Inhibition of B Lymphopoiesis by Adipocytes and IL-1–Producing Myeloid-Derived Suppressor Cells

Kennedy, Domenick E.; Knight, Katherine L.

doi:10.4049/jimmunol.1500957

Cited by 88 publications

(81 citation statements)

References 78 publications

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“…In the mouse retrovirus immunodeficiency system, ex vivo derived M-MDSCs from LP-BM5-infected mice also induced a moderate expansion of Tregs in vitro, but concurrently suppressed their IL-10 production (114 (44,162). More recent study showed that MDSCs in the bone marrow of aged mice suppressed B cell lymphopoiesis in an IL-1-dependent manner (74,75). B cells play crucial roles in cancer as sources of malignant cells in several lymphomas (136) and as sources of tumor-specific antibodies (144).…”

Section: Cd4mentioning

confidence: 99%

The Role of Myeloid-Derived Suppressor Cells in Viral Infection

2017

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Myeloid-derived suppressor cells (MDSCs) are heterogeneous immature myeloid cells that are well described as potent immune regulatory cells during human cancer and murine tumor models. Reports of MDSCs during viral infections remain limited, and their association with immunomodulation of viral diseases is still being defined. Here, we provide an overview of MDSCs or MDSC-like cells identified during viral infections, including murine viral models and human viral diseases. Understanding the similarities and/or differences of virally induced versus tumor-derived MDSCs will be important for designing future immunotherapeutic approaches.

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Section: Cd4mentioning

confidence: 99%

The Role of Myeloid-Derived Suppressor Cells in Viral Infection

2017

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“…B lymphopoiesis cultures of rabbit BM cells and OP9 stromal cells were performed in the presence of adipocyte-conditioned medium (ACM), and they found that the production of CD79a + B lineage cells was greatly inhibited, suggesting that adipocytes produce factors that negatively regulate B lymphopoiesis. In similar cultures of progenitors from human and mouse BM, ACM also inhibited B lymphopoiesis (Bilwani and Knight, 2012, Kennedy and Knight, 2015). In fact, the inhibitory activity of ACM appears to be conserved between mammals, as we found human, mouse, and rabbit B lymphopoiesis were all inhibited by ACM generated from adipocytes of these species interchangeably.…”

Section: Age-related Changes To the Bm Microenvironmentmentioning

confidence: 90%

“…MDSCs are most known for their capacity to inhibit T cell responses (Gabrilovich and Nagaraj, 2009), while only few studies have explored their interactions with other cell types (Green et al, 2013, Green et al, 2015, Kennedy and Knight, 2015, O’Connor et al, 2015, Zhu et al, 2007). Because the identification of MDSCs as suppressors of B lymphopoiesis is novel, we became intrigued by how this might be occurring.…”

Section: Age-related Changes To the Bm Microenvironmentmentioning

confidence: 99%

Bone marrow fat and the decline of B lymphopoiesis in rabbits

Kennedy

Witte

Knight

2016

Developmental & Comparative Immunology

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B lymphopoiesis is necessary to generate a diverse pool of naïve B cells that are able to respond to a broad spectrum of antigens during immune responses to pathogens and to vaccination. Rabbits have been utilized for many years to generate high affinity monoclonal and polyclonal antibodies. Specific antibodies generated in rabbits have greatly advanced scientific discoveries, but the unique qualities of rabbit B cell development have been underappreciated. Unlike in humans and mice, where B lymphopoiesis declines in mid to late life, B lymphopoiesis in rabbits arrests early in life, between 2–4 months of age. This review focuses on the early loss of B cell development in rabbits and the contribution of the bone marrow microenvironment to this process. We also propose directions for future research in this area, and discuss how the rabbit can be used as a model to understand the decline of B lymphopoiesis that occurs in humans late in life. Such studies will be important for developing therapeutics targeted to prevent and/or reverse declining B lymphopoiesis in the elderly, as well as boosting immunity and antibody responses after infection or vaccination.

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“…Our laboratory discovered that these M-MDSCs also strongly inhibited B cell proliferation (7) and B regulatory cell IL-10 responses (11); to our knowledge, this is the first report of MDSC-mediated suppression of B cells. Subsequently, additional evidence for B cells as targets of MDSCs has been presented (12)(13)(14), particularly in autoimmunity (15)(16)(17)(18) and during B cell lymphopoiesis (19)(20)(21). There is increasing appreciation of the role MDSCs play in viral systems (22).…”

Section: Introductionmentioning

confidence: 99%