Your search keyword '"Kaufman, Randal J"' showing total 12 results

1. The IRE1[alpha]/XBP1 pathway sustains cytokine responses of group 3 innate lymphoid cells in inflammatory bowel disease

Author

Cao, Siyan, Fachi, Jose L., Ma, Kaiming, Antonova, Alina Ulezko, Wang, Qianli, Cai, Zhangying, Kaufman, Randal J., Ciorba, Matthew A., Deepak, Parakkal, and Colonna, Marco

Subjects

Cytokines -- Analysis, Inflammatory bowel diseases -- Diagnosis -- Care and treatment, Inositol -- Dosage and administration, Disease susceptibility -- Analysis, Health care industry, Diagnosis, Care and treatment, Analysis, Dosage and administration

Abstract

Group 3 innate lymphoid cells (ILC3s) are key players in intestinal homeostasis. ER stress is linked to inflammatory bowel disease (IBD). Here, we used cell culture, mouse models, and human specimens to determine whether ER stress in ILC3s affects IBD pathophysiology. We show that mouse intestinal ILC3s exhibited a 24-hour rhythmic expression pattern of the master ER stress response regulator inositol-requiring kinase 1[alpha]/X-box-binding protein 1 (IRE1[alpha]/XBP1). Proinflammatory cytokine IL-23 selectively stimulated IRE1[alpha]/XBP1 in mouse ILC3s through mitochondrial ROS (mtROS). IRE1[alpha]/XBP1 was activated in ILC3s from mice exposed to experimental colitis and in inflamed human IBD specimens. Mice with Ire1[alpha] deletion in ILC3s ([Ire1[alpha].sup.[DELTA]Rorc]) showed reduced expression of the ER stress response and cytokine genes including Il22 in ILC3s and were highly vulnerable to infections and colitis. Administration of IL-22 counteracted their colitis susceptibility. In human ILC3s, IRE1 inhibitors suppressed cytokine production, which was upregulated by an IRE1 activator. Moreover, the frequencies of intestinal [XBP1s.sup.+] ILC3s in patients with Crohn's disease before administration of ustekinumab, an anti-IL-12/IL- 23 antibody, positively correlated with the response to treatment. We demonstrate that a noncanonical mtROS-IRE1[alpha]/XBP1 pathway augmented cytokine production by ILC3s and identify [XBP1s.sup.+] ILC3s as a potential biomarker for predicting the response to anti-IL-23 therapies in IBD., Introduction Innate lymphoid cells (ILCs) are a group of immune cells that exhibit lymphoid characteristics yet lack antigen-specific receptors found on T and B cells (1). Group 3 ILCs (ILC3s) [...]

Published

2024

2. ATF6 protects against protein misfolding during cardiac hypertrophy

Author

Hofmann, Christoph, Aghajani, Marjan, Alcock, Cecily D., Blackwood, Erik A., Sandmann, Clara, Herzog, Nicole, Groß, Julia, Plate, Lars, Wiseman, R. Luke, Kaufman, Randal J., Katus, Hugo A., Jakobi, Tobias, Völkers, Mirko, Glembotski, Christopher C., and Doroudgar, Shirin

Published

2024

3. TLR9-independent CD8+ T cell responses in hepatic AAV gene transfer through IL-1R1-MyD88 signaling

Author

Kumar, Sandeep R.P., Biswas, Moanaro, Cao, Di, Arisa, Sreevani, Muñoz-Melero, Maite, Lam, Anh K., Piñeros, Annie R., Kapur, Reuben, Kaisho, Tsuneyasu, Kaufman, Randal J., Xiao, Weidong, Shayakhmetov, Dmitry M., Terhorst, Cox, de Jong, Ype P., and Herzog, Roland W.

Published

2024

4. Conditional hepatocyte ablation of PDIA1 uncovers indispensable roles in both APOB and MTTP folding to support VLDL secretion

Author

Chen, Zhouji, Wang, Shiyu, Pottekat, Anita, Duffey, Alec, Jang, Insook, Chang, Benny H., Cho, Jaehyung, Finck, Brian N., Davidson, Nicholas O., and Kaufman, Randal J.

