46 results on '"Rakoff-Nahoum S"'
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2. Role of the Innate Immune System and Host-Commensal Mutualism
- Author
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Rakoff-Nahoum, S., Medzhitov, R., Compans, R. W., editor, Cooper, M. D., editor, Honjo, T., editor, Koprowski, H., editor, Melchers, F., editor, Oldstone, M. B. A., editor, Olsnes, S., editor, Vogt, P. K., editor, Wagner, H., editor, Honjo, Tasuku, editor, and Melchers, Fritz, editor
- Published
- 2006
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3. Role of toll-like receptors in tissue repair and tumorigenesis
- Author
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Rakoff-Nahoum, S. and Medzhitov, R.
- Published
- 2008
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4. The fight for glycans in reproductive tract microbial ecology
- Author
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Hood Pishchany, M.I., primary and Rakoff-Nahoum, S., additional
- Published
- 2019
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5. Role of the Innate Immune System and Host-Commensal Mutualism
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Rakoff-Nahoum, S., primary and Medzhitov, R., additional
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6. Innate immune recognition of the indigenous microbial flora
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Rakoff-Nahoum, S, primary and Medzhitov, R, additional
- Published
- 2008
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7. Regulation of class II expression in monocytic cells after HIV-1 infection.
- Author
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Rakoff-Nahoum, S., primary, Chen, H., additional, Kraus, T., additional, George, I., additional, Oei, E., additional, Tyorkin, M., additional, Salik, E., additional, Beuria, P., additional, and Sperber, K., additional
- Published
- 2005
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8. Role of the Innate Immune System and Host-Commensal Mutualism.
- Author
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Compans, R. W., Cooper, M. D., Honjo, T., Koprowski, H., Melchers, F., Oldstone, M. B. A., Olsnes, S., Vogt, P. K., Wagner, H., Honjo, Tasuku, Melchers, Fritz, Rakoff-Nahoum, S., and Medzhitov, R.
- Abstract
Host organisms live in intimate contact with indigenous microflora. The interactions between the host and commensal microbiota are highly complex and heterogeneous. A growing body of evidence indicates that commensal symbionts provide many benefits to the host physiology, particularly in the gastrointestinal system. The molecularmechanisms of themutualistic interactions between the host and commensals are largely unknown but can be due either to bioactivity of the commensals or to the reaction of the host immune system to the commensal-derived products. Recent advances in our understanding of the innate immune system allow re-evaluation of some of the older findings regarding the mechanisms of benefits conferred by microflora. Here we review the examples of the benefits of host-commensal interactions that are due to recognition of commensal microbial products by the host innate immune system. [ABSTRACT FROM AUTHOR]
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- 2006
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9. Innate and adaptive immune connections in inflammatory bowel diseases.
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Rakoff-Nahoum S and Bousvaros A
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- 2010
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10. ABO blood groups and galectins: Implications in transfusion medicine and innate immunity.
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Arthur CM, Hollenhorst M, Wu SC, Jajosky R, Nakahara H, Jan HM, Zheng L, Covington M, Rakoff-Nahoum S, Yeung M, Lane W, Josephson C, Cummings RD, and Stowell SR
- Abstract
ABO blood group antigens, which are complex carbohydrate moieties, and the first human polymorphisms identified, are critical in transfusion medicine and transplantation. Despite their discovery over a century ago, significant questions remain about the development of anti-ABO antibodies and the structural features of ABO antigens that cause hemolytic transfusion reactions. Anti-ABO antibodies develop naturally during the first few months of life, in contrast to other red blood cell (RBC) alloantibodies which form after allogeneic RBC exposure. Anti-ABO antibodies are the most common immune barrier to transfusion and transplantation, but the factors driving their formation are incompletely understood. Some studies suggest that microbes that express glycans similar in structure to the blood group antigens could play a role in anti-blood group antibody formation. While the role of these microbes in clinically relevant anti-blood group antibody formation remains to be defined, the presence of these microbes raises questions about how blood group-positive individuals protect themselves against blood group molecular mimicry. Recent studies suggest that galectins can bind and kill microbes that mimic blood group antigens, suggesting a unique host defense mechanism against microbial molecular mimicry. However, new models are needed to fully define the impact of microbes, galectins, or other factors on the development of clinically relevant naturally occurring anti-blood group antibodies., (Copyright © 2024 Elsevier Ltd. All rights reserved.)
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- 2024
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11. Galectin-4 Antimicrobial Activity Primarily Occurs Through its C-Terminal Domain.
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Jan HM, Wu SC, Stowell CJ, Vallecillo-Zúniga ML, Paul A, Patel KR, Muthusamy S, Lin HY, Ayona D, Jajosky RP, Varadkar SP, Nakahara H, Chan R, Bhave D, Lane WJ, Yeung MY, Hollenhorst MA, Rakoff-Nahoum S, Cummings RD, Arthur CM, and Stowell SR
- Subjects
- Humans, Protein Domains, Protein Binding, Protein Multimerization, Blood Group Antigens metabolism, Escherichia coli metabolism, Anti-Infective Agents pharmacology, ABO Blood-Group System metabolism, ABO Blood-Group System immunology, Galectin 4 metabolism
- Abstract
Although immune tolerance evolved to reduce reactivity with self, it creates a gap in the adaptive immune response against microbes that decorate themselves in self-like antigens. This is particularly apparent with carbohydrate-based blood group antigens, wherein microbes can envelope themselves in blood group structures similar to human cells. In this study, we demonstrate that the innate immune lectin, galectin-4 (Gal-4), exhibits strain-specific binding and killing behavior towards microbes that display blood group-like antigens. Examination of binding preferences using a combination of microarrays populated with ABO(H) glycans and a variety of microbial strains, including those that express blood group-like antigens, demonstrated that Gal-4 binds mammalian and microbial antigens that have features of blood group and mammalian-like structures. Although Gal-4 was thought to exist as a monomer that achieves functional bivalency through its two linked carbohydrate recognition domains, our data demonstrate that Gal-4 forms dimers and that differences in the intrinsic ability of each domain to dimerize likely influences binding affinity. While each Gal-4 domain exhibited blood group-binding activity, the C-terminal domain (Gal-4C) exhibited dimeric properties, while the N-terminal domain (Gal-4N) failed to similarly display dimeric activity. Gal-4C not only exhibited the ability to dimerize but also possessed higher affinity toward ABO(H) blood group antigens and microbes expressing glycans with blood group-like features. Furthermore, when compared to Gal-4N, Gal-4C exhibited more potent antimicrobial activity. Even in the context of the full-length protein, where Gal-4N is functionally bivalent by virtue of Gal-4C dimerization, Gal-4C continued to display higher antimicrobial activity. These results demonstrate that Gal-4 exists as a dimer and exhibits its antimicrobial activity primarily through its C-terminal domain. In doing so, these data provide important insight into key features of Gal-4 responsible for its innate immune activity against molecular mimicry., Competing Interests: Conflict of interest The authors declare no competing interests., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)
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- 2024
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12. Enteric glia regulate Paneth cell secretion and intestinal microbial ecology.
- Author
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Prochera A, Muppirala AN, Kuziel GA, Soualhi S, Shepherd A, Sun L, Issac B, Rosenberg HJ, Karim F, Perez K, Smith KH, Archibald TH, Rakoff-Nahoum S, Hagen SJ, and Rao M
- Abstract
Glial cells of the enteric nervous system (ENS) interact closely with the intestinal epithelium and secrete signals that influence epithelial cell proliferation and barrier formation in vitro . Whether these interactions are important in vivo, however, is unclear because previous studies reached conflicting conclusions [1]. To better define the roles of enteric glia in steady state regulation of the intestinal epithelium, we characterized the glia in closest proximity to epithelial cells and found that the majority express PLP1 in both mice and humans. To test their functions using an unbiased approach, we genetically depleted PLP1
+ cells in mice and transcriptionally profiled the small and large intestines. Surprisingly, glial loss had minimal effects on transcriptional programs and the few identified changes varied along the gastrointestinal tract. In the ileum, where enteric glia had been considered most essential for epithelial integrity, glial depletion did not drastically alter epithelial gene expression but caused a modest enrichment in signatures of Paneth cells, a secretory cell type important for innate immunity. In the absence of PLP1+ glia, Paneth cell number was intact, but a subset appeared abnormal with irregular and heterogenous cytoplasmic granules, suggesting a secretory deficit. Consistent with this possibility, ileal explants from glial-depleted mice secreted less functional lysozyme than controls with corresponding effects on fecal microbial composition. Collectively, these data suggest that enteric glia do not exert broad effects on the intestinal epithelium but have an essential role in regulating Paneth cell function and gut microbial ecology.- Published
- 2024
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13. Stress Ulcer Prophylaxis Versus Placebo-A Blinded Pilot Randomized Controlled Trial to Evaluate the Safety of Two Strategies in Critically Ill Infants With Congenital Heart Disease.
