D-Index & Metrics Best Publications

Gregory L. Stahl

Brigham and Women's Hospital
United States

D-Index & Metrics D-index (Discipline H-index) only includes papers and citation values for an examined discipline in contrast to General H-index which accounts for publications across all disciplines.

Discipline name Citations Publications World Ranking National Ranking

Immunology D-index 62 Citations 12,263 158 World Ranking 2167 National Ranking 1046

Overview

What is he best known for?

The fields of study he is best known for:

Enzyme
Internal medicine
Gene

His main research concerns Immunology, Complement system, Lectin pathway, Inflammation and Pharmacology. His research integrates issues of Reperfusion injury, Ischemia and Myocardial infarction in his study of Immunology. Gregory L. Stahl interconnects Oxidative stress, Internal medicine, Endocrinology, Lectin and Neuropathic pain in the investigation of issues within Complement system.

His biological study spans a wide range of topics, including Collectin and Classical complement pathway. His research in Lectin pathway intersects with topics in Immunoglobulin A, Mannan-binding lectin and Complement. His Inflammation research is multidisciplinary, incorporating perspectives in Periodontitis, Chemotaxis, Endogeny and Arthritis.

His most cited work include:

Predominant role for C5b-9 in renal ischemia/reperfusion injury (387 citations)
Myocardial Infarction and Apoptosis After Myocardial Ischemia and Reperfusion Role of the Terminal Complement Components and Inhibition by Anti-C5 Therapy (382 citations)
Reduced Inflammation and Tissue Damage in Transgenic Rabbits Overexpressing 15-Lipoxygenase and Endogenous Anti-inflammatory Lipid Mediators (323 citations)

What are the main themes of his work throughout his whole career to date?

His primary areas of investigation include Complement system, Immunology, Mannan-binding lectin, Internal medicine and Molecular biology. His studies in Complement system integrate themes in fields like Lectin and Biochemistry. His Immunology research is multidisciplinary, relying on both Reperfusion injury and Pharmacology.

His research on Mannan-binding lectin also deals with topics like

Innate immune system, which have a strong connection to Effector,
Microbiology which intersects with area such as Immune system. As part of the same scientific family, Gregory L. Stahl usually focuses on Internal medicine, concentrating on Endocrinology and intersecting with Umbilical vein and Cell biology. The concepts of his Molecular biology study are interwoven with issues in Oxidative stress and Peptide sequence.

He most often published in these fields:

Complement system (47.12%)
Immunology (38.94%)
Mannan-binding lectin (27.40%)

What were the highlights of his more recent work (between 2009-2020)?

Complement system (47.12%)
Immunology (38.94%)
Mannan-binding lectin (27.40%)

In recent papers he was focusing on the following fields of study:

Gregory L. Stahl spends much of his time researching Complement system, Immunology, Mannan-binding lectin, Alternative complement pathway and Lectin. The Complement system study combines topics in areas such as Inflammation, Molecular biology, Microbiology and Arthritis. His Immunology study incorporates themes from Reperfusion injury, Stroke and Cell biology.

His Mannan-binding lectin study combines topics in areas such as Ebola virus, Innate immune system, Internal medicine and C-type lectin. His study in Alternative complement pathway is interdisciplinary in nature, drawing from both Inflammatory arthritis, Complement factor B, Factor H and Classical complement pathway. The various areas that Gregory L. Stahl examines in his Lectin study include Coagulation and Pharmacology.

Between 2009 and 2020, his most popular works were:

The Lectin Pathway of Complement Activation Is a Critical Component of the Innate Immune Response to Pneumococcal Infection (116 citations)
Role of C3a Receptors, C5a Receptors, and Complement Protein C6 Deficiency in Collagen Antibody-Induced Arthritis in Mice (91 citations)
Mannose-binding lectin and its associated proteases (MASPs) mediate coagulation and its deficiency is a risk factor in developing complications from infection, including disseminated intravascular coagulation (90 citations)

In his most recent research, the most cited papers focused on:

Enzyme
Internal medicine
Gene

Complement system, Immunology, Mannan-binding lectin, Lectin and Alternative complement pathway are his primary areas of study. His studies deal with areas such as Proteases, Molecular biology, Internal medicine and Endocrinology as well as Complement system. The study incorporates disciplines such as Reperfusion injury, Ischemia and Stroke in addition to Immunology.

His study focuses on the intersection of Ischemia and fields such as Pharmacology with connections in the field of Troponin I, Troponin and Complement component 5. Gregory L. Stahl has included themes like Innate immune system, Microbiology and Ebola virus in his Mannan-binding lectin study. His Alternative complement pathway study integrates concerns from other disciplines, such as Tumor necrosis factor alpha, Complement factor B, Complement membrane attack complex and Arthritis.

This overview was generated by a machine learning system which analysed the scientist’s body of work. If you have any feedback, you can contact us here.

Best Publications

Predominant role for C5b-9 in renal ischemia/reperfusion injury

Wuding Zhou;Conrad A. Farrar;Katsushige Abe;Julian R. Pratt.
Journal of Clinical Investigation (2000)

531 Citations

Myocardial Infarction and Apoptosis After Myocardial Ischemia and Reperfusion Role of the Terminal Complement Components and Inhibition by Anti-C5 Therapy

Antti P. Vakeva;Azin Agah;Scott A. Rollins;Louis A. Matis.
Circulation (1998)

526 Citations

Human IgA Activates the Complement System via the Mannan-Binding Lectin Pathway

Roos A;Bouwman Lh;van Gijlswijk-Janssen Dj;Faber-Krol Mc.
Journal of Immunology (2001)

454 Citations

Pharmacology and Biological Efficacy of a Recombinant, Humanized, Single-Chain Antibody C5 Complement Inhibitor in Patients Undergoing Coronary Artery Bypass Graft Surgery With Cardiopulmonary Bypass

Jane C. K. Fitch;Scott Rollins;Louis Matis;Bernadette Alford.
Circulation (1999)

447 Citations

Glomerular activation of the lectin pathway of complement in IgA nephropathy is associated with more severe renal disease.

Anja Roos;Maria Pia Rastaldi;Novella Calvaresi;Beatrijs D. Oortwijn.
Journal of The American Society of Nephrology (2006)

442 Citations

Complement Activation after Oxidative Stress : Role of the Lectin Complement Pathway

Charles D. Collard;Antti Väkevä;Margaret A. Morrissey;Azin Agah.
American Journal of Pathology (2000)

438 Citations

Reduced Inflammation and Tissue Damage in Transgenic Rabbits Overexpressing 15-Lipoxygenase and Endogenous Anti-inflammatory Lipid Mediators

Charles N. Serhan;Ashish Jain;Sylvie Marleau;Clary Clish.
Journal of Immunology (2003)

434 Citations

Inhibition of Mannose-Binding Lectin Reduces Postischemic Myocardial Reperfusion Injury

James E. Jordan;Michael C. Montalto;Gregory L. Stahl.
Circulation (2001)

333 Citations

Mannose-Binding Lectin Is a Regulator of Inflammation That Accompanies Myocardial Ischemia and Reperfusion Injury

Mary C. Walsh;Todd Bourcier;Kazue Takahashi;Lei Shi.
Journal of Immunology (2005)

309 Citations

Neutrophil-derived 5′-Adenosine Monophosphate Promotes Endothelial Barrier Function via CD73-mediated Conversion to Adenosine and Endothelial A2B Receptor Activation

Paul F. Lennon;Cormac T. Taylor;Gregory L. Stahl;Sean P. Colgan.
Journal of Experimental Medicine (1998)

278 Citations

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