2026 Jon M. Huibregtse: Biology and Biochemistry Researcher – H-Index, Publications & Awards

Discipline name	D-Index	World Ranking	Current World Ranking	National Ranking	Current National Ranking	Publications	Citations
Biology and Biochemistry	61	11094	10224	4798	4299	94	27430

Overview

Jon M. Huibregtse is affiliated with The University of Texas at Austin in the United States. Their research spans multiple areas within biochemistry, genetics, molecular biology, and medicine, with a substantial focus on molecular and cell biology subfields.

The main fields of study for Huibregtse include:

Biochemistry, Genetics and Molecular Biology
Medicine

The subfields of study explored in their work cover:

Molecular Biology
Cell Biology
Immunology
Infectious Diseases
Oncology

Primary topics in their research involve:

Cellular transport and secretion
Ubiquitin and proteasome pathways
Interferon and immune responses
Endoplasmic Reticulum Stress and Disease
Lipid Membrane Structure and Behavior
Cell Adhesion Molecules Research
SARS-CoV-2 and COVID-19 Research

Frequent co-authors collaborating with Huibregtse include:

Jeanne C. Stachowiak
Susovan Sarkar
Feng Yuan
Grant Ashby
Jessica Perez

The scientist's recent publications demonstrate involvement in studies on viral replication, protein degradation, and proteostasis. Key papers include:

"Modulation of Extracellular ISG15 Signaling by Pathogens and Viral Effector Proteins," 2020, Cell Reports
"Proteome-wide identification of HSP70/HSC70 chaperone clients in human cells," 2020, PLoS Biology
"6-Thioguanine blocks SARS-CoV-2 replication by inhibition of PLpro," 2021, iScience
"A masked initiation region in retinoblastoma protein regulates its proteasomal degradation," 2020, Nature Communications
"6-Thioguanine blocks SARS-CoV-2 replication by inhibition of PLpro protease activities," 2020, bioRxiv (Cold Spring Harbor Laboratory)

Huibregtse's work is regularly published in venues such as:

bioRxiv (Cold Spring Harbor Laboratory)
Biophysical Journal
Cell Reports
iScience
Nature Communications

Best Publications

The E6 oncoprotein encoded by human papillomavirus types 16 and 18 promotes the degradation of p53

Martin Scheffner;Bruce A. Werness;Jon M. Huibregtse;Arnold J. Levine

5280
Citations
The HPV-16 E6 and E6-AP complex functions as a ubiquitin-protein ligase in the ubiquitination of p53

Martin Scheffner;Jon M. Huibregtse;Richard D. Vierstra;Peter M. Howley

3154
Citations
A family of proteins structurally and functionally related to the E6-AP ubiquitin-protein ligase.

Jon M. Huibregtse;Martin Scheffner;Sylvie Beaudenon;Peter M. Howley

1433
Citations
Protein ubiquitination involving an E1–E2–E3 enzyme ubiquitin thioester cascade

Martin Scheffner;Ulrike Nuber;Jon M. Huibregtse

1305
Citations
A cellular protein mediates association of p53 with the E6 oncoprotein of human papillomavirus types 16 or 18.

Jon M. Huibregtse;Martin Scheffner;Peter M. Howley

1116
Citations
In Vivo Ubiquitination and Proteasome-mediated Degradation of p53

Carl G. Maki;Jon M. Huibregtse;Peter M. Howley

870
Citations
Cloning and expression of the cDNA for E6-AP, a protein that mediates the interaction of the human papillomavirus E6 oncoprotein with p53

Jon M. Huibregtse;Martin Scheffner;Peter M. Howley

737
Citations
Structure of an E6AP-UbcH7 complex: insights into ubiquitination by the E2-E3 enzyme cascade.

Lan Huang;Elspeth Kinnucan;Guangli Wang;Sylvie Beaudenon

734
Citations
Human Scribble (Vartul) Is Targeted for Ubiquitin-Mediated Degradation by the High-Risk Papillomavirus E6 Proteins and the E6AP Ubiquitin-Protein Ligase

Shunsuke Nakagawa;Jon M. Huibregtse

606
Citations
Mycobacterial Disease and Impaired IFN-γ Immunity in Humans with Inherited ISG15 Deficiency

Dusan Bogunovic;Minji Byun;Larissa A. Durfee;Avinash Abhyankar

592
Citations
A PPxY motif within the VP40 protein of Ebola virus interacts physically and functionally with a ubiquitin ligase: implications for filovirus budding.

Ronald N. Harty;Melissa E. Brown;Guangli Wang;Jon M Huibregtse

571
Citations
Human ISG15 conjugation targets both IFN-induced and constitutively expressed proteins functioning in diverse cellular pathways

Chen Zhao;Carilee Denison;Jon M. Huibregtse;Steven Gygi

561
Citations
Localization of the E6-AP regions that direct human papillomavirus E6 binding, association with p53, and ubiquitination of associated proteins

Jon M. Huibregtse;Martin Scheffner;Peter M. Howley

540
Citations
The transcriptional transactivation function of wild-type p53 is inhibited by SV40 large T-antigen and by HPV-16 E6 oncoprotein.

