Your search keyword '"Kay TW"' showing total 203 results

1. Investigating the efficacy of baricitinib in new onset type 1 diabetes mellitus (BANDIT)-study protocol for a phase 2, randomized, placebo controlled trial

Author

Waibel, M, Thomas, HE, Wentworth, JM, Couper, JJ, MacIsaac, RJ, Cameron, FJ, So, M, Krishnamurthy, B, Doyle, MC, Kay, TW, Waibel, M, Thomas, HE, Wentworth, JM, Couper, JJ, MacIsaac, RJ, Cameron, FJ, So, M, Krishnamurthy, B, Doyle, MC, and Kay, TW

Abstract

BACKGROUND: Type 1 diabetes (T1D) places an extraordinary burden on individuals and their families, as well as on the healthcare system. Despite recent advances in glucose sensors and insulin pump technology, only a minority of patients meet their glucose targets and face the risk of both acute and long-term complications, some of which are life-threatening. The JAK-STAT pathway is critical for the immune-mediated pancreatic beta cell destruction in T1D. Our pre-clinical data show that inhibitors of JAK1/JAK2 prevent diabetes and reverse newly diagnosed diabetes in the T1D non-obese diabetic mouse model. The goal of this study is to determine if the JAK1/JAK2 inhibitor baricitinib impairs type 1 diabetes autoimmunity and preserves beta cell function. METHODS: This will be as a multicentre, two-arm, double-blind, placebo-controlled randomized trial in individuals aged 10-30 years with recent-onset T1D. Eighty-three participants will be randomized in a 2:1 ratio within 100 days of diagnosis to receive either baricitinib 4mg/day or placebo for 48 weeks and then monitored for a further 48 weeks after stopping study drug. The primary outcome is the plasma C-peptide 2h area under the curve following ingestion of a mixed meal. Secondary outcomes include HbA1c, insulin dose, continuous glucose profile and adverse events. Mechanistic assessments will characterize general and diabetes-specific immune responses. DISCUSSION: This study will determine if baricitinib slows the progressive, immune-mediated loss of beta cell function that occurs after clinical presentation of T1D. Preservation of beta cell function would be expected to improve glucose control and prevent diabetes complications, and justify additional trials of baricitinib combined with other therapies and of its use in at-risk populations to prevent T1D. TRIAL REGISTRATION: ANZCTR ACTRN12620000239965 . Registered on 26 February 2020. CLINICALTRIALS: gov NCT04774224. Registered on 01 March 2021.

Published

2022

2. Australian experience with total pancreatectomy with islet autotransplantation to treat chronic pancreatitis

Author

Bampton, TJ, Holmes-Walker, DJ, Drogemuller, CJ, Radford, T, Anderson, P, Etherton, C, Russell, CH, Khurana, S, Torpy, DJ, Couper, JJ, Couper, RLT, Macintyre, P, Neo, EL, Benitez-Aguirre, P, Thomas, G, Loudovaris, T, Thomas, HE, Palmer, LJ, Wu, D, Rogers, NM, Williams, L, Hawthorne, WJ, O'Connell, PJ, Kay, TW, Pleass, H, Chen, JW, Coates, PT, Bampton, TJ, Holmes-Walker, DJ, Drogemuller, CJ, Radford, T, Anderson, P, Etherton, C, Russell, CH, Khurana, S, Torpy, DJ, Couper, JJ, Couper, RLT, Macintyre, P, Neo, EL, Benitez-Aguirre, P, Thomas, G, Loudovaris, T, Thomas, HE, Palmer, LJ, Wu, D, Rogers, NM, Williams, L, Hawthorne, WJ, O'Connell, PJ, Kay, TW, Pleass, H, Chen, JW, and Coates, PT

Abstract

BACKGROUND: This study aimed to describe the clinical outcomes of total pancreatectomy with islet autotransplantation (TP-IAT) in Australia. METHODS: Individuals selected for TP-IAT surgery according to the Minnesota Criteria (Appendix) without evidence of diabetes were evaluated including time to transplantation from pancreatectomy, islet numbers infused and post-transplantation HbA1c, C-peptide, total daily insulin and analgesic requirement. RESULTS: Sixteen individuals underwent TP-IAT from Australia and New Zealand between 2010 and 2020. Two recipients are deceased. The median islet equivalents/kg infused was 4244 (interquartile range (IQR) 2290-7300). The median C-peptide 1 month post-TP-IAT was 384 (IQR 210-579) pmol/L and at median 29.5 (IQR 14.5-46.5) months from transplant was 395 (IQR 139-862) pmol/L. Insulin independence was achieved in eight of 15 (53.3%) surviving recipients. A higher islet equivalents transplanted was most strongly associated with the likelihood of insulin independence (P < 0.05). Of the 15 surviving recipients, 14 demonstrated substantial reduction in analgesic requirement. CONCLUSION: The TP-IAT programme in Australia has been a successful new therapy for the management of individuals with chronic pancreatitis including hereditary forms refractory to medical treatment to improve pain management with 50% insulin independence rates.

