still remain unclear.

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Anna Sławek

Tregitopes regulate the tolerogenic immune response and decrease the foetal death rate in abortion-prone mouse matings

CD40, CD80, and CD86 Costimulatory Molecules are Differentially Expressed on Murine Splenic Antigen‐presenting Cells During the Pre‐implantation Period of Pregnancy, and they Modulate Regulatory T‐cell Abundance, Peripheral Cytokine Response, and Pregnancy Outcome

CD80 and CD86 Costimulatory Molecules Differentially Regulate OT-II CD4⁺T Lymphocyte Proliferation and Cytokine Response in Cocultures with Antigen-Presenting Cells Derived from Pregnant and Pseudopregnant Mice

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Anna Sławek

Tregitopes regulate the tolerogenic immune response and decrease the foetal death rate in abortion-prone mouse matings

CD40, CD80, and CD86 Costimulatory Molecules are Differentially Expressed on Murine Splenic Antigen‐presenting Cells During the Pre‐implantation Period of Pregnancy, and they Modulate Regulatory T‐cell Abundance, Peripheral Cytokine Response, and Pregnancy Outcome

CD80 and CD86 Costimulatory Molecules Differentially Regulate OT-II CD4+T Lymphocyte Proliferation and Cytokine Response in Cocultures with Antigen-Presenting Cells Derived from Pregnant and Pseudopregnant Mice

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CD80 and CD86 Costimulatory Molecules Differentially Regulate OT-II CD4⁺T Lymphocyte Proliferation and Cytokine Response in Cocultures with Antigen-Presenting Cells Derived from Pregnant and Pseudopregnant Mice