Your search keyword '"Bromberg, Jonathan S."' showing total 14 results

1. The lymph node stromal laminin [alpha]5 shapes alloimmunity

Author

Li, Lushen, Shirkey, Marina W., Zhang, Tianshu, Xiong, Yanbao, Piao, Wenji, Saxena, Vikas, Paluskievicz, Christina, Lee, Young, Toney, Nicholas, Cerel, Benjamin M., Li, Qinshan, Simon, Thomas, Smith, Kyle D., Hippen, Keli L., Blazar, Bruce R., Abdi, Reza, and Bromberg, Jonathan S.

Subjects

Thermo Fisher Scientific Inc., Antigens, Laminin, B cells, Integrins, Hybrid vehicles, Scientific equipment industry, T cells, Surgery, Lymphocytes, Transplantation, Cell differentiation, Phenotypes, Human migration, Endothelium, Brain, Homografts, Immune response, Health care industry

Abstract

Lymph node stromal cells (LNSCs) regulate immunity through constructing lymphocyte niches. LNSC-produced laminin [alpha]5 (Lama5) regulates [CD4.sup.+] T cells but the underlying mechanisms of its functions are poorly understood. Here we show that depleting Lama5 in LNSCs resulted in decreased Lama5 protein in the LN cortical ridge (CR) and around high endothelial venules (HEVs). Lama5 depletion affected LN structure with increased HEVs, upregulated chemokines, and cell adhesion molecules, and led to greater numbers of Tregs in the T cell zone. Mouse and human T cell transendothelial migration and T cell entry into LNs were suppressed by Lama5 through the receptors [alpha]6 integrin and [alpha]-dystroglycan. During immune responses and allograft transplantation, depleting Lama5 promoted antigen-specific [CD4.sup.+] T cell entry into the CR through HEVs, suppressed T cell activation, and altered T cell differentiation to suppressive regulatory phenotypes. Enhanced allograft acceptance resulted from depleting Lama5 or blockade of T cell Lama5 receptors. Lama5 and Lama4/Lama5 ratios in allografts were associated with the rejection severity. Overall, our results demonstrated that stromal Lama5 regulated immune responses through altering LN structures and T cell behaviors. This study delineated a stromal Lama5-T cell receptor axis that can be targeted for immune tolerance modulation., Introduction The lymph node (LN) is the central hub that exchanges antigen-presenting cells and immune cells with peripheral tissues or blood, permitting T cells to encounter cognate antigens and orchestrating [...]

Published

2020

2. Strain-specific alterations in gut microbiome and host immune responses elicited by tolerogenic Bifidobacterium pseudolongum.

Author

Ma, Bing, Gavzy, Samuel J., Saxena, Vikas, Song, Yang, Piao, Wenji, Lwin, Hnin Wai, Lakhan, Ram, Iyyathurai, Jegan, Li, Lushen, France, Michael, Paluskievicz, Christina, Shirkey, Marina W., Hittle, Lauren, Munawwar, Arshi, Mongodin, Emmanuel F., and Bromberg, Jonathan S.

Subjects

GUT microbiome, BIFIDOBACTERIUM, IMMUNE response, CELL culture, IMMUNOREGULATION, COMPARATIVE method, PROBIOTICS, COMPARATIVE genomics

Abstract

The beneficial effects attributed to Bifidobacterium are largely attributed to their immunomodulatory capabilities, which are likely to be species- and even strain-specific. However, their strain-specificity in direct and indirect immune modulation remain largely uncharacterized. We have shown that B. pseudolongum UMB-MBP-01, a murine isolate strain, is capable of suppressing inflammation and reducing fibrosis in vivo. To ascertain the mechanism driving this activity and to determine if it is specific to UMB-MBP-01, we compared it to a porcine tropic strain B. pseudolongum ATCC25526 using a combination of cell culture and in vivo experimentation and comparative genomics approaches. Despite many shared features, we demonstrate that these two strains possess distinct genetic repertoires in carbohydrate assimilation, differential activation signatures and cytokine responses signatures in innate immune cells, and differential effects on lymph node morphology with unique local and systemic leukocyte distribution. Importantly, the administration of each B. pseudolongum strain resulted in major divergence in the structure, composition, and function of gut microbiota. This was accompanied by markedly different changes in intestinal transcriptional activities, suggesting strain-specific modulation of the endogenous gut microbiota as a key to immune modulatory host responses. Our study demonstrated a single probiotic strain can influence local, regional, and systemic immunity through both innate and adaptive pathways in a strain-specific manner. It highlights the importance to investigate both the endogenous gut microbiome and the intestinal responses in response to probiotic supplementation, which underpins the mechanisms through which the probiotic strains drive the strain-specific effect to impact health outcomes. [ABSTRACT FROM AUTHOR]

Published

2023

3. Engineering the lymph node environment promotes antigen-specific efficacy in type 1 diabetes and islet transplantation.