Published

2024

5. Impact of eIF2α phosphorylation on the translational landscape of mouse embryonic stem cells

Author

Amiri, Mehdi, Kiniry, Stephen J., Possemato, Anthony P., Mahmood, Niaz, Basiri, Tayebeh, Dufour, Catherine R., Tabatabaei, Negar, Deng, Qiyun, Bellucci, Michael A., Harwalkar, Keerthana, Stokes, Matthew P., Giguère, Vincent, Kaufman, Randal J., Yamanaka, Yojiro, Baranov, Pavel V., Tahmasebi, Soroush, and Sonenberg, Nahum

Published

2024

6. IRE1α Mediates the Hypertrophic Growth of Cardiomyocytes Through Facilitating the Formation of Initiation Complex to Promote the Translation of TOP-Motif Transcripts

Author

Li, Chao, primary, Li, Shiqian, additional, Zhang, Guangyu, additional, Li, Qinfeng, additional, Song, Weidan, additional, Wang, Xiaoding, additional, Cook, Jane A., additional, van der Stoel, Miesje, additional, Wright, Bradley W., additional, Altamirano, Francisco, additional, Niewold, Erica L., additional, Han, Jungsoo, additional, Kimble, Garrett, additional, Zhang, Pengfei, additional, Luo, Xiang, additional, Urra, Hery, additional, May, Herman I., additional, Ferdous, Anwarul, additional, Sun, Xue-Nan, additional, Deng, Yingfeng, additional, Ikonen, Elina, additional, Hetz, Claudio, additional, Kaufman, Randal J., additional, Zhang, Kezhong, additional, Gillette, Thomas G., additional, Scherer, Philipp E., additional, Hill, Joseph A., additional, Chen, Jin, additional, and Wang, Zhao V., additional

Published

2024

7. Proinsulin folding and trafficking defects trigger a common pathological disturbance of endoplasmic reticulum homeostasis.

Author

Arunagiri, Anoop, Alam, Maroof, Haataja, Leena, Draz, Hassan, Alasad, Bashiyer, Samy, Praveen, Sadique, Nadeed, Tong, Yue, Cai, Ying, Shakeri, Hadis, Fantuzzi, Federica, Ibrahim, Hazem, Jang, Insook, Sidarala, Vaibhav, Soleimanpour, Scott A., Satin, Leslie S., Otonkoski, Timo, Cnop, Miriam, Itkin‐Ansari, Pamela, and Kaufman, Randal J.

Abstract

Primary defects in folding of mutant proinsulin can cause dominant‐negative proinsulin accumulation in the endoplasmic reticulum (ER), impaired anterograde proinsulin trafficking, perturbed ER homeostasis, diminished insulin production, and β‐cell dysfunction. Conversely, if primary impairment of ER‐to‐Golgi trafficking (which also perturbs ER homeostasis) drives misfolding of nonmutant proinsulin—this might suggest bi‐directional entry into a common pathological phenotype (proinsulin misfolding, perturbed ER homeostasis, and deficient ER export of proinsulin) that can culminate in diminished insulin storage and diabetes. Here, we've challenged β‐cells with conditions that impair ER‐to‐Golgi trafficking, and devised an accurate means to assess the relative abundance of distinct folded/misfolded forms of proinsulin using a novel nonreducing SDS‐PAGE/immunoblotting protocol. We confirm abundant proinsulin misfolding upon introduction of a diabetogenic INS mutation, or in the islets of db/db mice. Whereas blockade of proinsulin trafficking in Golgi/post‐Golgi compartments results in intracellular accumulation of properly‐folded proinsulin (bearing native disulfide bonds), impairment of ER‐to‐Golgi trafficking (regardless whether such impairment is achieved by genetic or pharmacologic means) results in decreased native proinsulin with more misfolded proinsulin. Remarkably, reversible ER‐to‐Golgi transport defects (such as treatment with brefeldin A or cellular energy depletion) upon reversal quickly restore the ER folding environment, resulting in the disappearance of pre‐existing misfolded proinsulin while preserving proinsulin bearing native disulfide bonds. Thus, proper homeostatic balance of ER‐to‐Golgi trafficking is linked to a more favorable proinsulin folding (as well as trafficking) outcome. [ABSTRACT FROM AUTHOR]