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Mills KI, Albert BD, Bechard LJ, Chu S, Duggan CP, Kaza A, Rakoff-Nahoum S, Sleeper LA, Newburger JW, Priebe GP, and Mehta NM
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- Humans, Critical Illness therapy, Gastrointestinal Hemorrhage prevention & control, Pilot Projects, Treatment Outcome, Ulcer complications, Infant, Heart Defects, Congenital complications, Peptic Ulcer prevention & control
- Abstract
Objectives: The routine use of stress ulcer prophylaxis (SUP) in infants with congenital heart disease (CHD) in the cardiac ICU (CICU) is controversial. We aimed to conduct a pilot study to explore the feasibility of performing a subsequent larger trial to assess the safety and efficacy of withholding SUP in this population (NCT03667703)., Design, Setting, Patients: Single-center, prospective, double-blinded, parallel group (SUP vs. placebo), pilot randomized controlled pilot trial (RCT) in infants with CHD admitted to the CICU and anticipated to require respiratory support for greater than 24 hours., Interventions: Patients were randomized 1:1 (stratified by age and admission type) to receive a histamine-2 receptor antagonist or placebo until respiratory support was discontinued, up to 14 days, or transfer from the CICU, if earlier., Measurements and Main Results: Feasibility was defined a priori by thresholds of screening rate, consent rate, timely drug allocation, and protocol adherence. The safety outcome was the rate of clinically significant upper gastrointestinal (UGI) bleeding. We screened 1,426 patients from February 2019 to March 2022; of 132 eligible patients, we gained informed consent in 70 (53%). Two patients did not require CICU admission after obtaining consent, and the remaining 68 patients were randomized to SUP (n = 34) or placebo (n = 34). Ten patients were withdrawn early, because of a change in eligibility (n = 3) or open-label SUP use (n = 7, 10%). Study procedures were completed in 58 patients (89% protocol adherence). All feasibility criteria were met. There were no clinically significant episodes of UGI bleeding during the pilot RCT. The percentage of patients with other nonserious adverse events did not differ between groups., Conclusions: Withholding of SUP in infants with CHD admitted to the CICU was feasible. A larger multicenter RCT designed to confirm the safety of this intervention and its impact on incidence of UGI bleeding, gastrointestinal microbiome, and other clinical outcomes is warranted., Competing Interests: Dr. Mills’ institution received funding from The Gerber Foundation. Dr. Duggan’s institution received funding from Takeda; he received funding from UpToDate. Drs. Duggan and Mehta received support for article research from the National Institutes of Health. Dr. Sleeper received funding from The Gerber Foundation and Tenaya Therapeutics. Dr. Newburger received funding from Pfizer, Daiichii-Sankyo, Bristol-Myer-Squibb, Novartis, and UpToDate. Dr. Priebe’s institution received funding from The Gerber Foundation’s National Research Grant (#5781) and the U.S. Department of Defense (grant # PR181874 and W81XWH-19-1-0208); he disclosed the off-label product use of famotidine and ranitidine. The remaining authors have disclosed that they do not have any potential conflicts of interest., (Copyright © 2023 by the Society of Critical Care Medicine and the World Federation of Pediatric Intensive and Critical Care Societies.)
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- 2024
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14. C. difficile intoxicates neurons and pericytes to drive neurogenic inflammation.
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Manion J, Musser MA, Kuziel GA, Liu M, Shepherd A, Wang S, Lee PG, Zhao L, Zhang J, Marreddy RKR, Goldsmith JD, Yuan K, Hurdle JG, Gerhard R, Jin R, Rakoff-Nahoum S, Rao M, and Dong M
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- Animals, Mice, Calcitonin Gene-Related Peptide antagonists & inhibitors, Calcitonin Gene-Related Peptide metabolism, Clostridium Infections microbiology, Receptors, Neurokinin-1 metabolism, Substance P antagonists & inhibitors, Substance P metabolism, Inflammation Mediators metabolism, Cecum drug effects, Cecum metabolism, Signal Transduction drug effects, Bacterial Toxins administration & dosage, Bacterial Toxins pharmacology, Clostridioides difficile pathogenicity, Neurogenic Inflammation chemically induced, Neurogenic Inflammation microbiology, Neurogenic Inflammation pathology, Pericytes drug effects, Pericytes microbiology, Pericytes pathology, Neurons, Afferent drug effects, Neurons, Afferent microbiology, Neurons, Afferent pathology
- Abstract
Clostridioides difficile infection (CDI) is a major cause of healthcare-associated gastrointestinal infections
1,2 . The exaggerated colonic inflammation caused by C. difficile toxins such as toxin B (TcdB) damages tissues and promotes C. difficile colonization3-6 , but how TcdB causes inflammation is unclear. Here we report that TcdB induces neurogenic inflammation by targeting gut-innervating afferent neurons and pericytes through receptors, including the Frizzled receptors (FZD1, FZD2 and FZD7) in neurons and chondroitin sulfate proteoglycan 4 (CSPG4) in pericytes. TcdB stimulates the secretion of the neuropeptides substance P (SP) and calcitonin gene-related peptide (CGRP) from neurons and pro-inflammatory cytokines from pericytes. Targeted delivery of the TcdB enzymatic domain, through fusion with a detoxified diphtheria toxin, into peptidergic sensory neurons that express exogeneous diphtheria toxin receptor (an approach we term toxogenetics) is sufficient to induce neurogenic inflammation and recapitulates major colonic histopathology associated with CDI. Conversely, mice lacking SP, CGRP or the SP receptor (neurokinin 1 receptor) show reduced pathology in both models of caecal TcdB injection and CDI. Blocking SP or CGRP signalling reduces tissue damage and C. difficile burden in mice infected with a standard C. difficile strain or with hypervirulent strains expressing the TcdB2 variant. Thus, targeting neurogenic inflammation provides a host-oriented therapeutic approach for treating CDI., (© 2023. The Author(s), under exclusive licence to Springer Nature Limited.)- Published
- 2023
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15. Bacterial amylases enable glycogen degradation by the vaginal microbiome.
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Jenkins DJ, Woolston BM, Hood-Pishchany MI, Pelayo P, Konopaski AN, Quinn Peters M, France MT, Ravel J, Mitchell CM, Rakoff-Nahoum S, Whidbey C, and Balskus EP
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- Female, Humans, Vagina microbiology, Bacteria genetics, Bacteria metabolism, Glycogen metabolism, Amylases, Microbiota physiology
- Abstract
The human vaginal microbiota is frequently dominated by lactobacilli and transition to a more diverse community of anaerobic microbes is associated with health risks. Glycogen released by lysed epithelial cells is believed to be an important nutrient source in the vagina. However, the mechanism by which vaginal bacteria metabolize glycogen is unclear, with evidence implicating both bacterial and human enzymes. Here we biochemically characterize six glycogen-degrading enzymes (GDEs), all of which are pullanases (PulA homologues), from vaginal bacteria that support the growth of amylase-deficient Lactobacillus crispatus on glycogen. We reveal variations in their pH tolerance, substrate preferences, breakdown products and susceptibility to inhibition. Analysis of vaginal microbiome datasets shows that these enzymes are expressed in all community state types. Finally, we confirm the presence and activity of bacterial and human GDEs in cervicovaginal fluid. This work establishes that bacterial GDEs can participate in the breakdown of glycogen, providing insight into metabolism that may shape the vaginal microbiota., (© 2023. The Author(s).)
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- 2023
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16. Blood group A enhances SARS-CoV-2 infection.