Published

2021

3. South Australian experience with paediatric total pancreatectomy and islet autotransplantation for PRSS1-associated hereditary pancreatitis

Author

Eldredge, J, Couper, MR, Moore, DJ, Khurana, S, Chen, JWC, Couper, JJ, Drogemuller, CJ, Radford, T, Kay, TW, Loudovaris, T, Wilks, M, Coates, PT, Couper, RTL, Eldredge, J, Couper, MR, Moore, DJ, Khurana, S, Chen, JWC, Couper, JJ, Drogemuller, CJ, Radford, T, Kay, TW, Loudovaris, T, Wilks, M, Coates, PT, and Couper, RTL

Published

2021

4. OR32-06 Opportunistic Assessment of Pituitary Gland with Routine MRI and PET/CT Can Guide in Earlier and Increased Identification of Hypophysitis in Patients Treated with Combination Checkpoint Inhibitors

Author

Galligan, A, Iravani, A, Lasocki, A, Wallace, R, Weppler, A, Au-Yeung, G, Sachithanandan, N, Chiang, CY, Wentworth, J, Colman, PG, Kay, TW, Krishnamurthy, B, Sandhu, S, Galligan, A, Iravani, A, Lasocki, A, Wallace, R, Weppler, A, Au-Yeung, G, Sachithanandan, N, Chiang, CY, Wentworth, J, Colman, PG, Kay, TW, Krishnamurthy, B, and Sandhu, S

Abstract

Background: Hypophysitis is one of the commonly reported adverse events related to immune checkpoint inhibitors (ICI), and the incidence is expected to rise with increased use of combined programmed cell death protein 1 (PD1) and cytotoxic T lymphocyte associated protein 4 (CTLA4) blockade. The clinical diagnosis can be delayed due to non-specific symptoms. At our centre, subjects undergo periodic imaging to assess tumour response to ICI. We reviewed whether neuroimaging studies can guide us in the diagnosis of hypophysitis and whether early changes can be detected before the onset of the clinical syndrome. Methods: We retrospectively reviewed the medical charts, biochemistry, structural brain imaging and whole-body positron emission tomography (PET) with specific reference to hypophysitis in 162 patients treated with combination ICI at a tertiary melanoma referral centre. Suspected cases were identified based on meeting one or more of the following criteria: 1) A documented diagnosis of hypophysitis or pituitary dysfunction found on chart review, 2) A relative change in pituitary size or appearance from baseline on neuroimaging studies, or 3) An increase in pituitary maximum standardized uptake value (SUVmax) greater than 25% from baseline on 18F-FDG PET. Results: 58/162 patients (36%) met criteria for suspected hypophysitis. Only 4 patients were identified on routine screening of early morning cortisol. 14 patients presented with symptoms leading to biochemical work up. A further 40 patients were found to have suspicious imaging changes, 13 of which went on to receive a formal diagnosis of hypophysitis. Of the remaining 27 patients, 23 were receiving high dose glucocorticoids for concomitant immune related adverse events at the time of the abnormal imaging study.Conclusion: We report the highest incidence to date of suspected hypophysitis in cohort of patients treated with combination ICI. This study highlights the important role of structural and functio

Published

2020

5. SUN-127 Diagnostic Challenges Associated with the Rising Incidence of Endocrine Toxicity in the Era of Combination Immunotherapy

Author

Galligan, A, Iravani, A, Lasocki, A, Wallace, R, Weppler, A, Au-Yeung, G, Sachithanandan, N, Chiang, CY, Wentworth, J, Colman, PG, Kay, TW, Krishnamurthy, B, Sandhu, S, Galligan, A, Iravani, A, Lasocki, A, Wallace, R, Weppler, A, Au-Yeung, G, Sachithanandan, N, Chiang, CY, Wentworth, J, Colman, PG, Kay, TW, Krishnamurthy, B, and Sandhu, S

