Your search keyword '"Matthew Lynberg"' showing total 4 results

1. GIMAP6 regulates autophagy, immune competence, and inflammation in mice and humans

Author

Yikun Yao, Ping Du Jiang, Brittany N. Chao, Deniz Cagdas, Satoshi Kubo, Arasu Balasubramaniyam, Yu Zhang, Bella Shadur, Adeeb NaserEddin, Les R. Folio, Benjamin Schwarz, Eric Bohrnsen, Lixin Zheng, Matthew Lynberg, Simone Gottlieb, Michael A. Leney-Greene, Ann Y. Park, Ilhan Tezcan, Ali Akdogan, Rahsan Gocmen, Sevgen Onder, Avi Rosenberg, Elizabeth J. Soilleux, Errin Johnson, Peter K. Jackson, Janos Demeter, Samuel D. Chauvin, Florian Paul, Matthias Selbach, Haydar Bulut, Menna R. Clatworthy, Zewen K. Tuong, Hanlin Zhang, Benjamin J. Stewart, Catharine M. Bosio, Polina Stepensky, Simon Clare, Sundar Ganesan, John C. Pascall, Oliver Daumke, Geoffrey W. Butcher, Andrew J. McMichael, Anna Katharina Simon, and Michael J. Lenardo

Subjects

Inflammation, Mice, Cancer Research, Cardiovascular and Metabolic Diseases, Immunology, Autophagy, Immunologic Deficiency Syndromes, Immunology and Allergy, Animals, Endothelial Cells, Humans, Function and Dysfunction of the Nervous System, GTP Phosphohydrolases

Abstract

Inborn errors of immunity (IEIs) unveil regulatory pathways of human immunity. We describe a new IEI caused by mutations in the GTPase of the immune-associated protein 6 (GIMAP6) gene in patients with infections, lymphoproliferation, autoimmunity, and multiorgan vasculitis. Patients and Gimap6−/− mice show defects in autophagy, redox regulation, and polyunsaturated fatty acid (PUFA)–containing lipids. We find that GIMAP6 complexes with GABARAPL2 and GIMAP7 to regulate GTPase activity. Also, GIMAP6 is induced by IFN-γ and plays a critical role in antibacterial immunity. Finally, we observed that Gimap6−/− mice died prematurely from microangiopathic glomerulosclerosis most likely due to GIMAP6 deficiency in kidney endothelial cells.

Published

2022

2. Human immunodeficiency reveals GIMAP5 as lymphocyte-specific regulator of senescence

Author

Elif Karakoc Aydine, Helen C. Su, John C. Pascall, Ann Y Park, Safa Baris, Silvia Vilarinho, Jahnavi Aluri, Aaron Morawski, Yu Zhang, Lixin Zheng, Rick P. Lifton, V. Koneti Rao, Sinan Sari, Ahmet Ozen, Helen F. Matthews, Brittany Chao, Isil Barlan, Xijin Xu, Michael Leney-Greene, Ping Jiang, Michael J. Lenardo, Geoff W. Butcher, Matthew Lynberg, and Ayca Kiykim

Subjects

Senescence, Lymphocyte, Spleen, Disease, mTORC1, Biology, medicine.disease, medicine.disease_cause, Autoimmunity, medicine.anatomical_structure, Immune system, Immunology, medicine, Immunodeficiency

Abstract

Elucidating the molecular basis of immunodeficiency diseases is a powerful approach to discovering new immunoregulatory pathways in humans. Here we report 10 affected individuals from 4 families with a new immunodeficiency disease comprising of severe progressive lymphopenia, autoimmunity, immunodeficiency, and liver disease due to recessive loss of function variants in “GTPase of immunity-associated proteins” protein 5 (GIMAP5). We show that the disease involves the progressive loss of naïve T lymphocytes and a corresponding increase in antigen-experienced, but poorly functional and replicatively senescent T cells. In vivo treatment of Gimap5-deficient mice with rapamycin (an inhibitor of mTORC1) significantly restores the fraction of naïve T lymphocytes. Furthermore, a GIMAP5-deficient human patient who was treated with rapamycin (sirolimus) showed a remarkable reduction in spleen/lymph node size. Together, these observations reveal that GIMAP5 plays a critical role in lymphocyte metabolism which is essential for senescence prevention and immune competence, suggesting that an inhibitor of mTORC1 could be a valuable clinical intervention in treating patients deficient for GIMAP5.