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Wu SC, Arthur CM, Jan HM, Garcia-Beltran WF, Patel KR, Rathgeber MF, Verkerke HP, Cheedarla N, Jajosky RP, Paul A, Neish AS, Roback JD, Josephson CD, Wesemann DR, Kalman D, Rakoff-Nahoum S, Cummings RD, and Stowell SR
- Subjects
- Humans, SARS-CoV-2, ABO Blood-Group System, Galectins, COVID-19
- Abstract
Among the risk factors for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), ABO(H) blood group antigens are among the most recognized predictors of infection. However, the mechanisms by which ABO(H) antigens influence susceptibility to COVID-19 remain incompletely understood. The receptor-binding domain (RBD) of SARS-CoV-2, which facilitates host cell engagement, bears significant similarity to galectins, an ancient family of carbohydrate-binding proteins. Because ABO(H) blood group antigens are carbohydrates, we compared the glycan-binding specificity of SARS-CoV-2 RBD with that of galectins. Similar to the binding profile of several galectins, the RBDs of SARS-CoV-2, including Delta and Omicron variants, exhibited specificity for blood group A. Not only did each RBD recognize blood group A in a glycan array format, but each SARS-CoV-2 virus also displayed a preferential ability to infect blood group A-expressing cells. Preincubation of blood group A cells with a blood group-binding galectin specifically inhibited the blood group A enhancement of SARS-CoV-2 infection, whereas similar incubation with a galectin that does not recognize blood group antigens failed to impact SARS-CoV-2 infection. These results demonstrated that SARS-CoV-2 can engage blood group A, providing a direct link between ABO(H) blood group expression and SARS-CoV-2 infection., (© 2023 by The American Society of Hematology.)
- Published
- 2023
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17. Vaginal microbiome-host interactions modeled in a human vagina-on-a-chip.
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Mahajan G, Doherty E, To T, Sutherland A, Grant J, Junaid A, Gulati A, LoGrande N, Izadifar Z, Timilsina SS, Horváth V, Plebani R, France M, Hood-Pishchany I, Rakoff-Nahoum S, Kwon DS, Goyal G, Prantil-Baun R, Ravel J, and Ingber DE
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- Female, Pregnancy, Humans, Lab-On-A-Chip Devices, Vagina, Cytokines, Microbiota, Vaginosis, Bacterial
- Abstract
Background: A dominance of non-iners Lactobacillus species in the vaginal microbiome is optimal and strongly associated with gynecological and obstetric health, while the presence of diverse obligate or facultative anaerobic bacteria and a paucity in Lactobacillus species, similar to communities found in bacterial vaginosis (BV), is considered non-optimal and associated with adverse health outcomes. Various therapeutic strategies are being explored to modulate the composition of the vaginal microbiome; however, there is no human model that faithfully reproduces the vaginal epithelial microenvironment for preclinical validation of potential therapeutics or testing hypotheses about vaginal epithelium-microbiome interactions., Results: Here, we describe an organ-on-a-chip (organ chip) microfluidic culture model of the human vaginal mucosa (vagina chip) that is lined by hormone-sensitive, primary vaginal epithelium interfaced with underlying stromal fibroblasts, which sustains a low physiological oxygen concentration in the epithelial lumen. We show that the Vagina Chip can be used to assess colonization by optimal L. crispatus consortia as well as non-optimal Gardnerella vaginalis-containing consortia, and to measure associated host innate immune responses. Co-culture and growth of the L. crispatus consortia on-chip was accompanied by maintenance of epithelial cell viability, accumulation of D- and L-lactic acid, maintenance of a physiologically relevant low pH, and down regulation of proinflammatory cytokines. In contrast, co-culture of G. vaginalis-containing consortia in the vagina chip resulted in epithelial cell injury, a rise in pH, and upregulation of proinflammatory cytokines., Conclusion: This study demonstrates the potential of applying human organ chip technology to create a preclinical model of the human vaginal mucosa that can be used to better understand interactions between the vaginal microbiome and host tissues, as well as to evaluate the safety and efficacy of live biotherapeutics products. Video Abstract., (© 2022. The Author(s).)
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- 2022
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18. Innate immune Galectin-7 specifically targets microbes that decorate themselves in blood group-like antigens.
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Wu SC, Kamili NA, Dias-Baruffi M, Josephson CD, Rathgeber MF, Yeung MY, Lane WJ, Wang J, Jan HM, Rakoff-Nahoum S, Cummings RD, Stowell SR, and Arthur CM
- Abstract
Adaptive immunity can target a nearly infinite range of antigens, yet it is tempered by tolerogenic mechanisms that limit autoimmunity. Such immunological tolerance, however, creates a gap in adaptive immunity against microbes decorated with self-like antigens as a form of molecular mimicry. Our results demonstrate that the innate immune lectin galectin-7 (Gal-7) binds a variety of distinct microbes, all of which share features of blood group-like antigens. Gal-7 binding to each blood group expressing microbe, including strains of Escherichia coli , Klebsiella pneumoniae , Providencia alcalifaciens, and Streptococcus pneumoniae , results in loss of microbial viability. Although Gal-7 also binds red blood cells (RBCs), this interaction does not alter RBC membrane integrity. These results demonstrate that Gal-7 recognizes a diverse range of microbes, each of which use molecular mimicry while failing to induce host cell injury, and thus may provide an innate form of immunity against molecular mimicry., Competing Interests: The authors declare no competing interests., (© 2022 The Author(s).)
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- 2022
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19. The gut microbiome.
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Kuziel GA and Rakoff-Nahoum S
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- Animals, Bacteria, Mammals, Gastrointestinal Microbiome physiology, Microbiota
- Abstract
All animals, from cnidarians to humans, are colonized with microbes, and the greatest diversity and magnitude of these host-associated microorganisms resides within the intestine. Referred to as the gut microbiome, membership can be as simple as one species of bacteria or can be composed of hundreds to thousands of different microbes across the domains of life. The relationship between the gut microbiome and host span from beneficial to detrimental; interactions may be context-dependent and occur across host physiology and organ systems. In this Primer, we focus on the mammalian host to discuss basic mechanisms by which the gut microbiome impacts the host and review mechanisms by which hosts and the environment shape the microbiome. We end by highlighting key concepts and discussing future directions for the field that will be critical for generating the next generation of knowledge of the gut microbiome., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2022 Elsevier Inc. All rights reserved.)
- Published
- 2022
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20. Strain-level fitness in the gut microbiome is an emergent property of glycans and a single metabolite.
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Park SY, Rao C, Coyte KZ, Kuziel GA, Zhang Y, Huang W, Franzosa EA, Weng JK, Huttenhower C, and Rakoff-Nahoum S
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- Acyl Coenzyme A metabolism, Amino Acid Sequence, Amino Acids, Branched-Chain metabolism, Bacteroidetes drug effects, Bacteroidetes genetics, Bacteroidetes growth & development, Butyrates chemistry, Butyrates pharmacology, Coenzyme A-Transferases chemistry, Coenzyme A-Transferases metabolism, Genetic Variation drug effects, Hydrogen-Ion Concentration, Polymorphism, Single Nucleotide genetics, Promoter Regions, Genetic genetics, Species Specificity, Stress, Physiological drug effects, Stress, Physiological genetics, Transcription, Genetic drug effects, Gastrointestinal Microbiome drug effects, Gastrointestinal Microbiome genetics, Metabolome drug effects, Metabolome genetics, Polysaccharides metabolism
- Abstract
The human gut microbiota resides within a diverse chemical environment challenging our ability to understand the forces shaping this ecosystem. Here, we reveal that fitness of the Bacteroidales, the dominant order of bacteria in the human gut, is an emergent property of glycans and one specific metabolite, butyrate. Distinct sugars serve as strain-variable fitness switches activating context-dependent inhibitory functions of butyrate. Differential fitness effects of butyrate within the Bacteroides are mediated by species-level variation in Acyl-CoA thioesterase activity and nucleotide polymorphisms regulating an Acyl-CoA transferase. Using in vivo multi-omic profiles, we demonstrate Bacteroides fitness in the human gut is associated together, but not independently, with Acyl-CoA transferase expression and butyrate. Our data reveal that each strain of the Bacteroides exists within a unique fitness landscape based on the interaction of chemical components unpredictable by the effect of each part alone mediated by flexibility in the core genome., Competing Interests: Declaration of interests J.K.W. is a member of the SAB and a shareholder of DoubleRainbow Biosciences, Galixir, and Inari Agriculture. The other authors declare no competing interests., (Copyright © 2022 Elsevier Inc. All rights reserved.)
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- 2022
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21. Multi-kingdom ecological drivers of microbiota assembly in preterm infants.