Abstract

Background: Immune checkpoint blockade is now established as standard of care in several malignancies. Trials involving combined cytotoxic T lymphocyte associated protein 4 (CTLA4) and programmed cell death protein 1 (PD1) blockade demonstrate improved tumour responses in melanoma but at the cost of severe grade 3-4 immune related adverse events (irAEs) in 55%, and endocrine irAEs in up to 10% [1]. Immune-mediated damage to endocrine glands can be a diagnostic and management challenge. We aimed to review the incidence, biochemical evolution and imaging findings of endocrine toxicity related to combined anti CTLA-4 and anti-PD-1 therapy. Methods: We undertook a retrospective chart review of patients who received combined ipilimumab and nivolumab for metastatic melanoma at a tertiary referral centre between 2016-2019. We recorded onset and duration of abnormal biochemistry in endocrine irAEs, reviewed all available MRI images for pituitary size (mm) and appearance and 18-F FDG PET images for features of hypophysitis, thyroiditis and pancreatitis. Results: 162 patients received combination therapy. At least one irAE was recorded in 135 patients (83%), 100 (62%) required glucocorticoids, and 84 (52%) had an unplanned hospital presentation due to irAEs. Thyroiditis occurred in 50 (30.9%), with median time to onset of 30.9 days (range 1-234 days). 35 cases were identified with routine biochemistry performed every 4-6 weeks. TSH receptor antibody was measured in 13 patients and all were negative. 29 (58%) developed permanent hypothyroidism. Central cortisol deficiency was documented in 31 (19%) with a median time to diagnosis of 67.5 days (range 5-286). 4 cases were diagnosed on routine biochemistry and 14 presented with symptoms prompting investigation. 13 were diagnosed after routine neuroimaging demonstrated a pituitary abnormality, and a further 27 patients without the clinical syndrome had features of hypophysitis on neuroimaging. New onset diabetes occurred

Published

2020

6. Opportunistic Assessment of Pituitary Gland with Routine MRI and PET/CT Can Guide in Earlier and Increased Identification of Hypophysitis in Patients Treated with Combination Checkpoint Inhibitors

Author

Galligan, A, Iravani, A, Lasocki, A, Wallace, R, Weppler, A, Au-Yeung, G, Sachithanandan, N, Chiang, CY, Wentworth, J, Colman, PG, Kay, TW, Krishnamurthy, B, Sandhu, S, Galligan, A, Iravani, A, Lasocki, A, Wallace, R, Weppler, A, Au-Yeung, G, Sachithanandan, N, Chiang, CY, Wentworth, J, Colman, PG, Kay, TW, Krishnamurthy, B, and Sandhu, S

Abstract

Background: Hypophysitis is one of the commonly reported adverse events related to immune checkpoint inhibitors (ICI), and the incidence is expected to rise with increased use of combined programmed cell death protein 1 (PD1) and cytotoxic T lymphocyte associated protein 4 (CTLA4) blockade. The clinical diagnosis can be delayed due to non-specific symptoms. At our centre, subjects undergo periodic imaging to assess tumour response to ICI. We reviewed whether neuroimaging studies can guide us in the diagnosis of hypophysitis and whether early changes can be detected before the onset of the clinical syndrome. Methods: We retrospectively reviewed the medical charts, biochemistry, structural brain imaging and whole-body positron emission tomography (PET) with specific reference to hypophysitis in 162 patients treated with combination ICI at a tertiary melanoma referral centre. Suspected cases were identified based on meeting one or more of the following criteria: 1) A documented diagnosis of hypophysitis or pituitary dysfunction found on chart review, 2) A relative change in pituitary size or appearance from baseline on neuroimaging studies, or 3) An increase in pituitary maximum standardized uptake value (SUVmax) greater than 25% from baseline on 18F-FDG PET. Results: 58/162 patients (36%) met criteria for suspected hypophysitis. Only 4 patients were identified on routine screening of early morning cortisol. 14 patients presented with symptoms leading to biochemical work up. A further 40 patients were found to have suspicious imaging changes, 13 of which went on to receive a formal diagnosis of hypophysitis. Of the remaining 27 patients, 23 were receiving high dose glucocorticoids for concomitant immune related adverse events at the time of the abnormal imaging study.Conclusion: We report the highest incidence to date of suspected hypophysitis in cohort of patients treated with combination ICI. This study highlights the important role of structural and functional neuro

