Publications

Most significant publications

My research program investigates the interface between the nervous and immune systems in health and disease. The immune system has long been known to impact nervous system function through neuroinflammatory pathways. Importantly and conversely, neural circuits have more recently been shown to control inflammatory responses through direct, structural interfaces between immune and nervous tissues. These cellular and molecular points of engagement are distributed across the body to serve important homeostatic and developmental functions. Their dysregulation, in turn, contribute to disease, including neurodevelopmental disorders.

Three primary avenues of my research program have made significant contributions to our growing understanding of the neuro-immune interface:

1. Pro-inflammatory programmed cell death pathways in disease

Volchuk A, Ye A, Chi L, Steinberg BE* & Goldenberg NM*. Indirect Regulation of HMGB1 Release by Gasdermin D. Nature Commmunications. 2020; 11(1):4561.

In this recent publication from my group on which I am a senior author, we characterized the regulation of danger-associated molecular patterns by the inflammasome executioner protein gasdermin D during pyroptosis. The field had postulated that like interleuin-1β, which is secreted through gasdermin D pores, intracellular danger molecules (e.g. HMGB1) would be released into the extracellular space to propagate inflammatory response by a similar mechanism. We discovered, in contrast, that HMGB1 release requires gasdermin D but that it does not permeate through its pore. Therefore, this work changed our understanding of how programmed cell death pathways trigger and propagate pro-inflammatory immune responses. These studies emphasize my laboratory’s experience and focus on inflammasome physiology and methodological expertise. We are now advancing these findings to better understand how pro-inflammatory programmed cell death pathways, such as gasdermin D-mediated pyroptosis, impact on neurodevelopment and neurodevelopmental diseases. Our preliminary investigations are revealing an important role for this pathway in the adverse structural and functional consequences of early life tissue injury as experienced by preterm neonates receiving NICU and operative care.

2. Neuronal sensing and modulation of inflammation

Steinberg BE*, Silverman HA*. Robbiati S*, Gunasekaran MK, Tsaava T, Battinelli E, Stiegler A, Bouton C, Chavan SS, Tracey KJ & Huerta PT. Cytokine-specific neurograms in the sensory vagus nerve. Bioelectronic Medicine. 2016; 7-17.

This seminal publication focuses on the interface between the immune and nervous systems to delineate how the nervous system monitors inflammation. Using electrical recordings, we demonstrated that sensory nerves are differentially activated by pro-inflammatory molecules (e.g. cytokines and bacterial products). Building on this discovery, we and others are establishing a compendium of cytokine-specific neural signatures to determine whether these unique signatures can be identified in neural recordings from preclinical models of systemic inflammatory disease or infection. This work has implications in the development of new bioelectronic assays and technologies for the diagnosis of neuroinflammatory diseases, responses to therapies, and prognostication.

3. Immune modulation of autonomic nervous system function

Olofsson PS, Steinberg BE, Sobbi R, Cox MA, Ahmed MN, Oswald O Szekeres F, Hanes WM, Introini A, Liu SF, Holodick NE, Rothstein TL, Lövdahl C, Chavan SS, Yang H, Pavlov VA, Broliden K, Andersson U, Diamond B, Miller EJ, Arner A, Gregersen PK, Backx PH, Mak TW & Tracey KJ. Blood pressure regulation by CD4+ lymphocytes expressing choline acetyltransferase. Nature Biotechnology. 2016; 34(10):1066-1071.
Cox MA, Duncan GS, Lin GHY, Steinberg BE, Yu LX, Brenner D, Buckler LN, Elia AJ, Wakeham AC, Neiman B, Dominguez-Brauer C, Elford AR, Gill KT, Kubli SP, Haight J, Berger T, Ohashi PS, Tracey KJ, Olofsson PS & Mak TW. Choline acetyltransferase-expressing T cells are required to control chronic viral infection. Science. 2019; 363(6427):639-644.

In these publications, we identify and characterize a unique subset of immune cells that modulate systemic blood pressure and chronic viral infection in mice. Genetically abolishing these cells leads to hypertension, whereas their administration lowers blood pressure. In addition to establishing that immune cells impact the cardiovascular system, this work identifies a novel therapeutic target for the management of hypertension. This same subset of immune cells promotes vasodilation that enhances the migration of lymphocytes into tissue chronically infected with virus, thereby facilitating clearance of viral infections.

These and other projects in my laboratory are providing a new understanding of the fundamental interaction between the nervous and immune systems, including in neurodevelopment. We aim to translate our findings toward the treatment of preterm neonates at-risk of adverse neurodevelopmental outcomes and improve their lifelong brain health.

We provide the first evidence that a sensory nerve is activated by systemic inflammation in a mediator-specific fashion. This work lays the foundation for an immunological sensory neural code that may allow neural recordings to aid the clinical diagnosis and monitoring of inflammatory disease.