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Rao C, Coyte KZ, Bainter W, Geha RS, Martin CR, and Rakoff-Nahoum S
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- Bacterial Load, Diet, Female, Gestational Age, Humans, Infant, Infant, Newborn, Male, Microbial Interactions, Reproducibility of Results, Biodiversity, Gastrointestinal Microbiome, Infant, Premature
- Abstract
The gut microbiota of preterm infants develops predictably
1-7 , with pioneer species colonizing the gut after birth, followed by an ordered succession of microorganisms. The gut microbiota is vital to the health of preterm infants8,9 , but the forces that shape these predictable dynamics of microbiome assembly are unknown. The environment, the host and interactions between microorganisms all potentially shape the dynamics of the microbiota, but in such a complex ecosystem, identifying the specific role of any individual factor is challenging10-14 . Here we use multi-kingdom absolute abundance quantification, ecological modelling and experimental validation to address this challenge. We quantify the absolute dynamics of bacteria, fungi and archaea in a longitudinal cohort of 178 preterm infants. We uncover microbial blooms and extinctions, and show that there is an inverse correlation between bacterial and fungal loads in the infant gut. We infer computationally and demonstrate experimentally in vitro and in vivo that predictable assembly dynamics may be driven by directed, context-dependent interactions between specific microorganisms. Mirroring the dynamics of macroscopic ecosystems15-17 , a late-arriving member of the microbiome, Klebsiella, exploits the pioneer microorganism, Staphylococcus, to gain a foothold within the gut. Notably, we find that interactions between different kingdoms can influence assembly, with a single fungal species-Candida albicans-inhibiting multiple dominant genera of gut bacteria. Our work reveals the centrality of simple microbe-microbe interactions in shaping host-associated microbiota, which is critical both for our understanding of microbiota ecology and for targeted microbiota interventions.- Published
- 2021
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22. Ecological rules for the assembly of microbiome communities.
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Coyte KZ, Rao C, Rakoff-Nahoum S, and Foster KR
- Subjects
- Humans, Infant, Newborn, Milk, Human microbiology, Models, Theoretical, Symbiosis, Infant, Premature, Microbiota
- Abstract
Humans and many other hosts establish a diverse community of beneficial microbes anew each generation. The order and identity of incoming symbionts is critical for health, but what determines the success of the assembly process remains poorly understood. Here we develop ecological theory to identify factors important for microbial community assembly. Our method maps out all feasible pathways for the assembly of a given microbiome-with analogies to the mutational maps underlying fitness landscapes in evolutionary biology. Building these "assembly maps" reveals a tradeoff at the heart of the assembly process. Ecological dependencies between members of the microbiota make assembly predictable-and can provide metabolic benefits to the host-but these dependencies may also create barriers to assembly. This effect occurs because interdependent species can fail to establish when each relies on the other to colonize first. We support our predictions with published data from the assembly of the preterm infant microbiota, where we find that ecological dependence is associated with a predictable order of arrival. Our models also suggest that hosts can overcome barriers to assembly via mechanisms that either promote the uptake of multiple symbiont species in one step or feed early colonizers. This predicted importance of host feeding is supported by published data on the impacts of breast milk in the assembly of the human microbiome. We conclude that both microbe to microbe and host to microbe interactions are important for the trajectory of microbiome assembly., Competing Interests: The authors have declared that no competing interests exist.
- Published
- 2021
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23. Combined immunodeficiency due to a mutation in the γ1 subunit of the coat protein I complex.
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Bainter W, Platt CD, Park SY, Stafstrom K, Wallace JG, Peters ZT, Massaad MJ, Becuwe M, Salinas SA, Jones J, Beaussant-Cohen S, Jaber F, Yang JS, Walther TC, Orange JS, Rao C, Rakoff-Nahoum S, Tsokos M, Naseem SUR, Al-Tamemi S, Chou J, Hsu VW, and Geha RS
- Subjects
- Amino Acid Substitution, Animals, Apoptosis genetics, Coatomer Protein genetics, Endoplasmic Reticulum genetics, Endoplasmic Reticulum immunology, Endoplasmic Reticulum Stress genetics, Golgi Apparatus genetics, Golgi Apparatus immunology, Humans, Mice, Mice, Mutant Strains, Receptors, Peptide genetics, Receptors, Peptide immunology, Severe Combined Immunodeficiency genetics, Apoptosis immunology, B-Lymphocytes immunology, Endoplasmic Reticulum Stress immunology, Lymphocyte Activation, Mutation, Missense, Severe Combined Immunodeficiency immunology, T-Lymphocytes immunology
- Abstract
The coat protein I (COPI) complex mediates retrograde trafficking from the Golgi to the endoplasmic reticulum (ER). Five siblings with persistent bacterial and viral infections and defective humoral and cellular immunity had a homozygous p.K652E mutation in the γ1 subunit of COPI (γ1-COP). The mutation disrupts COPI binding to the KDEL receptor and impairs the retrieval of KDEL-bearing chaperones from the Golgi to the ER. Homozygous Copg1K652E mice had increased ER stress in activated T and B cells, poor antibody responses, and normal numbers of T cells that proliferated normally, but underwent increased apoptosis upon activation. Exposure of the mutants to pet store mice caused weight loss, lymphopenia, and defective T cell proliferation that recapitulated the findings in the patients. The ER stress-relieving agent tauroursodeoxycholic acid corrected the immune defects of the mutants and reversed the phenotype they acquired following exposure to pet store mice. This study establishes the role of γ1-COP in the ER retrieval of KDEL-bearing chaperones and thereby the importance of ER homeostasis in adaptive immunity.
- Published
- 2021
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24. Stress ulcer prophylaxis versus placebo-a blinded randomized control trial to evaluate the safety of two strategies in critically ill infants with congenital heart disease (SUPPRESS-CHD).
- Author
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Mills KI, Albert BD, Bechard LJ, Duggan CP, Kaza A, Rakoff-Nahoum S, Vlamakis H, Sleeper LA, Newburger JW, Priebe GP, and Mehta NM
- Subjects
- Anti-Ulcer Agents adverse effects, Critical Illness, Cross Infection etiology, Double-Blind Method, Enterocolitis, Pseudomembranous etiology, Gastrointestinal Hemorrhage mortality, Histamine H2 Antagonists adverse effects, Humans, Infant, Intensive Care Units, Peptic Ulcer etiology, Peptic Ulcer mortality, Pilot Projects, Pneumonia etiology, Prospective Studies, Randomized Controlled Trials as Topic, Anti-Ulcer Agents administration & dosage, Gastrointestinal Hemorrhage prevention & control, Heart Defects, Congenital complications, Histamine H2 Antagonists administration & dosage, Peptic Ulcer prevention & control
- Abstract
Background: Critically ill infants with congenital heart disease (CHD) are often prescribed stress ulcer prophylaxis (SUP) to prevent upper gastrointestinal bleeding, despite the low incidence of stress ulcers and limited data on the safety and efficacy of SUP in infants. Recently, SUP has been associated with an increased incidence of hospital-acquired infections, community-acquired pneumonia, and necrotizing enterocolitis. The objective of this pilot study is to investigate the feasibility of performing a randomized controlled trial to assess the safety and efficacy of withholding SUP in infants with congenital heart disease admitted to the cardiac intensive care unit., Methods: A single center, prospective, double-blinded, randomized placebo-controlled pilot feasibility trial will be performed in infants with CHD admitted to the cardiac intensive care unit and anticipated to require respiratory support for > 24 h. Patients will be randomized to receive a histamine-2 receptor antagonist (H2RA) or placebo until they are discontinued from respiratory support. Randomization will be performed within 2 strata defined by admission type (medical or surgical) and age (neonate, age < 30 days, or infant, 1 month to 1 year). Allocation will be a 1:1 ratio using permuted blocks to ensure balanced allocations across the two treatment groups within each stratum. The primary outcomes include feasibility of screening, consent, timely allocation of study drug, and protocol adherence. The primary safety outcome is the rate of clinically significant upper gastrointestinal bleeding. The secondary outcomes are the difference in the relative and absolute abundance of the gut microbiota and functional microbial profiles between the two study groups. We plan to enroll 100 patients in this pilot study., Discussion: Routine use of SUP to prevent upper gastrointestinal bleeding in infants is controversial due to a low incidence of bleeding events and concern for adverse effects. The role of SUP in infants with CHD has not been examined, and there is equipoise on the risks and benefits of withholding this therapy. In addition, this therapy has been discontinued in other neonatal populations due to the concern for hospital-acquired infections and necrotizing enterocolitis. Furthermore, exploring changes to the microbiome after exposure to SUP may highlight the mechanisms by which SUP impacts potential microbial dysbiosis of the gut and its association with hospital-acquired infections. Assessment of the feasibility of a trial of withholding SUP in critically ill infants with CHD will facilitate planning of a larger multicenter trial of safety and efficacy of SUP in this vulnerable population., Trial Registration: ClinicalTrials.gov , NCT03667703. Registered 12 September 2018, https://clinicaltrials.gov/ct2/show/NCT03667703?term=SUPPRESS+CHD&draw=2&rank=1 . All WHO Trial Registration Data Set Criteria are met in this manuscript.