Published

2020

7. Australia and New Zealand Islet and Pancreas Transplant Registry Annual Report 2018-Islet Donations, Islet Isolations, and Islet Transplants

Author

Webster, AC, Hedley, JA, Anderson, PF, Hawthorne, WJ, Radford, T, Drogemuller, C, Rogers, N, Goodman, D, Lee, MH, Loudovaris, T, Kelly, PJ, O'Connell, PJ, Holmes-Walker, DJ, Kay, TW, MacIsaac, RJ, Ward, GM, Howe, MK, Coates, PT, Torpy, D, Roberts, A, Russell, C, Olakkengil, S, Webster, AC, Hedley, JA, Anderson, PF, Hawthorne, WJ, Radford, T, Drogemuller, C, Rogers, N, Goodman, D, Lee, MH, Loudovaris, T, Kelly, PJ, O'Connell, PJ, Holmes-Walker, DJ, Kay, TW, MacIsaac, RJ, Ward, GM, Howe, MK, Coates, PT, Torpy, D, Roberts, A, Russell, C, and Olakkengil, S

Abstract

BACKGROUND: This is an excerpt from chapter 4 of the annual registry report from the Australia and New Zealand islet and pancreas transplant registry. The full report is available at http://anziptr.org/reports/. METHODS: We report data for all allogeneic islet isolation and transplant activity from 2002 to end 2017. Solid organ pancreas transplantation activity is reported separately. New Zealand does not have an islet transplant program. Data analysis was performed using Stata software version 14 (StataCorp, College Station, TX). RESULTS: From 2002 to 2017, a total of 104 allogeneic islet transplants were performed in 62 recipients. CONCLUSIONS: The number of islet transplants performed in Australia was slightly lower in 2017 but continues to increase over time.

Published

2019

8. Mortality in People With Type 1 Diabetes, Severe Hypoglycemia, and Impaired Awareness of Hypoglycemia Referred for Islet Transplantation

Author

Lee, MH, Ward, GM, MacIsaac, RJ, Howe, K, Holmes-Walker, DJ, Anderson, P, Radford, T, Coates, PT, Kay, TW, O'Connell, PJ, Goodman, DJ, Lee, MH, Ward, GM, MacIsaac, RJ, Howe, K, Holmes-Walker, DJ, Anderson, P, Radford, T, Coates, PT, Kay, TW, O'Connell, PJ, and Goodman, DJ

Published

2018

9. Cognate antigen engagement on parenchymal cells stimulates CD8+ T cell proliferation in situ

Author

Sutherland, RM, Londrigan, SL, Brady, JL, Carrington, EM, Marchingo, JM, Heinzel, S, Hodgkin, PD, Graham, KL, Kay, TW, Zhan, Y, Lew, AM, Sutherland, RM, Londrigan, SL, Brady, JL, Carrington, EM, Marchingo, JM, Heinzel, S, Hodgkin, PD, Graham, KL, Kay, TW, Zhan, Y, and Lew, AM

Abstract

T-cell responses are initiated upon cognate presentation by professional antigen presenting cells in lymphoid tissue. T cells then migrate to inflamed tissues, but further T-cell stimulation in these parenchymal target sites is not well understood. Here we show that T-cell expansion within inflamed tissues is a distinct phase that is neither a classical primary nor classical secondary response. This response, which we term 'the mezzanine response', commences within days after initial antigen encounter, unlike the secondary response that usually occurs weeks after priming. A further distinction of this response is that T-cell proliferation is driven by parenchymal cell antigen presentation, without requiring professional antigen presenting cells, but with increased dependence on IL-2. The mezzanine response might, therefore, be a new target for inhibiting T-cell responses in allograft rejection and autoimmunity or for enhancing T-cell responses in the context of microbial or tumour immunity.