J.A. Mietz;T. Unger;J.M. Huibregtse;P.M. Howley

507
Citations
INTERACTIONS OF HPV E6 AND E7 ONCOPROTEINS WITH TUMOUR SUPPRESSOR GENE PRODUCTS

K. Munger;M. Scheffner;J. M. Huibregtse;P. M. Howley

410
Citations
The ISG15 Conjugation System Broadly Targets Newly Synthesized Proteins: Implications for the Antiviral Function of ISG15

Larissa A. Durfee;Nancy Lyon;Kyungwoon Seo;Jon M. Huibregtse

393
Citations
The UbcH8 ubiquitin E2 enzyme is also the E2 enzyme for ISG15, an IFN-α/β-induced ubiquitin-like protein

Chen Zhao;Sylvie L. Beaudenon;Melissa L. Kelley;M. Brett Waddell

375
Citations
Herc5, an Interferon-induced HECT E3 Enzyme, Is Required for Conjugation of ISG15 in Human Cells

Anahita Dastur;Sylvie Beaudenon;Melissa Kelley;Robert M. Krug

372
Citations
Identification of a human ubiquitin-conjugating enzyme that mediates the E6-AP-dependent ubiquitination of p53.

Martin Scheffner;Jon M. Huibregtse;Peter M. Howley

364
Citations
Correction: A Family of Proteins Structurally and Functionally Related to the E6-AP Ubiquitin-Protein Ligase

Jon M. Huibregtse;Martin Scheffner;Sylvie Beaudenon;Peter M. Howley

195
Citations

Frequent Co-Authors

Peter M. Howley Harvard Medical School

Martin Scheffner University of Konstanz

Karl Münger Tufts University

Robert M. Krug The University of Texas at Austin

Jean-Laurent Casanova The University of Texas Southwestern Medical Center

Tanya T. Paull The University of Texas at Austin

Jue Chen Rockefeller University

Donald P. McDonnell Duke University

Andreas T Matouschek The University of Texas at Austin

Saleh Al-Muhsen King Saud University

External Links

Personal website of Jon M. Huibregtse

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Online study in these areas allows for career progression and supports a wide range of interests within biology, health, and biochemistry.

Jon M. Huibregtse

D-Index & Metrics

D-Index & Metrics

Biology and Biochemistry

Overview

Best Publications

The E6 oncoprotein encoded by human papillomavirus types 16 and 18 promotes the degradation of p53

The HPV-16 E6 and E6-AP complex functions as a ubiquitin-protein ligase in the ubiquitination of p53

A family of proteins structurally and functionally related to the E6-AP ubiquitin-protein ligase.

Protein ubiquitination involving an E1–E2–E3 enzyme ubiquitin thioester cascade

A cellular protein mediates association of p53 with the E6 oncoprotein of human papillomavirus types 16 or 18.

In Vivo Ubiquitination and Proteasome-mediated Degradation of p53

Cloning and expression of the cDNA for E6-AP, a protein that mediates the interaction of the human papillomavirus E6 oncoprotein with p53

Structure of an E6AP-UbcH7 complex: insights into ubiquitination by the E2-E3 enzyme cascade.

Human Scribble (Vartul) Is Targeted for Ubiquitin-Mediated Degradation by the High-Risk Papillomavirus E6 Proteins and the E6AP Ubiquitin-Protein Ligase

Mycobacterial Disease and Impaired IFN-γ Immunity in Humans with Inherited ISG15 Deficiency

A PPxY motif within the VP40 protein of Ebola virus interacts physically and functionally with a ubiquitin ligase: implications for filovirus budding.

Human ISG15 conjugation targets both IFN-induced and constitutively expressed proteins functioning in diverse cellular pathways

Localization of the E6-AP regions that direct human papillomavirus E6 binding, association with p53, and ubiquitination of associated proteins

The transcriptional transactivation function of wild-type p53 is inhibited by SV40 large T-antigen and by HPV-16 E6 oncoprotein.

INTERACTIONS OF HPV E6 AND E7 ONCOPROTEINS WITH TUMOUR SUPPRESSOR GENE PRODUCTS

The ISG15 Conjugation System Broadly Targets Newly Synthesized Proteins: Implications for the Antiviral Function of ISG15

The UbcH8 ubiquitin E2 enzyme is also the E2 enzyme for ISG15, an IFN-α/β-induced ubiquitin-like protein

Herc5, an Interferon-induced HECT E3 Enzyme, Is Required for Conjugation of ISG15 in Human Cells

Identification of a human ubiquitin-conjugating enzyme that mediates the E6-AP-dependent ubiquitination of p53.

Correction: A Family of Proteins Structurally and Functionally Related to the E6-AP Ubiquitin-Protein Ligase

Frequent Co-Authors

External Links

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