Published

2024

8. TLR9-independent CD8+T cell responses in hepatic AAV gene transfer through IL-1R1-MyD88 signaling

Author

Kumar, Sandeep R.P., Biswas, Moanaro, Cao, Di, Arisa, Sreevani, Muñoz-Melero, Maite, Lam, Anh K., Piñeros, Annie R., Kapur, Reuben, Kaisho, Tsuneyasu, Kaufman, Randal J., Xiao, Weidong, Shayakhmetov, Dmitry M., Terhorst, Cox, de Jong, Ype P., and Herzog, Roland W.

Abstract

Upon viral infection of the liver, CD8+T cell responses may be triggered despite the immune suppressive properties that manifest in this organ. We sought to identify pathways that activate responses to a neoantigen expressed in hepatocytes, using adeno-associated viral (AAV) gene transfer. It was previously established that cooperation between plasmacytoid dendritic cells (pDCs), which sense AAV genomes by Toll-like receptor 9 (TLR9), and conventional DCs promotes cross-priming of capsid-specific CD8+T cells. Surprisingly, we find local initiation of a CD8+T cell response against antigen expressed in ∼20% of murine hepatocytes, independent of TLR9 or type I interferons and instead relying on IL-1 receptor 1-MyD88 signaling. Both IL-1α and IL-1β contribute to this response, which can be blunted by IL-1 blockade. Upon AAV administration, IL-1-producing pDCs infiltrate the liver and co-cluster with XCR1+DCs, CD8+T cells, and Kupffer cells. Analogous events were observed following coagulation factor VIII gene transfer in hemophilia A mice. Therefore, pDCs have alternative means of promoting anti-viral T cell responses and participate in intrahepatic immune cell networks similar to those that form in lymphoid organs. Combined TLR9 and IL-1 blockade may broadly prevent CD8+T responses against AAV capsid and transgene product.

Published

2024

9. 994 NANOSTRING GEOMX SPATIAL TRANSCRIPTOMIC ANALYSIS OF PANCREATIC ISLETS IN DIABETIC AND NONDIABETIC PANCREATIC CANCER PATIENTS REVEALS BETA CELL DEDIFFERENTIATION ASSOCIATED WITH ER STRESS PATHWAYS AND ALTERED LIPID METABOLISM

Author

Waldron, Richard T., Lugea, Aurelia, Yong, Jing, Muranaka, Hayato, Che, Mingtian, Ramanujan, V. Krishnan, Muzumdar, Mandar D., Kaufman, Randal J., and Pandol, Stephen J.

Published

2024

10. 991 RESTRAINING PANCREATIC DUCTAL ADENOCARCINOMA PROGRESSION WITH CHOP DEPLETION IN PANCREATIC EPITHELIAL CELLS

Author

Muranaka, Hayato, Yong, Jing, Waldron, Richard T., Aquino, Albert-Fred, Jang, Insook, Kaufman, Randal J., Pandol, Stephen J., and Lugea, Aurelia

Published

2024

11. Tapasin assembly surveillance by the RNF185/Membralin ubiquitin ligase complex regulates MHC-I surface expression.

Author

van de Weijer ML, Samanta K, Sergejevs N, Jiang L, Dueñas ME, Heunis T, Huang TY, Kaufman RJ, Trost M, Sanyal S, Cowley SA, and Carvalho P

