Your search keyword '"Kaddis, John S."' showing total 3 results

1. Generation of human islet cell type-specific identity genesets.

Author

van Gurp, Léon, Fodoulian, Leon, Oropeza, Daniel, Furuyama, Kenichiro, Bru-Tari, Eva, Vu, Anh Nguyet, Kaddis, John S., Rodríguez, Iván, Thorel, Fabrizio, and Herrera, Pedro L.

Subjects

PANCREATIC beta cells, ISLANDS of Langerhans, EMBRYOLOGY, CELLULAR therapy, ISLANDS, HUMAN beings

Abstract

Generation of surrogate cells with stable functional identities is crucial for developing cell-based therapies. Efforts to produce insulin-secreting replacement cells to treat diabetes require reliable tools to assess islet cellular identity. Here, we conduct a thorough single-cell transcriptomics meta-analysis to identify robustly expressed markers used to build genesets describing the identity of human α-, β-, γ- and δ-cells. These genesets define islet cellular identities better than previously published genesets. We show their efficacy to outline cell identity changes and unravel some of their underlying genetic mechanisms, whether during embryonic pancreas development or in experimental setups aiming at developing glucose-responsive insulin-secreting cells, such as pluripotent stem-cell differentiation or in adult islet cell reprogramming protocols. These islet cell type-specific genesets represent valuable tools that accurately benchmark gain and loss in islet cell identity traits. Cell therapy to replace β-cells is a potential therapeutic avenue to treat diabetes, but the production of insulin-secreting replacement cells requires reliable tools to assess islet cellular identity. Here the authors use single-cell transcriptomics meta-analysis to construct gene sets that describe the identity of human α-, β-, γ- and δ-cells. [ABSTRACT FROM AUTHOR]

Published

2022

2. Chronic marijuana usage by human pancreas donors is associated with impaired islet function.

Author

Qi, Meirigeng, Kaddis, John S., Chen, Kuan-Tsen, Rawson, Jeffrey, Omori, Keiko, Chen, Zhen Bouman, Dhawan, Sangeeta, Isenberg, Jeffrey S., Kandeel, Fouad, Roep, Bart O., and Al-Abdullah, Ismail H.

Subjects

*ISLANDS of Langerhans, *ISLANDS, *PANCREATIC beta cells, *CANNABINOID receptors, *PANCREAS, *MARIJUANA, *INSULIN

Abstract

We investigated the effect of chronic marijuana use, defined as 4 times weekly for more than 3 years, on human pancreatic islets. Pancreata from deceased donors who chronically used marijuana were compared to those from age, sex and ethnicity matched non-users. The islets from marijuana-users displayed reduced insulin secretion as compared to islets from non-users upon stimulation with high glucose (AUC, 3.41 ± 0.62 versus 5.14 ±0.47, p<0.05) and high glucose plus KCl (AUC, 4.48 ± 0.41 versus 7.69 ± 0.58, p<0.001). When human islets from chronic marijuana-users were transplanted into diabetic mice, the mean reversal rate of diabetes was 35% versus 77% in animals receiving islets from non-users (p<0.01). Immunofluorescent staining for cannabinoid receptor type 1 (CB1R) was shown to be colocalized with insulin and enhanced significantly in beta cells from marijuana-users vs. non-users (CB1R intensity/islet area, 14.95 ± 2.71 vs. 3.23 ± 0.87, p<0.001). In contrast, CB1R expression was not co-localized with glucagon or somatostatin. Furthermore, isolated islets from chronic marijuana-users appeared hypertrophic. In conclusion, excessive marijuana use affects islet endocrine phenotype and function in vitro and in vivo. Given the increasing use of marijuana, our results underline the importance of including lifestyle when evaluating human islets for transplantation or research. [ABSTRACT FROM AUTHOR]

Published

2021

3. Human Pancreatic Islets and Diabetes Research.

Author

Kaddis, John S., Olack, Barbara J., Sowinski, Janice, Cravens, James, Contreras, Juan L., and Niland, Joyce C.

Subjects

*ISLANDS of Langerhans, *PANCREAS, *ENDOCRINE glands, *DIABETES, *RESEARCH institutes, *PANCREATIC beta cells

Abstract

The article presents an overview of the important role that human islet research plays in understanding the cellular biology of the pancreas and in developing therapeutic options for diabetics. A profile of the national Islet Cell Research Center Consortium, which provides human pancreatic islet cells for diabetes research and addresses the need to improve islet isolation and transplantation technologies, is offered. A discussion of the limitations of using human islets in diabetes research is presented.

Published

2009