Olofsson PS, Steinberg BE, Sobbi R, Cox MA, Ahmed MN, Oswald O Szekeres F, Hanes WM, Introini A, Liu SF, Holodick NE, Rothstein TL, Lövdahl C, Chavan SS, Yang H, Pavlov VA, Broliden K, Andersson U, Diamond B, Miller EJ, Arner A, Gregersen PK, Backx PH, Mak TW & Tracey KJ. Blood pressure regulation by CD4+ lymphocytes expressing choline acetyltransferase. Nature Biotechnology. 2016; 34(10):1066-1071.
Cox MA, Duncan GS, Lin GHY, Steinberg BE, Yu LX, Brenner D, Buckler LN, Elia AJ, Wakeham AC, Neiman B, Dominguez-Brauer C, Elford AR, Gill KT, Kubli SP, Haight J, Berger T, Ohashi PS, Tracey KJ, Olofsson PS & Mak TW. Choline acetyltransferase-expressing T cells are required to control chronic viral infection. Science. 2019; 363(6427):639-644.

Goldenberg NM*, Steinberg BE*, Slutsky AS & Lee WL. Broken barriers: a new take on sepsis pathogenesis. Science Translational Medicine. 2011; 3(88):88ps25.

Therapy for sepsis remains primarily supportive despite intense research into its pathogenesis. Here, we highlight the importance of leaky vasculature and tissue edema in sepsis, and present the endothelium and barrier integrity as a new target for sepsis therapeutics, providing several potential treatment approaches.

Steinberg BE, Huynh KK, Brodovitch A, Jabs S, Stauber T, Jentsch TJ, & Grinstein S. A cation counterflux supports lysosomal acidification. Journal of Cell Biology. 2010; 189(7):1171-1186.

Using multiple cell biological approaches, we deconstruct the ion fluxes within lysosomes that allow for their acidification, In addition to delineating a fundamental cell physiologic process, this work has significant implications on the pathogenesis of cystic fibrosis, particularly patient susceptibility to bacterial infections.