Subjects

Humans, HEK293 Cells, Membrane Proteins metabolism, Membrane Proteins genetics, Membrane Transport Proteins metabolism, Membrane Transport Proteins genetics, Histocompatibility Antigens Class I metabolism, Histocompatibility Antigens Class I immunology, Ubiquitin-Protein Ligases metabolism, Ubiquitin-Protein Ligases genetics, Endoplasmic Reticulum-Associated Degradation, Antigen Presentation, Endoplasmic Reticulum metabolism

Abstract

Immune surveillance by cytotoxic T cells eliminates tumor cells and cells infected by intracellular pathogens. This process relies on the presentation of antigenic peptides by Major Histocompatibility Complex class I (MHC-I) at the cell surface. The loading of these peptides onto MHC-I depends on the peptide loading complex (PLC) at the endoplasmic reticulum (ER). Here, we uncovered that MHC-I antigen presentation is regulated by ER-associated degradation (ERAD), a protein quality control process essential to clear misfolded and unassembled proteins. An unbiased proteomics screen identified the PLC component Tapasin, essential for peptide loading onto MHC-I, as a substrate of the RNF185/Membralin ERAD complex. Loss of RNF185/Membralin resulted in elevated Tapasin steady state levels and increased MHC-I at the surface of professional antigen presenting cells. We further show that RNF185/Membralin ERAD complex recognizes unassembled Tapasin and limits its incorporation into PLC. These findings establish a novel mechanism controlling antigen presentation and suggest RNF185/Membralin as a potential therapeutic target to modulate immune surveillance., (© 2024. The Author(s).)

Published

2024

12. Proinsulin folding and trafficking defects trigger a common pathological disturbance of endoplasmic reticulum homeostasis.

Author

Arunagiri A, Alam M, Haataja L, Draz H, Alasad B, Samy P, Sadique N, Tong Y, Cai Y, Shakeri H, Fantuzzi F, Ibrahim H, Jang I, Sidarala V, Soleimanpour SA, Satin LS, Otonkoski T, Cnop M, Itkin-Ansari P, Kaufman RJ, Liu M, and Arvan P

Subjects

Mice, Animals, Proinsulin genetics, Proinsulin chemistry, Protein Folding, Insulin chemistry, Endoplasmic Reticulum, Homeostasis, Disulfides chemistry, Diabetes Mellitus, Insulin-Secreting Cells

Abstract

Primary defects in folding of mutant proinsulin can cause dominant-negative proinsulin accumulation in the endoplasmic reticulum (ER), impaired anterograde proinsulin trafficking, perturbed ER homeostasis, diminished insulin production, and β-cell dysfunction. Conversely, if primary impairment of ER-to-Golgi trafficking (which also perturbs ER homeostasis) drives misfolding of nonmutant proinsulin-this might suggest bi-directional entry into a common pathological phenotype (proinsulin misfolding, perturbed ER homeostasis, and deficient ER export of proinsulin) that can culminate in diminished insulin storage and diabetes. Here, we've challenged β-cells with conditions that impair ER-to-Golgi trafficking, and devised an accurate means to assess the relative abundance of distinct folded/misfolded forms of proinsulin using a novel nonreducing SDS-PAGE/immunoblotting protocol. We confirm abundant proinsulin misfolding upon introduction of a diabetogenic INS mutation, or in the islets of db/db mice. Whereas blockade of proinsulin trafficking in Golgi/post-Golgi compartments results in intracellular accumulation of properly-folded proinsulin (bearing native disulfide bonds), impairment of ER-to-Golgi trafficking (regardless whether such impairment is achieved by genetic or pharmacologic means) results in decreased native proinsulin with more misfolded proinsulin. Remarkably, reversible ER-to-Golgi transport defects (such as treatment with brefeldin A or cellular energy depletion) upon reversal quickly restore the ER folding environment, resulting in the disappearance of pre-existing misfolded proinsulin while preserving proinsulin bearing native disulfide bonds. Thus, proper homeostatic balance of ER-to-Golgi trafficking is linked to a more favorable proinsulin folding (as well as trafficking) outcome., (© 2024 The Authors. Protein Science published by Wiley Periodicals LLC on behalf of The Protein Society.)

Published

2024