- Published
- 2020
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25. Distribution and storage of inflammatory memory in barrier tissues.
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Ordovas-Montanes J, Beyaz S, Rakoff-Nahoum S, and Shalek AK
- Subjects
- Adaptive Immunity, Cell Lineage, Dendritic Cells immunology, Humans, Immunity, Innate, Neurons immunology, Plasma Cells immunology, Stromal Cells immunology, B-Lymphocytes immunology, Epithelial Cells immunology, Epithelium immunology, Immunologic Memory immunology, Inflammation immunology, Macrophages immunology, T-Lymphocytes immunology
- Abstract
Memories of previous immune events enable barrier tissues to rapidly recall distinct environmental exposures. To effectively inform future responses, these past experiences can be stored in cell types that are long-term residents or essential constituents of tissues. There is an emerging understanding that, in addition to antigen-specific immune cells, diverse haematopoietic, stromal, parenchymal and neuronal cell types can store inflammatory memory. Here, we explore the impact of previous immune activity on various cell lineages with the goal of presenting a unified view of inflammatory memory to environmental exposures (such as allergens, antigens, noxious agents and microorganisms) at barrier tissues. We propose that inflammatory memory is distributed across diverse cell types and stored through shifts in cell states, and we provide a framework to guide future experiments. This distribution and storage may promote adaptation or maladaptation in homeostatic, maintenance and disease settings - especially if the distribution of memory favours cellular cooperation during storage or recall.
- Published
- 2020
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26. Understanding Competition and Cooperation within the Mammalian Gut Microbiome.
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Coyte KZ and Rakoff-Nahoum S
- Subjects
- Animals, Gastrointestinal Microbiome, Mammals microbiology, Microbial Interactions
- Abstract
The mammalian gut harbors a vast community of microorganisms - termed the microbiota - whose composition and dynamics are considered to be critical drivers of host health. These factors depend, in part, upon the manner in which microbes interact with one another. Microbes are known to engage in a myriad of different ways, ranging from unprovoked aggression to actively feeding each other. However, the relative extent to which these different interactions occur between microbes within the gut is unclear. In this minireview we assess our current knowledge of microbe-microbe interactions within the mammalian gut microbiota, and the array of methods used to uncover them. In particular, we highlight the discrepancies between different methodologies: some studies have revealed rich networks of cross-feeding interactions between microbes, whereas others suggest that microbes are more typically locked in conflict and actively cooperate only rarely. We argue that to reconcile these contradictions we must recognize that interactions between members of the microbiota can vary across condition, space, and time - and that only through embracing this dynamism will we be able to comprehensively understand the ecology of our gut communities., (Copyright © 2019. Published by Elsevier Ltd.)
- Published
- 2019
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27. Harnessing single-cell genomics to improve the physiological fidelity of organoid-derived cell types.
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Mead BE, Ordovas-Montanes J, Braun AP, Levy LE, Bhargava P, Szucs MJ, Ammendolia DA, MacMullan MA, Yin X, Hughes TK, Wadsworth MH 2nd, Ahmad R, Rakoff-Nahoum S, Carr SA, Langer R, Collins JJ, Shalek AK, and Karp JM
- Subjects
- Humans, Models, Biological, Proteomics, Sequence Analysis, RNA, Stem Cell Niche, Genomics methods, Organoids cytology, Paneth Cells cytology, Single-Cell Analysis methods
- Abstract
Background: Single-cell genomic methods now provide unprecedented resolution for characterizing the component cell types and states of tissues such as the epithelial subsets of the gastrointestinal tract. Nevertheless, functional studies of these subsets at scale require faithful in vitro models of identified in vivo biology. While intestinal organoids have been invaluable in providing mechanistic insights in vitro, the extent to which organoid-derived cell types recapitulate their in vivo counterparts remains formally untested, with no systematic approach for improving model fidelity., Results: Here, we present a generally applicable framework that utilizes massively parallel single-cell RNA-seq to compare cell types and states found in vivo to those of in vitro models such as organoids. Furthermore, we leverage identified discrepancies to improve model fidelity. Using the Paneth cell (PC), which supports the stem cell niche and produces the largest diversity of antimicrobials in the small intestine, as an exemplar, we uncover fundamental gene expression differences in lineage-defining genes between in vivo PCs and those of the current in vitro organoid model. With this information, we nominate a molecular intervention to rationally improve the physiological fidelity of our in vitro PCs. We then perform transcriptomic, cytometric, morphologic and proteomic characterization, and demonstrate functional (antimicrobial activity, niche support) improvements in PC physiology., Conclusions: Our systematic approach provides a simple workflow for identifying the limitations of in vitro models and enhancing their physiological fidelity. Using adult stem cell-derived PCs within intestinal organoids as a model system, we successfully benchmark organoid representation, relative to that in vivo, of a specialized cell type and use this comparison to generate a functionally improved in vitro PC population. We predict that the generation of rationally improved cellular models will facilitate mechanistic exploration of specific disease-associated genes in their respective cell types.
- Published
- 2018
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28. The evolution of the host microbiome as an ecosystem on a leash.
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Foster KR, Schluter J, Coyte KZ, and Rakoff-Nahoum S
- Subjects
- Animals, Biodiversity, Health, Humans, Microbial Interactions drug effects, Microbial Interactions immunology, Microbiota drug effects, Microbiota immunology, Species Specificity, Symbiosis drug effects, Symbiosis immunology, Biological Evolution, Ecosystem, Microbial Interactions physiology, Microbiota physiology, Models, Biological, Symbiosis physiology
- Abstract
The human body carries vast communities of microbes that provide many benefits. Our microbiome is complex and challenging to understand, but evolutionary theory provides a universal framework with which to analyse its biology and health impacts. Here we argue that to understand a given microbiome feature, such as colonization resistance, host nutrition or immune development, we must consider how hosts and symbionts evolve. Symbionts commonly evolve to compete within the host ecosystem, while hosts evolve to keep the ecosystem on a leash. We suggest that the health benefits of the microbiome should be understood, and studied, as an interplay between microbial competition and host control.
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- 2017
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29. Interplay between microbial d-amino acids and host d-amino acid oxidase modifies murine mucosal defence and gut microbiota.
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Sasabe J, Miyoshi Y, Rakoff-Nahoum S, Zhang T, Mita M, Davis BM, Hamase K, and Waldor MK
- Subjects
- Amino Acids biosynthesis, Amino Acids chemistry, Animals, Bacteria genetics, Bacteria growth & development, D-Amino-Acid Oxidase biosynthesis, D-Amino-Acid Oxidase deficiency, D-Amino-Acid Oxidase genetics, Goblet Cells enzymology, Homeostasis, Humans, Hydrogen Peroxide metabolism, Immunoglobulin A, Secretory analysis, Intestinal Mucosa cytology, Intestinal Mucosa immunology, Intestines cytology, Intestines enzymology, Mice, RNA, Ribosomal, 16S, Vibrio cholerae growth & development, Vibrio cholerae metabolism, Amino Acids metabolism, Bacteria metabolism, D-Amino-Acid Oxidase metabolism, Gastrointestinal Microbiome immunology, Host-Pathogen Interactions, Immunity, Mucosal, Intestinal Mucosa enzymology
- Abstract
L-Amino acids are the building blocks for proteins synthesized in ribosomes in all kingdoms of life, but d-amino acids (d-aa) have important non-ribosome-based functions(1). Mammals synthesize d-Ser and d-Asp, primarily in the central nervous system, where d-Ser is critical for neurotransmission(2). Bacteria synthesize a largely distinct set of d-aa, which become integral components of the cell wall and are also released as free d-aa(3,4). However, the impact of free microbial d-aa on host physiology at the host-microbial interface has not been explored. Here, we show that the mouse intestine is rich in free d-aa that are derived from the microbiota. Furthermore, the microbiota induces production of d-amino acid oxidase (DAO) by intestinal epithelial cells, including goblet cells, which secrete the enzyme into the lumen. Oxidative deamination of intestinal d-aa by DAO, which yields the antimicrobial product H2O2, protects the mucosal surface in the small intestine from the cholera pathogen. DAO also modifies the composition of the microbiota and is associated with microbial induction of intestinal sIgA. Collectively, these results identify d-aa and DAO as previously unrecognized mediators of microbe-host interplay and homeostasis on the epithelial surface of the small intestine., Competing Interests: The authors declare no competing financial interests.