Peer-reviewed publications

Journal Articles

Ghaffari S, Jang E, Nabi FN, Sanwal R, Khosraviani N, Wang C, Steinberg BE, Goldenberg NM, Ikeda J & Lee WL. Endothelial HMGB1 is a Critical Regulator of LDL Transcytosis via an SREBP2-SR-BI Axis. Arterioscler Thromb Vasc Bio. 2020 Oct 15:ATVBAHA120314557.
Steinberg BE, Aoyama K, McVey M, Levin D, Siddiqui A, Munshey F, Goldenberg NM, Faraoni D & Maynes JT. Efficacy and safety of decontamination for N95 respirator reuse: a systematic literature search and narrative synthesis. Can J Anaesth. 2020 (in press).
Fergusson DA, Avey MT, Barron CC, Bocock M, Biefer KE, Boet S, Bourque SL, Conic I, Chen K, Dong YY, Fox GM, George RB, Goldenberg NM, Gragasin FS, Harsha P, Hong PJ, James TE, Larrigan SM, MacNeil JL, Manuel CA, Maximos S, Mazer D, Mittal R, McGinn R, Nguyen LH, Patel A, Richebé P, Saha TK, Steinberg BE, Sampson SD, Stewart DJ, Syed S, Vella K, Wesch NL, Lalu MM; Canadian Perioperative Anesthesia Clinical Trials Group. Reporting preclinical anesthesia study (REPEAT): Evaluating the quality of reporting in the preclinical anesthesiology literature. PLoS One. 2019; 14(5):e0215221.
Goldenberg NM, Rabinovitch M & Steinberg BE. The inflammatory basis of pulmonary arterial hypertension. Anesthesiology. 2019; 131(4):898-907.
Levin DN, Strantzas S & Steinberg BE. Intra-operative neuro-monitoring in paediatric spinal surgery. British Journal of Anaesthesia Education. 2019; 19(5):165-171.
Goldenberg NM, Hu Y, Hu X, Volchuk A, Zhao YD, de Perrot M, Tracey KJ, Al-Abed Y, Steinberg BE* & Kuebler WM*. Therapeutic targeting of high mobility group box-1 in pulmonary arterial hypertension. American Journal of Respiratory and Critical Care Medicine. 2019; 199(12):1566-1569.
Goldenberg NM & Steinberg BE. Inflammation drives pulmonary arterial hypertension. Anesthesiology. 2019; 130(5):820-821.
Battinelli Masi E, Valdes-Ferrer SI & Steinberg BE. The vagus neruo-metabolic interface and clinical disease. International Journal of Obesity. 2018; 42(6):1101-1111.
Silverman HA, Stiegler A, Tsaava T, Newman J, Steinberg BE, Battinelli Masi E, Robbiati S, Bouton C, Huerta PT, Chavan SS & Tracey KJ. Standardization of methods to record vagus nerve activity in mice. Bioelectronic Medicine. 2018; 4:3.
Goldenberg NM, Steinberg BE, Rutka JT, Chen R, Kapus A & Lee WL. Research projects in the Surgeon-Scientist and Clinician-Investigator programs at the University of Toronto (1987-2016): a cohort study. CMAJ Open. 2016; 4(3):E444-447.
Steinberg BE, Sundman E, Terrando N, Ericsson LI & Olofsson PS. The Neural Control of Inflammation: Implications for perioperative and critical care. Anesthesiology. 2016; 124(5):1174-1189.
Steinberg BE, Goldenberg NM, Fairn GD, Kuebler WM, Slutsky AS & Lee WL. Where has the basic science gone? The decline of biomedical research in the medical literature. FASEB Journal. 2015; 30(2):515-518.
Goldenberg NM, Steinberg BE, Lee WL, Wijeysundera D & Kavanagh B. Lung Protective Ventilation for the Operating Room. Anesthesiology. 2014; 121(1):184-188.
Schlam D, Chatilialoglu A, Steinberg BE, Ueyama T, Du G, Grinstein S & Fairn GD. Diacylglycerol kinases terminate diacylglycerol signalling during the respiratory burst leading to heterogeneous phagosomal NADPH oxidase activity. Journal of Biological Chemistry. 2013; 288(32):23090-23104.
Steinberg BE*, Goldenberg NM* & Lee WL. Do viral infections mimic bacterial sepsis? The role of microvascular permeability: A review of mechanisms and methods. Antiviral Research. 2012; 93(1):2-15.
Goldenberg NM*, Steinberg BE*, Slutsky AS & Lee WL. Broken barriers: a new take on sepsis pathogenesis. Science Translational Medicine. 2011; 3(88):88ps25.
Koivusalo M*, Steinberg BE*, Mason D & Grinstein S. In situ measurement of the electrical potential across the lysosomal membrane using FRET. Traffic. 2011; 12(8):972-982.
DiCiccio JE & Steinberg BE. Lysosomal pH and the analysis of the counter-ion pathways that support acidification. Journal of General Physiology. 2011; 189(7):1171-1186.
Steinberg BE, Huynh KK, Brodovitch A, Jabs S, Stauber T, Jentsch TJ, & Grinstein S. A cation counterflux supports lysosomal acidification. Journal of Cell Biology. 2010; 189(7):1171-1186.
Lee HK, Mattei LM, Steinberg BE, Alberts P, Lee YH, Chervonsky A, Mizushima N, Grinstein S, & Iwasaki A. In vivo requirement for Atg5 in antigen presentation by dendritic cells. Immunity. 2010; 32(2):227-239.
Goldenberg NM & Steinberg BE. Surface charge: a key determinant of protein localization and function. Cancer Research. 2010; 70(4):1277-1280.
Huang JJ, Canadian V, Lam GY, Steinberg BE, Dinauer MC, Magalhaes MAO, Glogauer M, Grinstein S, & Brumell JH. Activation of anti-bacterial autophagy: a novel function for NADPH oxidases in host defense. Proceedings of the National Academy of Science U.S.A. 2009; 106:6226-6231.
Mohammad-Panah R, Wellhauser L, Steinberg BE, Wang Y, Huan LJ, Liu XD, & Bear CE. An essential role for ClC-4 in transferrin receptor function revealed in studies of fibroblasts derived from Clcn4 null mice. Journal of Cell Science. 2009; 15:1229-1237.
Steinberg BE & Grinstein S. Pathogen destruction vs. intracellular survival: the role of lipids as phagosomal fate determinints. Journal of Clinical Investigation. 2008; 118:2002-2011.
Birmingham CL, Canadien V, Kaniuk NA, Steinberg BE, Higgins DE, Brumell JH. Listeriolysin O allows Listeria monocytogenes replication in macrophage vacuoles. Nature. 2008; 451(7176):350-354.
Steinberg BE, Huynh KK, & Grinstein S. Phagosome acidification: measurement, manipulation and functional consequences. Biochemical Society Transactions. 2007l 35(Pt 5):1083-1087.
Steinberg BE, Touret N, Vargas-Caballero M, & Grinstein S. In situ measurements of the electrical potential across the phagosomal membrane using FRET and its contribution to the proton-motive force. Proceedings of the National Academy of Science U.S.A. 2007; 104:9523-9528.
Steinberg BE & Grinstein S. Unconventional roles of the NADPH oxidase: signaling, ion homeostasis, and cell death. Science STKE. 2007; 27;2007(379):pe11.
Steinberg BE, Scott CC, & Grinstein S. High-throughput assays of phagocytosis, phagosome maturation and bacterial invasion. American Journal of Physiology Cell Physiology. 2007; 292:C945-952
Tabeta K, Hoebe K, Janssen EM, Du X, Georgel P, Crozat K, Mudd S, Mann N, Sovath S, Goode J, Shamel L, Herskovits AA, Portnoy DA, Cooke M, Tarantino LM, Wiltshire T, Steinberg BE, Grinstein S, & Beutler B. The Unc93b1 mutation 3d disrupts exogenous antigen presentation and signaling via Toll-like receptors 3, 7 and 9. Nature Immunology. 2006; 7:156-164.
Steinberg BE, Glass L, Shrier A & Bub G. The role of heterogeneities and intercellular coupling in wave propagation in cardiac tissue. Philosophical Transactions of the Royal Society A. 2006; 364:1299-1311.
Steinberg BE, Wang Y, Huang H, & Miura RM. Spatial buffering mechanism: A mathematical model and computer simulation. Mathematical Biosciences and Engineering 2005; 2:675-702.