Author

Gammon, Joshua M., Carey, Sean T., Saxena, Vikas, Eppler, Haleigh B., Tsai, Shannon J., Paluskievicz, Christina, Xiong, Yanbao, Li, Lushen, Ackun-Farmmer, Marian, Tostanoski, Lisa H., Gosselin, Emily A., Yanes, Alexis A., Zeng, Xiangbin, Oakes, Robert S., Bromberg, Jonathan S., and Jewell, Christopher M.

Subjects

TYPE 1 diabetes, LYMPH nodes, REGULATORY T cells, T cells, GRAFT rejection, IMMUNE response

Abstract

Antigen-specific tolerance is a key goal of experimental immunotherapies for autoimmune disease and allograft rejection. This outcome could selectively inhibit detrimental inflammatory immune responses without compromising functional protective immunity. A major challenge facing antigen-specific immunotherapies is ineffective control over immune signal targeting and integration, limiting efficacy and causing systemic non-specific suppression. Here we use intra-lymph node injection of diffusion-limited degradable microparticles that encapsulate self-antigens with the immunomodulatory small molecule, rapamycin. We show this strategy potently inhibits disease during pre-clinical type 1 diabetes and allogenic islet transplantation. Antigen and rapamycin are required for maximal efficacy, and tolerance is accompanied by expansion of antigen-specific regulatory T cells in treated and untreated lymph nodes. The antigen-specific tolerance in type 1 diabetes is systemic but avoids non-specific immune suppression. Further, microparticle treatment results in the development of tolerogenic structural microdomains in lymph nodes. Finally, these local structural and functional changes in lymph nodes promote memory markers among antigen-specific regulatory T cells, and tolerance that is durable. This work supports intra-lymph node injection of tolerogenic microparticles as a powerful platform to promote antigen-dependent efficacy in type 1 diabetes and allogenic islet transplantation. Antigen-specific tolerance represents a promising strategy to treat type 1 diabetes and islet allograft rejection. Here, the authors deliver immune signals to lymph nodes to promote antigen-specific regulatory T cells and prevent disease in models of type 1 diabetes and allogenic islet transplantation. [ABSTRACT FROM AUTHOR]

Published

2023

4. Regulation of the Immune System by Laminins.

Author

Simon, Thomas and Bromberg, Jonathan S.

Subjects

*LAMININS, *IMMUNOREGULATION, *IMMUNE response, *AUTOIMMUNE disease treatment, *TRANSPLANTATION immunology

Abstract

Laminins are trimeric proteins that are major components of the basement membranes that separate endothelia and epithelia from the underlying tissue. Sixteen laminin isoforms have been described, each with distinct tissue expression patterns and functions. While laminins have a critical structural role, recent evidence also indicates that they also impact the migration and functions of immune cells. Laminins are differentially expressed upon immunity or tolerance and orientate the immune response. This review will summarize the structure of laminins, the modulation of their expression, and their interactions with the immune system. Finally, the role of the laminins in autoimmune diseases and transplantation will be discussed. [ABSTRACT FROM AUTHOR]

Published

2017

5. Author Correction: Strain-specific alterations in gut microbiome and host immune responses elicited by tolerogenic Bifidobacterium pseudolongum.

Author

Ma, Bing, Gavzy, Samuel J., Saxena, Vikas, Song, Yang, Piao, Wenji, Lwin, Hnin Wai, Lakhan, Ram, Iyyathurai, Jegan, Li, Lushen, France, Michael, Paluskievicz, Christina, Shirkey, Marina W., Hittle, Lauren, Munawwar, Arshi, Mongodin, Emmanuel F., and Bromberg, Jonathan S.

Subjects

GUT microbiome, IMMUNE response, BIFIDOBACTERIUM, SPELLING errors

Abstract

The original article can be found online at https://doi.org/10.1038/s41598-023-27706-0. Correction to: I Scientific Reports i https://doi.org/10.1038/s41598-023-27706-0, published online 19 January 2023 The original version of this Article contained an error in the spelling of the author Jegan Iyyathurai which was incorrectly given as Jegan Lyyathurai. [Extracted from the article]

Published

2023

6. Lymphangiogenesis Is Required for Pancreatic Islet Inflammation and Diabetes.

Author

,4Na Yin, Nan Zhang, Lal, Girdhari, Jiangnan Xu, Minhong Yan, Yaozhong Ding, and Bromberg, Jonathan S.