Published

2017

10. Transplantation sites for human and murine islets

Author

Stokes, RA, Cheng, K, Lalwani, A, Swarbrick, MM, Thomas, HE, Loudovaris, T, Kay, TW, Hawthorne, WJ, O'Connell, PJ, Gunton, JE, Stokes, RA, Cheng, K, Lalwani, A, Swarbrick, MM, Thomas, HE, Loudovaris, T, Kay, TW, Hawthorne, WJ, O'Connell, PJ, and Gunton, JE

Abstract

AIMS/HYPOTHESIS: Beta cell replacement is a potential cure for type 1 diabetes. In humans, islet transplants are currently infused into the liver via the portal vein, although this site has disadvantages. Here, we investigated alternative transplantation sites for human and murine islets in recipient mice, comparing the portal vein with quadriceps muscle and kidney, liver and spleen capsules. METHODS: Murine islets were isolated from C57BL6/J mice and transplanted into syngeneic recipients. Human islets were isolated and transplanted into either severe combined immunodeficiency (SCID) or recombination-activating gene 1 (RAG-1) immunodeficient recipient mice. All recipient mice were 8-12 weeks of age and had been rendered diabetic (defined as blood glucose concentrations ≥20 mmol/l on two consecutive days before transplantation) by alloxan tetrahydrate treatment. Islets were transplanted into five different sites (portal vein, quadriceps muscle, kidney, liver and spleen capsules). Blood glucose concentrations were monitored twice weekly until mice were killed. Dose-response studies were also performed to determine the minimum number of islets required to cure diabetes ('cure' is defined for this study as random fed blood glucose of <15 mmol/l). RESULTS: For transplantation of murine islets into the different sites, the kidney yielded 100% success, followed by muscle (70%), portal vein (60%), spleen capsule (29%) and liver capsule (0%). For human islets, transplantation into the kidney cured diabetes in 75-80% of recipient mice. Transplantation into muscle and portal vein had intermediate success (both 29% at 2000 islet equivalents), while transplantation into liver and spleen capsule failed (0%). With increased islet mass, success rates for muscle grafts improved to 52-56%. CONCLUSIONS/INTERPRETATION: For both human and murine islets, equivalent or superior glucose lowering results were obtained for transplantation into skeletal muscle, compared with the portal vein.

Published

2017

11. Improving outcomes in clinical islet transplantation: 1999-2010

Author

Barton, FB, Rickels, MR, Alejandro, R, Hering, BJ, Wease, S, Naziruddin, B, Oberholzer, J, Odorico, JS, Garfinkel, MR, Levy, M, Pattou, F, Berney, T, Messinger, S, Senior, PA, Maffi, P, Posselt, A, Stock, PG, Kaufman, DB, Luo, X, Kandeel, F, Cagliero, E, Turgeon, NA, Witkowski, P, Naji, A, O'Connell, PJ, Greenbaum, C, Kudva, YC, Brayman, KL, Aull, MJ, Larsen, C, Kay, TW, Fernandez, LA, Vantyghem, MC, Bellin, M, Shapiro, AM, SECCHI , ANTONIO, Barton, Fb, Rickels, Mr, Alejandro, R, Hering, Bj, Wease, S, Naziruddin, B, Oberholzer, J, Odorico, J, Garfinkel, Mr, Levy, M, Pattou, F, Berney, T, Secchi, Antonio, Messinger, S, Senior, Pa, Maffi, P, Posselt, A, Stock, Pg, Kaufman, Db, Luo, X, Kandeel, F, Cagliero, E, Turgeon, Na, Witkowski, P, Naji, A, O'Connell, Pj, Greenbaum, C, Kudva, Yc, Brayman, Kl, Aull, Mj, Larsen, C, Kay, Tw, Fernandez, La, Vantyghem, Mc, Bellin, M, and Shapiro, Am

Abstract

OBJECTIVEdTo describe trends of primary efficacy and safety outcomes of islet transplantationin type 1 diabetes recipients with severe hypoglycemia from the Collaborative Islet TransplantRegistry (CITR) from 1999 to 2010.RESEARCH DESIGN AND METHODSdA total of 677 islet transplant-alone or isletafter-kidney recipients with type 1 diabetes in the CITR were analyzed for five primary efficacyoutcomes and overall safety to identify any differences by early (1999–2002), mid (2003–2006),or recent (2007–2010) transplant era based on annual follow-up to 5 years.RESULTSdInsulin independence at 3 years after transplant improved from 27% in the early era(1999–2002, n = 214) to 37% in the mid (2003–2006, n = 255) and to 44% in the most recent era(2007–2010, n = 208; P = 0.006 for years-by-era; P = 0.01 for era alone). C-peptide $0.3 ng/mL,indicative of islet graft function,was retained longer in themost recent era (P,0.001). Reduction ofHbA1c and resolution of severe hypoglycemia exhibited enduring long-term effects. Fasting bloodglucose stabilization also showed improvements in the most recent era. There were also modestreductions in the occurrence of adverse events. The islet reinfusion rate was lower: 48% by 1 yearin 2007–2010 vs. 60–65% in 1999–2006 (P , 0.01). Recipients that ever achieved insulinindependenceexperienced longer duration of islet graft function (P , 0.001).CONCLUSIONSdThe CITR shows improvement in primary efficacy and safety outcomes ofislet transplantation in recipients who received transplants in 2007–2010 compared with thosein 1999–2006, with fewer islet infusions and adverse events per recipient.