- Published
- 2016
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30. The evolution of cooperation within the gut microbiota.
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Rakoff-Nahoum S, Foster KR, and Comstock LE
- Subjects
- Animals, Bacteroides enzymology, Bacteroides genetics, Dietary Carbohydrates metabolism, Germ-Free Life, Glycoside Hydrolases metabolism, Humans, In Vitro Techniques, Intestines microbiology, Inulin metabolism, Male, Mice, Bacteroides physiology, Biological Evolution, Gastrointestinal Microbiome physiology, Symbiosis
- Abstract
Cooperative phenotypes are considered central to the functioning of microbial communities in many contexts, including communication via quorum sensing, biofilm formation, antibiotic resistance, and pathogenesis. The human intestine houses a dense and diverse microbial community critical to health, yet we know little about cooperation within this important ecosystem. Here we test experimentally for evolved cooperation within the Bacteroidales, the dominant Gram-negative bacteria of the human intestine. We show that during growth on certain dietary polysaccharides, the model member Bacteroides thetaiotaomicron exhibits only limited cooperation. Although this organism digests these polysaccharides extracellularly, mutants lacking this ability are outcompeted. In contrast, we discovered a dedicated cross-feeding enzyme system in the prominent gut symbiont Bacteroides ovatus, which digests polysaccharide at a cost to itself but at a benefit to another species. Using in vitro systems and gnotobiotic mouse colonization models, we find that extracellular digestion of inulin increases the fitness of B. ovatus owing to reciprocal benefits when it feeds other gut species such as Bacteroides vulgatus. This is a rare example of naturally-evolved cooperation between microbial species. Our study reveals both the complexity and importance of cooperative phenotypes within the mammalian intestinal microbiota.
- Published
- 2016
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31. Another Reason to Thank Mom: Gestational Effects of Microbiota Metabolites.
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Rakoff-Nahoum S
- Subjects
- Animals, Female, Pregnancy, Gastrointestinal Microbiome immunology, Immune System growth & development, Immune System microbiology, Immunity, Innate immunology, Immunity, Maternally-Acquired immunology, Intestines immunology
- Abstract
Microbial colonization after birth profoundly affects development of the host. In a recent paper, Gomez de Agüero et al. (2016) reveal a new aspect of ontogeny influenced by the microbiota: the impact of gestational gut bacterial metabolites on early immune maturation of the neonatal intestine., (Copyright © 2016 Elsevier Inc. All rights reserved.)
- Published
- 2016
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32. Host Selection of Microbiota via Differential Adhesion.
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McLoughlin K, Schluter J, Rakoff-Nahoum S, Smith AL, and Foster KR
- Subjects
- Bacterial Physiological Phenomena, Humans, Bacterial Adhesion, Bacterial Infections metabolism, Bacterial Infections microbiology, Gastrointestinal Microbiome, Host Specificity, Host-Pathogen Interactions, Intestinal Mucosa microbiology
- Abstract
The host epithelium is the critical interface with microbial communities, but the mechanisms by which the host regulates these communities are poorly understood. Here we develop the hypothesis that hosts use differential adhesion to select for and against particular members of their microbiota. We use an established computational, individual-based model to study the impact of host factors that regulate adhesion at the epithelial surface. Our simulations predict that host-mediated adhesion can increase the competitive advantage of microbes and create ecological refugia for slow-growing species. We show how positive selection via adhesion can be transformed into negative selection if the host secretes large quantities of a matrix such as mucus. Our work predicts that adhesion is a powerful mechanism for both positive and negative selection within the microbiota. We discuss molecules-mucus glycans and IgA-that affect microbe adhesion and identify testable predictions of the adhesion-as-selection model., (Copyright © 2016 Elsevier Inc. All rights reserved.)
- Published
- 2016
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33. The Regulation of Immunological Processes by Peripheral Neurons in Homeostasis and Disease.
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Ordovas-Montanes J, Rakoff-Nahoum S, Huang S, Riol-Blanco L, Barreiro O, and von Andrian UH
- Subjects
- Animals, Humans, Immune System cytology, Immune System physiology, Peripheral Nervous System physiology, Signal Transduction, Homeostasis, Neuroimmunomodulation, Neurons metabolism, Peripheral Nervous System immunology, Peripheral Nervous System metabolism
- Abstract
The nervous system and the immune system are the principal sensory interfaces between the internal and external environment. They are responsible for recognizing, integrating, and responding to varied stimuli, and have the capacity to form memories of these encounters leading to learned or 'adaptive' future responses. We review current understanding of the cross-regulation between these systems. The autonomic and somatosensory nervous systems regulate both the development and deployment of immune cells, with broad functions that impact on hematopoiesis as well as on priming, migration, and cytokine production. In turn, specific immune cell subsets contribute to homeostatic neural circuits such as those controlling metabolism, hypertension, and the inflammatory reflex. We examine the contribution of the somatosensory system to autoimmune, autoinflammatory, allergic, and infectious processes in barrier tissues and, in this context, discuss opportunities for therapeutic manipulation of neuro-immune interactions., (Copyright © 2015 Elsevier Ltd. All rights reserved.)
- Published
- 2015
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34. Analysis of gene-environment interactions in postnatal development of the mammalian intestine.
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Rakoff-Nahoum S, Kong Y, Kleinstein SH, Subramanian S, Ahern PP, Gordon JI, and Medzhitov R
- Subjects
- Animals, Computational Biology, Mice, Mice, Knockout, Receptors, Interleukin-1 genetics, Toll-Like Receptors genetics, Gene-Environment Interaction, Intestines growth & development
- Abstract
Unlike mammalian embryogenesis, which takes place in the relatively predictable and stable environment of the uterus, postnatal development can be affected by a multitude of highly variable environmental factors, including diet, exposure to noxious substances, and microorganisms. Microbial colonization of the intestine is thought to play a particularly important role in postnatal development of the gastrointestinal, metabolic, and immune systems. Major changes in environmental exposure occur right after birth, upon weaning, and during pubertal maturation into adulthood. These transitions include dramatic changes in intestinal contents and require appropriate adaptations to meet changes in functional demands. Here, we attempt to both characterize and provide mechanistic insights into postnatal intestinal ontogeny. We investigated changes in global intestinal gene expression through postnatal developmental transitions. We report profound alterations in small and large intestinal transcriptional programs that accompany both weaning and puberty in WT mice. Using myeloid differentiation factor 88 (MyD88)/TIR-domain-containing adapter-inducing interferon-β (TRIF) double knockout littermates, we define the role of toll-like receptors (TLRs) and interleukin (IL)-1 receptor family member signaling in postnatal gene expression programs and select ontogeny-specific phenotypes, such as vascular and smooth muscle development and neonatal epithelial and mast cell homeostasis. Metaanalysis of the effect of the microbiota on intestinal gene expression allowed for mechanistic classification of developmentally regulated genes by TLR/IL-1R (TIR) signaling and/or indigenous microbes. We find that practically every aspect of intestinal physiology is affected by postnatal transitions. Developmental timing, microbial colonization, and TIR signaling seem to play distinct and specific roles in regulation of gene-expression programs throughout postnatal development.
- Published
- 2015
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35. Immunology: Starve a fever, feed the microbiota.
- Author
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Rakoff-Nahoum S and Comstock LE
- Subjects
- Animals, Female, Male, Disease, Epithelium metabolism, Epithelium microbiology, Fucose metabolism, Intestine, Small metabolism, Intestine, Small microbiology, Symbiosis
- Published
- 2014
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36. An ecological network of polysaccharide utilization among human intestinal symbionts.
- Author
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Rakoff-Nahoum S, Coyne MJ, and Comstock LE
- Subjects
- Ecosystem, Humans, Intestinal Mucosa metabolism, Bacteroidetes metabolism, Intestines microbiology, Polysaccharides metabolism, Symbiosis
- Abstract
Background: The human intestine is colonized with trillions of microorganisms important to health and disease. There has been an intensive effort to catalog the species and genetic content of this microbial ecosystem. However, little is known of the ecological interactions between these microbes, a prerequisite to understanding the dynamics and stability of this host-associated microbial community. Here we perform a systematic investigation of public goods-based syntrophic interactions among the abundant human gut bacteria, the Bacteroidales., Results: We find evidence for a rich interaction network based on the breakdown and use of polysaccharides. Species that utilize a particular polysaccharide (producers) liberate polysaccharide breakdown products (PBPs) that are consumed by other species unable to grow on the polysaccharide alone (recipients). Cross-species gene addition experiments demonstrate that recipients can grow on a polysaccharide if the producer-derived glycoside hydrolase, responsible for PBP generation, is provided. These producer-derived glycoside hydrolases are public goods transported extracellularly in outer membrane vesicles allowing for the creation of PBP and concomitant recipient growth spatially distant from the producer. Recipients can exploit these ecological interactions and conditionally outgrow producers. Finally, we show that these public goods-based interactions occur among Bacteroidales species coresident within a natural human intestinal community., Conclusions: This study examines public goods-based syntrophic interactions between bacterial members of the human gut microbial ecosystem. This polysaccharide-based network likely represents foundational relationships creating organized ecological units within the intestinal microbiota, knowledge of which can be applied to impact human health., (Copyright © 2014 Elsevier Ltd. All rights reserved.)