Subjects

TRANSPLANTATION of organs, tissues, etc., INFLAMMATION, IMMUNE response, AUTOIMMUNITY, STREPTOZOTOCIN, CHEMOKINES

Abstract

Lymphangiogenesis is a common phenomenon observed during inflammation and engraftment of transplants, but its precise role in the immune response and underlying mechanisms of regulation remain poorly defined. Here we showed that in response to injury and autoimmunity, lymphangiogenesis occurred around islets and played a key role in the islet inflammation in mice. Vascular endothelial growth factors receptor 3 (VEGFR3) is specifically involved in lymphangiogenesis, and blockade of VEGFR3 potently inhibited lymphangiogenesis in both islets and the draining LN during multiple low-dose streptozotocin (MLDS) induced autoimmune insulitis, which resulted in less T cell infiltration, preservation of islets and prevention of the onset of diabetes. In addition to their well-known conduit function, lymphatic endothelial cells (LEC) also produced chemokines in response to inflammation. These LEC attracted two distinct CX3CR1hi and LYVE-1+ macrophage subsets to the inflamed islets and CX3CR1hi cells were influenced by LEC to differentiate into LYVE-1+ cells closely associated with lymphatic vessels. These observations indicate a linkage among lymphangiogenesis and myeloid cell inflammation during insulitis. Thus, inhibition of lymphangiogenesis holds potential for treating insulitis and autoimmune diabetes. [ABSTRACT FROM AUTHOR]

Published

2011

7. CD4+CD25+ Regulatory T-Cells Inhibit the Islet Innate Immune Response and Promote Islet Engraftment.

Author

Chen, Dongmei, Zhang, Nan, Fu, Shuang, Schröppel, Bernd, Guo, Qiongfen, Garin, Alexandre, Lira, Sergio A., and Bromberg, Jonathan S.

Subjects

ISLANDS of Langerhans, CELL transplantation, PHYSIOLOGICAL stress, IMMUNE response, INFLAMMATION

Abstract

Early islet cell loss is a significant problem in clinical islet cell transplantation. Diverse stress stimuli induce innate immune responses in islets that contribute to β-cell dysfunction, inflammation, and loss. Here, we show that cytokine-stimulated murine islets express multiple inflammatory chemokines that recruit T-cells and thereby impair islet function in vitro and in vivo. Both nonislet ductal and exocrine elements and the individual islet cellular components contribute to this innate immune response. CD4+CD25+ regulatory T-cells inhibit islet chemokine expression through a cell contact-dependent, soluble factor-independent mechanism and inhibit effector T-cell migration to the islet. Regulatory T-cells can also migrate to stimulated islets. Cotransfer of regulatory T-cells with islets in a transplantation model prevents islet innate immune responses and inflammation and preserves normal architecture and engraftment. Regulatory T-cell inhibition of multiple components of innate immune responses may be a fundamental aspect of their function that influences ischemia-reperfusion injury and adaptive immunity. Diabetes 55:1011-1021, 2006 [ABSTRACT FROM AUTHOR]

Published

2006

8. Islet implantation in a pocket.

Author

Bromberg, Jonathan S

Subjects

*ISLANDS of Langerhans transplantation, *PANCREATIC diseases, *PORTAL vein surgery, *HOMOGRAFTS, *IMMUNE response, *THERAPEUTICS

Abstract

The article focuses on a study related to transplantation of pancreatic islets in mice conducted by A.M. Shapiro. It states that clinically approved nylon cathers were subcutaneously implemented, inducing a vascularized pocket in which the islets were infused and mentions that the technique removes the hurdles related to technical and physiological restrictions related to portal vein infusion. It cites that challenges pertaining to tissue allograft such as immunological factors.

Published

2015

9. Regulatory T cell migration during an immune response

Author

Ding, Yaozhong, Xu, Jiangnan, and Bromberg, Jonathan S.

Subjects

*T cells, *CELL migration, *IMMUNE response, *INFLAMMATION, *LYMPH nodes, *TRANSCRIPTION factors

Abstract

CD4+CD25+Foxp3+ regulatory T (Treg) cells migrate into both inflammatory sites and draining lymph nodes (LNs) during an immune response, and have unique and overlaping functions in each location. Current studies suggest that Treg cells in draining LNs and inflamatory sites may not simply be a division of labor, but rather Treg cells migrate in a coordinated fashion between peripheral tissues and draining LNs. Trafficking between inflammatory sites and draining LNs is not only crucial for Treg cells to act, but also for them to acquire optimal immune regulatory activities. Furthermore, recent work has revealed that T helper (Th)1, Th2 and Th17 cell master transcription factors control Treg cell function by regulating genes important for Treg cell migration and suppression, and consequently affect disease pathogenesis. [Copyright &y& Elsevier]

Published

2012

10. Lymph node fibroblastic reticular cells steer immune responses.

Author

Li, Lushen, Wu, Jing, Abdi, Reza, Jewell, Christopher M., and Bromberg, Jonathan S.