Published

2021

3. SCAMP3 is a mutant EGFR phosphorylation target and a tumor suppressor in lung adenocarcinoma

Author

Udayan Guha, Maryam Waris, Noelle Dayal, Asebot Abebe, Abhilash Venugopalan, Xu Zhang, Khoa Nguyen, Tapan K. Maity, Constance M. Cultraro, and Matthew Lynberg

Subjects

0301 basic medicine, Cancer Research, Adenocarcinoma of Lung, medicine.disease_cause, Article, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, Epidermal growth factor receptor, Phosphorylation, Lung cancer, Molecular Biology, Gene knockdown, biology, Phosphoproteomics, medicine.disease, ErbB Receptors, 030104 developmental biology, Membrane protein, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Carcinogenesis, Tyrosine kinase

Abstract

Mutations in the epidermal growth factor receptor (EGFR) tyrosine kinase domain constitutively activate EGFR resulting in lung tumorigenesis. Activated EGFR modulates downstream signaling by altering phosphorylation-driven interactions that promote growth and survival. Secretory carrier membrane proteins (SCAMPs) are a family of transmembrane proteins that regulate recycling of receptor proteins, including EGFR. The potential role of SCAMPs in mutant EGFR function and tumorigenesis has not been elucidated. Using quantitative mass-spectrometry-based phosphoproteomics, we identified SCAMP3 as a target of mutant EGFRs in lung adenocarcinoma and sought to further investigate the role of SCAMP3 in the regulation of lung tumorigenesis. Here we show that activated EGFR, either directly or indirectly phosphorylates SCAMP3 at Y86 and this phosphorylation increases the interaction of SCAMP3 with both wild-type and mutant EGFRs. SCAMP3 knockdown increases lung adenocarcinoma cell survival and increases xenograft tumor growth in vivo, demonstrating a tumor suppressor role of SCAMP3 in lung tumorigenesis. The tumor suppressor function is a result of SCAMP3 promoting EGFR degradation and attenuating MAP kinase signaling pathways. SCAMP3 knockdown also increases multinucleated cells in culture, suggesting that SCAMP3 is required for efficient cytokinesis. The enhanced growth, increased colony formation, reduced EGFR degradation and multinucleation phenotype of SCAMP3-depleted cells were reversed by re-expression of wild-type SCAMP3, but not SCAMP3 Y86F, suggesting that Y86 phosphorylation is critical for SCAMP3 function. Taken together, the results of this study demonstrate that SCAMP3 functions as a novel tumor suppressor in lung cancer by modulating EGFR signaling and cytokinesis that is partly Y86 phosphorylation-dependent.

Published

2020

4. Epigenetic Reprogramming Driven By Metabolic Alterations As A Mechanism Of EGFR – Tyrosine Kinase Inhibitor Resistance In Human Lung Adenocarcinoma

Author

Xu Zhang, Tapan K Maity, Abhilash Venugopalan, Daniel R. Crooks, Vikram Misra, Nitin Roper, Andrew N. Lane, Andresson Thorkell, King C. Chan, W. Marston Linehan, Udayan Guha, Khoa Dang Nguyen, Constance M. Cultraro, Yue Qi, and Matthew Lynberg

Subjects

Chemistry, Mechanism (biology), Inhibitor resistance, medicine.disease, Biochemistry, Human lung, medicine.anatomical_structure, Genetics, medicine, Cancer research, Adenocarcinoma, Molecular Biology, Reprogramming, Egfr tyrosine kinase, Biotechnology

Published

2020