- Published
- 2014
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37. Toll-like receptors and cancer.
- Author
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Rakoff-Nahoum S and Medzhitov R
- Subjects
- Animals, Homeostasis, Humans, Immunologic Surveillance, Immunotherapy, Adoptive, Infections immunology, Infections physiopathology, Inflammation immunology, Inflammation physiopathology, Ligands, Mice, Myeloid Differentiation Factor 88 deficiency, Myeloid Differentiation Factor 88 physiology, Neoplasms immunology, Neoplasms therapy, Regeneration physiology, Signal Transduction physiology, T-Lymphocyte Subsets immunology, Wound Healing physiology, Cell Transformation, Neoplastic, Neoplasm Proteins physiology, Neoplasms metabolism, Toll-Like Receptors physiology
- Abstract
Toll-like receptors (TLRs) are a family of pattern recognition receptors that are best-known for their role in host defence from infection. Emerging evidence also suggests that TLRs have an important role in maintaining tissue homeostasis by regulating the inflammatory and tissue repair responses to injury. The development of cancer has been associated with microbial infection, injury, inflammation and tissue repair. Here we discuss how the function of TLRs may relate to these processes in the context of carcinogenesis.
- Published
- 2009
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38. T cell responses to human endogenous retroviruses in HIV-1 infection.
- Author
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Garrison KE, Jones RB, Meiklejohn DA, Anwar N, Ndhlovu LC, Chapman JM, Erickson AL, Agrawal A, Spotts G, Hecht FM, Rakoff-Nahoum S, Lenz J, Ostrowski MA, and Nixon DF
- Subjects
- Cohort Studies, Cross-Sectional Studies, Flow Cytometry, HIV Infections immunology, HIV-1, Humans, RNA, Viral blood, Reverse Transcriptase Polymerase Chain Reaction, Viral Load, Antigens, Viral immunology, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes virology, Endogenous Retroviruses immunology, HIV Infections virology
- Abstract
Human endogenous retroviruses (HERVs) are remnants of ancient infectious agents that have integrated into the human genome. Under normal circumstances, HERVs are functionally defective or controlled by host factors. In HIV-1-infected individuals, intracellular defense mechanisms are compromised. We hypothesized that HIV-1 infection would remove or alter controls on HERV activity. Expression of HERV could potentially stimulate a T cell response to HERV antigens, and in regions of HIV-1/HERV similarity, these T cells could be cross-reactive. We determined that the levels of HERV production in HIV-1-positive individuals exceed those of HIV-1-negative controls. To investigate the impact of HERV activity on specific immunity, we examined T cell responses to HERV peptides in 29 HIV-1-positive and 13 HIV-1-negative study participants. We report T cell responses to peptides derived from regions of HERV detected by ELISPOT analysis in the HIV-1-positive study participants. We show an inverse correlation between anti-HERV T cell responses and HIV-1 plasma viral load. In HIV-1-positive individuals, we demonstrate that HERV-specific T cells are capable of killing cells presenting their cognate peptide. These data indicate that HIV-1 infection leads to HERV expression and stimulation of a HERV-specific CD8+ T cell response. HERV-specific CD8+ T cells have characteristics consistent with an important role in the response to HIV-1 infection: a phenotype similar to that of T cells responding to an effectively controlled virus (cytomegalovirus), an inverse correlation with HIV-1 plasma viral load, and the ability to lyse cells presenting their target peptide. These characteristics suggest that elicitation of anti-HERV-specific immune responses is a novel approach to immunotherapeutic vaccination. As endogenous retroviral sequences are fixed in the human genome, they provide a stable target, and HERV-specific T cells could recognize a cell infected by any HIV-1 viral variant. HERV-specific immunity is an important new avenue for investigation in HIV-1 pathogenesis and vaccine design.
- Published
- 2007
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39. Regulation of spontaneous intestinal tumorigenesis through the adaptor protein MyD88.
- Author
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Rakoff-Nahoum S and Medzhitov R
- Subjects
- Animals, Apoptosis, Cell Proliferation, Colonic Neoplasms genetics, Colonic Neoplasms immunology, Colonic Neoplasms pathology, Colonic Neoplasms physiopathology, Disease Models, Animal, Female, Gene Expression Regulation, Neoplastic, Genes, APC, Immunity, Innate, Intestinal Neoplasms genetics, Intestinal Neoplasms immunology, Intestinal Neoplasms pathology, Intestine, Large pathology, Intestine, Small pathology, Male, Mice, Mice, Inbred C57BL, Myeloid Differentiation Factor 88 genetics, Intestinal Neoplasms physiopathology, Myeloid Differentiation Factor 88 physiology, Signal Transduction
- Abstract
Inflammation is increasingly recognized as an important component of tumorigenesis, although the mechanisms and pathways involved are not well understood. Tumor development is regulated by products of several modifier genes, but instructions for their tumor-specific expression are currently unknown. We show that the signaling through the adaptor protein MyD88 has a critical role in spontaneous tumor development in mice with heterozygous mutation in the adenomatous polyposis coli (APC) gene. We found that MyD88-dependent signaling controls the expression of several key modifier genes of intestinal tumorigenesis and has a critical role in both spontaneous and carcinogen-induced tumor development. This study thus reveals the important role of an innate immune signaling pathway in intestinal tumorigenesis.
- Published
- 2007
- Full Text
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40. Prostaglandin-secreting cells: a portable first aid kit for tissue repair.
- Author
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Rakoff-Nahoum S and Medzhitov R
- Subjects
- Cell Division, Homeostasis, Humans, Models, Biological, Stem Cells physiology, Intestinal Mucosa physiology, Intestines physiology, Prostaglandins metabolism, Regeneration physiology
- Abstract
After intestinal injury, both the number and type of intestinal epithelial cells must be restored. Intestinal stem cells, located at the base of the intestinal crypt, repopulate the depleted crypt in a process known as compensatory proliferation. In this issue of the JCI, Brown et al. describe a new mechanism by which this process is regulated (see the related article beginning on page 258). Surprisingly, they find that a subset of stromal cells present within the intestinal tissue and expressing the proliferative factor prostaglandin-endoperoxidase synthase 2 (Ptgs2) is repositioned next to the intestinal stem cell compartment where local production of PGE(2) controls injury-induced epithelial cell proliferation.
- Published
- 2007
- Full Text
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41. Why cancer and inflammation?
- Author
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Rakoff-Nahoum S
- Subjects
- Animals, Cell Death, Cell Transformation, Neoplastic, DNA Damage, Fibronectins chemistry, Genes, Tumor Suppressor, Genetic Predisposition to Disease, Homeostasis, Humans, Immune System, Models, Biological, NF-kappa B metabolism, Neoplasms etiology, Inflammation complications, Neoplasms complications
- Abstract
Central to the development of cancer are genetic changes that endow these "cancer cells" with many of the hallmarks of cancer, such as self-sufficient growth and resistance to anti-growth and pro-death signals. However, while the genetic changes that occur within cancer cells themselves, such as activated oncogenes or dysfunctional tumor suppressors, are responsible for many aspects of cancer development, they are not sufficient. Tumor promotion and progression are dependent on ancillary processes provided by cells of the tumor environment but that are not necessarily cancerous themselves. Inflammation has long been associated with the development of cancer. This review will discuss the reflexive relationship between cancer and inflammation with particular focus on how considering the role of inflammation in physiologic processes such as the maintenance of tissue homeostasis and repair may provide a logical framework for understanding the connection between the inflammatory response and cancer.
- Published
- 2006
42. Retraction: Regulation of class II expression in monocytic cells after HIV-1 infection.
- Author
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Rakoff-Nahoum S, Chen H, Kraus T, George I, Oei E, Tyorkin M, Salik E, Beuria P, and Sperber K
- Published
- 2006
- Full Text
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43. Role of toll-like receptors in spontaneous commensal-dependent colitis.