Subjects

*IMMUNE response, *FOLLICULAR dendritic cells, *LYMPH nodes, *THERAPEUTICS, *GRAFT survival

Abstract

Lymph nodes (LNs), where immune responses are initiated, are organized into distinctive compartments by fibroblastic reticular cells (FRCs). FRCs imprint immune responses by supporting LN architecture, recruiting immune cells, coordinating immune cell crosstalk, and presenting antigens. Recent high-resolution transcriptional and histological analyses have enriched our knowledge of LN FRC genetic and spatial heterogeneities. Here, we summarize updated anatomic, phenotypic, and functional identities of FRC subsets, delve into topological and transcriptional remodeling of FRCs in inflammation, and illustrate the crosstalk between FRCs and immune cells. Discussing FRC functions in immunity and tolerance, we highlight state-of-the-art FRC-based therapeutic approaches for maintaining physiological homeostasis, steering protective immunity, inducing transplantation tolerance, and treating diverse immune-related diseases. High-resolution genetic and phenotypic studies have recently unveiled discrete fibroblast reticular cell (FRC) subsets in mice and humans; these harbor distinct functions and microanatomic distributions. FRC clusters create a variety of environmental niches in lymph nodes (LNs). The B cell-interacting reticular cells (BRCs), including marginal reticular cells (MRCs), light-and dark-zone follicular dendritic cells (LZ/DZ FDCs), and T–B border reticular cells (TBRCs), establish a feed-forward system determining germinal center responses in mice. The molecular identity of LZ/DZ FDCs is predetermined in the steady state. FRCs contribute to the regulation of inflammation-induced LN remodeling in mice and humans. Inflammation stimulates rapid FRC expansion, resulting in LN swelling, immune cell recruitment, vascular expansion, and alteration of conduit transport function. FRCs contribute to the maintenance of immune homeostasis, thereby protecting tissues from autoimmune attack. The maintenance of FRC integrity can reverse immunological scarring and preserve LN function for immune activation and for anticancer immunity. FRCs can constrain excessive immune responses. In murine transplantation, administration of FRCs to recipients or modification of FRC gene expression can ameliorate LN pathology and improve allograft survival. [ABSTRACT FROM AUTHOR]

Published

2021

11. Lymph node fibroblastic reticular cells deposit fibrosis-associated collagen following organ transplantation.

Author

Xiaofei Li, Jing Zhao, Kasinath, Vivek, Mayuko Uehara, Liwei Jiang, Banouni, Naima, McGrath, Martina M., Takaharu Ichimura, Fiorina, Paolo, Lemos, Dario R., Su Ryon Shin, Ware, Carl F., Bromberg, Jonathan S., Abdi, Reza, Li, Xiaofei, Zhao, Jing, Uehara, Mayuko, Jiang, Liwei, Ichimura, Takaharu, and Shin, Su Ryon

Subjects

*TRANSPLANTATION of organs, tissues, etc., *LYMPH nodes, *COLLAGEN, *MAST cells, *IMMUNE response

Abstract

Although the immune response within draining lymph nodes (DLNs) has been studied for decades, how their stromal compartment contributes to this process remains to be fully explored. Here, we show that donor mast cells were prominent activators of collagen I deposition by fibroblastic reticular cells (FRCs) in DLNs shortly following transplantation. Serial analysis of the DLN indicated that the LN stroma did not return to its baseline microarchitecture following organ rejection and that the DLN contained significant fibrosis following repetitive organ transplants. Using several FRC conditional-knockout mice, we show that induction of senescence in the FRCs of the DLN resulted in massive production of collagen I and a proinflammatory milieu within the DLN. Stimulation of herpes virus entry mediator (HVEM) on FRCs by its ligand LIGHT contributed chiefly to the induction of senescence in FRCs and overproduction of collagen I. Systemic administration of ex vivo-expanded FRCs to mice decreased DLN fibrosis and strengthened the effect of anti-CD40L in prolonging heart allograft survival. These data demonstrate that the transformation of FRCs into proinflammatory myofibroblasts is critically important for the maintenance of a proinflammatory milieu within a fibrotic DLN. [ABSTRACT FROM AUTHOR]

Published

2020

12. Regulatory T Cell Induction, Migration, and Function in Transplantation.

Author

Burrell, Bryna E., Nakayama, Yumi, Jiangnan Xu, Brinkman, C. Colin, and Bromberg, Jonathan S.

