Modulation of factor VIII‐specific memory B cells

Reipert, Birgit M.; Allacher, Peter; Hausl, Christina; Pordes, Aniko Ginta; Ahmad, Rafi; Lang, Isabell; Ilas, Josenato; Windyga, Jerzy; Klukowska, Anna; Muchitsch, Eva-Maria; Schwarz, Hans

doi:10.1111/j.1365-2516.2008.01962.x

Cited by 24 publications

(29 citation statements)

References 46 publications

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“…This mechanism depends on induction of Tregs, and the continued presence of these cells is required to maintain tolerance. The high expression of F.IX in mice following hepatic gene transfer (~20-40% of normal) may also be responsible for this rapid clearance of F.IX-specific antibodies due to suppression of memory B cells (4, 51). Though this phenomenon is understandably difficult to verify in human studies, it is encouraging that, to date, none of the patients treated with a liver-directed AAV vector have formed a F.IX-specific immune response (52, 53).…”

Section: Gene Therapies For Hemophlia Bmentioning

confidence: 99%

Gene therapy for hemophilia

Rogers

Herzog

2015

Front Biosci

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Hemophilia is an X-linked inherited bleeding disorder consisting of two classifications, hemophilia A and hemophilia B, depending on the underlying mutation. Although the disease is currently treatable with intravenous delivery of replacement recombinant clotting factor, this approach represents a significant cost both monetarily and in terms of quality of life. Gene therapy is an attractive alternative approach to the treatment of hemophilia that would ideally provide life-long correction of clotting activity with a single injection. In this review, we will discuss the multitude of approaches that have been explored for the treatment of both hemophilia A and B, including both in vivo and ex vivo approaches with viral and nonviral delivery vectors.

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Section: Gene Therapies For Hemophlia Bmentioning

confidence: 99%

Gene therapy for hemophilia

Rogers

Herzog

2015

Front Biosci

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“…To further validate Gal-9 as a new MSC-driven immune regulator, we extended our investigation and analyzed MSCs and Gal-9 in vivo in a disease model of allo immunization. Immunization against FVIII is the most frequent complication in hemophilia A treatment and FVIII triggers a profound IgG response in mice [54]. Because Rafei et al [55] demonstrated that MSC application support the clearance of anti-FVIII titers in mice, we wanted to know whether activated MSCs were capable of suppressing FVIII immune response simultaneously.…”

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confidence: 99%

Galectin-9 Is a Suppressor of T and B Cells and Predicts the Immune Modulatory Potential of Mesenchymal Stromal Cell Preparations

Ungerer

Quade-Lyssy

Radeke

et al. 2014

Stem Cells and Development

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Therapeutic approaches using multipotent mesenchymal stromal cells (MSCs) are advancing in regenerative medicine, transplantation, and autoimmune diseases. The mechanisms behind MSC immune modulation are still poorly understood and the prediction of the immune modulatory potential of single MSC preparations remains a major challenge for possible clinical applications. Here, we highlight galectin-9 (Gal-9) as a novel, important immune modulator expressed by MSCs, which is strongly upregulated upon activation of the cells by interferong (IFN-g). Further, we demonstrate that Gal-9 is a major mediator of the anti-proliferative and functional effects of MSCs not only on T cells but also on B cells. Here, Gal-9 and activated MSCs contribute to the suppression of antigen triggered immunoglobulin release. Moreover, we determined that Gal-9 expression could serve as a marker to predict a higher or lower immune modulatory potential of single cell preparations and therefore to distinguish the therapeutic potency of MSCs derived from different donors. Also in vivo co-administration of MSCs or murine Gal-9 resulted in significantly reduced IgG titers in mice immunized with human coagulation factor VIII (FVIII). In conclusion, Gal-9 acts as an immune modulator interfering with multiple cell types including B cells and Gal-9 may serve as a predictive indicator for clinical MSC therapy.

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“…Therefore, it is paramount to treat patients with high-titer inhibitory antibodies with effective strategies to reduce and best eliminate pre-existing inhibitory antibodies before attempting tolerance induction. Blockade of co-stimulatory pathway has been shown to prevent FVIII-specific murine memory B cells from becoming re-stimulated by FVIII in vitro and in vivo[37]. In our previous experiments, we have demonstrated that the combination treatment of IL-2/IL-2mAb complexes + rapamycin + anti-CD20 + FVIII reduced FVIII-specific memory B cells and ASCs from the spleen, leading to transient decreases of pre-existing neutralizing antibody titers [17].…”

Section: Discussionmentioning

confidence: 99%

Strategies to target long-lived plasma cells for treating hemophilia A inhibitors

Liu

Lyle²,

Shin³

et al. 2016

Cellular Immunology

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Long-lived plasma cells (LLPCs) can persistently produce anti-factor VIII (FVIII) antibodies which disrupt therapeutic effect of FVIII in hemophilia A patients with inhibitors, The migration of plasma cells to BM where they become LLPCs is largely controlled by an interaction between the chemokine ligand CXCL12 and its receptor CXCR4. AMD3100 combined with G-CSF inhibit their interactions, thus facilitating the mobilization of CD34+ cells and blocking the homing of LLPCs. These reagents were combined with anti-CD20 to reduce B-cells and the specific IL-2/IL-2mAb (JES6-1) complexes to induce Treg expansion for targeting anti-FVIII immune responses. Groups of mice primed with FVIII plasmid and protein respectively were treated with the combined regimen for six weeks, and a significant reduction of anti-FVIII inhibitor titers was observed, associated with the dramatic decrease of circulating and bone marrow CXCR4+ plasma cells. The combination regimens are highly promising in modulating pre-existing anti-FVIII antibodies in FVIII primed subjects.

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Modulation of factor VIII‐specific memory B cells

Cited by 24 publications

References 46 publications

Gene therapy for hemophilia

Gene therapy for hemophilia

Galectin-9 Is a Suppressor of T and B Cells and Predicts the Immune Modulatory Potential of Mesenchymal Stromal Cell Preparations

Strategies to target long-lived plasma cells for treating hemophilia A inhibitors

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