- Author
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Rakoff-Nahoum S, Hao L, and Medzhitov R
- Subjects
- Adaptor Proteins, Signal Transducing metabolism, Animals, Cell Movement, Colitis immunology, Colitis pathology, Dendritic Cells cytology, Dendritic Cells immunology, Dendritic Cells metabolism, Interleukin-10 deficiency, Interleukin-10 genetics, Interleukin-10 metabolism, Interleukin-2 deficiency, Interleukin-2 genetics, Interleukin-2 metabolism, Lymphocyte Activation immunology, Mice, Mice, Knockout, Myeloid Differentiation Factor 88, Signal Transduction, T-Lymphocytes immunology, T-Lymphocytes metabolism, Th1 Cells metabolism, Toll-Like Receptors immunology, Colitis metabolism, Toll-Like Receptors metabolism
- Abstract
Inflammatory bowel disease (IBD) is thought to result from a dysregulated interaction between the host immune system and its commensal microflora. Heterogeneity of disease susceptibility in humans and rodents suggest that multiple mechanisms are responsible for the etiology of IBD. In particular, deficiencies in anti-inflammatory and immune-suppressive mechanisms play an important role in the development of IBD. However, it is unknown how the indigenous microflora stimulates the immune system and how this response is regulated. To address these questions, we investigated the role of Toll-like receptor (TLR) signaling in the development of spontaneous, commensal-dependent colitis in interleukin (IL)-2- and IL-10-deficient mice. We report that colitis was dependent on TLR signaling in Il10(-/-) mice. In contrast, Il2(-/-) mice developed intestinal inflammation in the absence of TLR signaling pathways. These results demonstrate a differential role of innate immune recognition by TLRs in the development of commensal-dependent colitis.
- Published
- 2006
- Full Text
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44. Detection of T lymphocytes specific for human endogenous retrovirus K (HERV-K) in patients with seminoma.
- Author
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Rakoff-Nahoum S, Kuebler PJ, Heymann JJ, E Sheehy M, Ortiz GM, S Ogg G, Barbour JD, Lenz J, Steinfeld AD, and Nixon DF
- Subjects
- Antibodies, Viral blood, Endogenous Retroviruses genetics, Female, Humans, Male, Middle Aged, Seminoma metabolism, Seminoma virology, T-Lymphocytes metabolism, Virus Integration, Antibodies, Viral analysis, Endogenous Retroviruses immunology, Seminoma immunology, T-Lymphocytes immunology
- Abstract
Human endogenous retrovirus K (HERV-K) is distinctive among the retroviruses that comprise about 8% of the human genome in that multiple HERV-K proviruses encode full-length viral proteins, and many HERV-K proviruses formed during recent human evolution. HERV-K gag proteins are found in the cytoplasm of primary tumor cells of patients with seminoma. We identified HERV-K-specific T cells in patients with a past history of seminoma using the interferon-gamma ELISPOT assay and an MHC-HERV-K peptide-specific tetramer. A minority of apparently healthy subjects without evident germ cell tumors also made HERV-K-specific T cell responses. In summary, we detected T cell reactivity to HERV-K peptides in both past seminoma patients and a minority of apparently healthy controls.
- Published
- 2006
- Full Text
- View/download PDF
45. Recognition of commensal microflora by toll-like receptors is required for intestinal homeostasis.
- Author
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Rakoff-Nahoum S, Paglino J, Eslami-Varzaneh F, Edberg S, and Medzhitov R
- Subjects
- Adaptor Proteins, Signal Transducing, Animals, Antigens, Differentiation genetics, Cells, Cultured, Chemotaxis, Leukocyte genetics, Colon immunology, Colon injuries, Colon microbiology, Cytokines metabolism, Female, Heat-Shock Proteins metabolism, Immunity immunology, Immunity, Innate immunology, Intestinal Mucosa injuries, Ligands, Male, Mice, Mice, Knockout, Myeloid Differentiation Factor 88, Receptors, Immunologic deficiency, Receptors, Immunologic genetics, Toll-Like Receptors, Bacteria immunology, Homeostasis immunology, Intestinal Mucosa immunology, Intestinal Mucosa microbiology, Membrane Glycoproteins immunology, Receptors, Cell Surface immunology, Symbiosis immunology
- Abstract
Toll-like receptors (TLRs) play a crucial role in host defense against microbial infection. The microbial ligands recognized by TLRs are not unique to pathogens, however, and are produced by both pathogenic and commensal microorganisms. It is thought that an inflammatory response to commensal bacteria is avoided due to sequestration of microflora by surface epithelia. Here, we show that commensal bacteria are recognized by TLRs under normal steady-state conditions, and this interaction plays a crucial role in the maintenance of intestinal epithelial homeostasis. Furthermore, we find that activation of TLRs by commensal microflora is critical for the protection against gut injury and associated mortality. These findings reveal a novel function of TLRs-control of intestinal epithelial homeostasis and protection from injury-and provide a new perspective on the evolution of host-microbial interactions.
- Published
- 2004
- Full Text
- View/download PDF
46. Regulation of class II expression in monocytic cells after HIV-1 infection.
- Author
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Rakoff-Nahoum S, Chen H, Kraus T, George I, Oei E, Tyorkin M, Salik E, Beuria P, and Sperber K
- Subjects
- Antigens, Differentiation, B-Lymphocyte biosynthesis, Antigens, Differentiation, B-Lymphocyte genetics, CCAAT-Enhancer-Binding Proteins biosynthesis, CCAAT-Enhancer-Binding Proteins genetics, CCAAT-Enhancer-Binding Proteins metabolism, Cell Compartmentation genetics, Cell Compartmentation immunology, DNA-Binding Proteins biosynthesis, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Gene Expression Regulation immunology, Genes, MHC Class II, HIV Antigens genetics, HIV Antigens physiology, HIV-1 genetics, HLA-D Antigens biosynthesis, HLA-D Antigens genetics, HLA-DR Antigens genetics, HLA-DR Antigens metabolism, Histocompatibility Antigens Class II biosynthesis, Histocompatibility Antigens Class II genetics, Humans, Hybridomas, Monocytes immunology, NFI Transcription Factors, Nuclear Proteins, Protein Binding genetics, Protein Binding immunology, Protein Transport genetics, Protein Transport immunology, Regulatory Factor X Transcription Factors, Transcription Factors biosynthesis, Transcription Factors genetics, Transcription Factors metabolism, Transfection, U937 Cells, Viral Regulatory and Accessory Proteins genetics, Viral Regulatory and Accessory Proteins physiology, Y-Box-Binding Protein 1, HIV-1 immunology, HLA-DR Antigens biosynthesis, Monocytes metabolism, Monocytes virology
- Abstract
Human macrophage hybridoma cells were used to study HLA-DR expression after HIV-1 infection. HLA-DR surface expression was lost 2 wk after infection that was associated with decreased mRNA transcription. Transfecting HLA-DR-alpha and HLA-DR-beta cDNA driven by a nonphysiological CMV promoter restored expression, suggesting that regulatory DNA-binding proteins may be affected by HIV-1 infection. There was no protein binding to conserved class II DNA elements (W/Z/S box, X-1 and X-2 boxes, and Y box) in a HIV-1-infected human macrophage hybridoma cell line, 43(HIV), and in primary monocytes that lost HLA-DR expression after HIV-1(BaL) infection. PCR analysis of the HIV-1-infected cells that lost HLA-DR expression revealed mRNA for W/Z/S (RFX-5), X-1 (RFX-5), X-2 (hX-2BP), and one Y box DNA-binding protein (NF-YB), and CIITA, a non-DNA-binding protein necessary for class II transcription. There was no mRNA for the Y box-binding protein, NF-YA. However, HLA-DR expression could be restored by transfection with NF-YA driven by a CMV promoter, although HLA-DR failed to localize in either the late endosomes, lysosomes, or acidic compartments. This was associated with a loss of class II-associated invariant chain peptide and leupeptin-induced protein in the 43(HIV) cells. To address this further, non-HIV-1-infected 43 cells were infected with vaccinia virus containing HIV-1 gag, nef, pol, and env proteins. HLA-DR failed to localize in neither the late endosomes, lysosomes, or acidic compartments in the vaccinia-infected cells containing HIV-1 env protein. HIV-1 appears to have multiple effects on class II expression in monocytic cells that may contribute to the immune defects seen in HIV-1-infected patients.
- Published
- 2001
- Full Text
- View/download PDF
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