Subjects

*T cells, *CELLULAR control mechanisms, *CELL migration, *CELL transplantation, *HOMEOSTASIS, *IMMUNE response, *IMMUNOLOGIC diseases, *LABORATORY mice

Abstract

Regulatory T cells (Treg) are important in maintaining immune homeostasis and in regulating a variety of immune responses, making them attractive targets for modulating immune-related diseases. Success in using induction or transfer of Treg in mice to mediate transplant tolerance suggests Treg-based therapies as mechanisms of long-term drug-free transplant tolerance in human patients. Although more work is needed, critical analyses suggest that key factors in Treg induction, migration, and function are important areas to concentrate investigative efforts and therapeutic development. Elucidation of basic biology will aid in translating data gleaned from mice to humans so that Treg therapies become a reality for patients. [ABSTRACT FROM AUTHOR]

Published

2012

13. Myeloid-derived suppressor cells: Natural regulators for transplant tolerance

Author

Boros, Peter, Ochando, Jordi C., Chen, Shu-Hsia, and Bromberg, Jonathan S.

Subjects

*CELL populations, *IMMUNE response, *CANCER patients, *IMMUNOREGULATION, *CYTOLOGY, *GENE targeting, *CELLULAR signal transduction

Abstract

Abstract: Myeloid derived suppressor cells (MDSC) contribute to the negative regulation of immune response in cancer patients. This review summarizes results on important issues related to MDSC biology, including expansion and activation of MDSC, phenotype, and subsets as well pathways and different mechanisms by which these cells exert their suppressive effect. Recent observations suggesting that MDSC may have roles in transplant tolerance are presented. Although therapeutic targeting and destruction of MDCS is of primary interest in cancer patients, in transplantation it will instead be necessary to induce, expand, and activate these cells; thus current possibilities for in vitro generation of MDSC are also discussed. [ABSTRACT FROM AUTHOR]

Published

2010

14. Monocytic suppressive cells mediate cardiovascular transplantation tolerance in mice.

Author

Rodriguez Garcia, Mercedes, Ledgerwood, Levi, Yu Yang, Jiangnan Xu, Lal, Girdhari, Burrell, Bryna, Ge Ma, Hashimoto, Daigo, Yansui Li, Boros, Peter, Grisotto, Marcos, van Rooijen, Nico, Matesanz, Rafael, Tacke, Frank, Ginhoux, Florent, Yaozhong Ding, Shu-Hsia Chen, Randolph, Gwendalyn, Merad, Miriam, and Bromberg, Jonathan S.

Subjects

*TRANSPLANTATION of organs, tissues, etc., *IMMUNOSUPPRESSIVE agents, *LABORATORY mice, *BONE marrow, *MONOCYTES, *IMMUNE response, *ANIMAL experimentation, *COMPARATIVE studies, *GLYCOPROTEINS, *GRAFT versus host reaction, *IMMUNOLOGICAL tolerance, *INTERLEUKIN-2, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *MONOCLONAL antibodies, *RESEARCH, *RESEARCH funding, *EVALUATION research

Abstract

One of the main unresolved questions in solid organ transplantation is how to establish indefinite graft survival that is free from long-term treatment with immunosuppressive drugs and chronic rejection (i.e., the establishment of tolerance). The failure to achieve this goal may be related to the difficulty in identifying the phenotype and function of the cell subsets that participate in the induction of tolerance. To address this issue, we investigated the suppressive roles of recipient myeloid cells that may be manipulated to induce tolerance to transplanted hearts in mice. Using depleting mAbs, clodronate-loaded liposomes, and transgenic mice specific for depletion of CD11c+, CD11b+, or CD115+ cells, we identified a tolerogenic role for CD11b+CD115+Gr1+ monocytes during the induction of tolerance by costimulatory blockade with CD40L-specific mAb. Early after transplantation, Gr1+ monocytes migrated from the bone marrow into the transplanted organ, where they prevented the initiation of adaptive immune responses that lead to allograft rejection and participated in the development of Tregs. Our results suggest that mobilization of bone marrow CD11b+CD115+Gr1+ monocytes under sterile inflammatory conditions mediates the induction of indefinite allograft survival. We propose that manipulating the common bone marrow monocyte progenitor could be a useful clinical therapeutic approach for inducing transplantation tolerance. [ABSTRACT FROM AUTHOR]

Published

2010