Published

2012

12. Evidence-Informed Clinical Practice Recommendations for Treatment of Type 1 Diabetes Complicated by Problematic Hypoglycemia

Author

Choudhary, P, Rickels, MR, Senior, PA, Vantyghem, M-C, Maffi, P, Kay, TW, Keymeulen, B, Inagaki, N, Saudek, F, Lehmann, R, Hering, BJ, Choudhary, P, Rickels, MR, Senior, PA, Vantyghem, M-C, Maffi, P, Kay, TW, Keymeulen, B, Inagaki, N, Saudek, F, Lehmann, R, and Hering, BJ

Abstract

Problematic hypoglycemia, defined as two or more episodes per year of severe hypoglycemia or as one episode associated with impaired awareness of hypoglycemia, extreme glycemic lability, or major fear and maladaptive behavior, is a challenge, especially for patients with long-standing type 1 diabetes. Individualized therapy for such patients should include a composite target: optimal glucose control without problematic hypoglycemia. Therefore, we propose a tiered, four-stage algorithm based on evidence of efficacy given the limitations of educational, technological, and transplant interventions. All patients with problematic hypoglycemia should undergo structured or hypoglycemia-specific education programs (stage 1). Glycemic and hypoglycemia treatment targets should be individualized and reassessed every 3-6 months. If targets are not met, one diabetes technology-continuous subcutaneous insulin infusion or continuous glucose monitoring-should be added (stage 2). For patients with continued problematic hypoglycemia despite education (stage 1) and one diabetes technology (stage 2), sensor-augmented insulin pumps preferably with an automated low-glucose suspend feature and/or very frequent contact with a specialized hypoglycemia service can reduce hypoglycemia (stage 3). For patients whose problematic hypoglycemia persists, islet or pancreas transplant should be considered (stage 4). This algorithm provides an evidence-informed approach to resolving problematic hypoglycemia; it should be used as a guide, with individual patient circumstances directing suitability and acceptability to ensure the prudent use of technology and scarce transplant resources. Standardized reporting of hypoglycemia outcomes and inclusion of patients with problematic hypoglycemia in studies of new interventions may help to guide future therapeutic strategies.

Published

2015

13. Granzyme B Is Dispensable in the Development of Diabetes in Non-Obese Diabetic Mice

Author

Chatenoud, L, Mollah, ZU, Graham, KL, Krishnamurthy, B, Trivedi, P, Brodnicki, TC, Trapani, JA, Kay, TW, Thomas, HE, Chatenoud, L, Mollah, ZU, Graham, KL, Krishnamurthy, B, Trivedi, P, Brodnicki, TC, Trapani, JA, Kay, TW, and Thomas, HE

Abstract

Pancreatic beta cell destruction in type 1 diabetes is mediated by cytotoxic CD8(+) T lymphoctyes (CTL). Granzyme B is an effector molecule used by CTL to kill target cells. We previously showed that granzyme B-deficient allogeneic CTL inefficiently killed pancreatic islets in vitro. We generated granzyme B-deficient non-obese diabetic (NOD) mice to test whether granzyme B is an important effector molecule in spontaneous type 1 diabetes. Granzyme B-deficient islet antigen-specific CD8(+) T cells had impaired homing into islets of young mice. Insulitis was reduced in granzyme B-deficient mice at 70 days of age (insulitis score 0.043±0.019 in granzyme B-deficient versus 0.139±0.034 in wild-type NOD mice p<0.05), but was similar to wild-type at 100 and 150 days of age. We observed a reduced frequency of CD3(+)CD8(+) T cells in the islets and peripheral lymphoid tissues of granzyme B-deficient mice (p<0.005 and p<0.0001 respectively), but there was no difference in cell proportions in the thymus. Antigen-specific CTL developed normally in granzyme B-deficient mice, and were able to kill NOD islet target cells as efficiently as wild-type CTL in vitro. The incidence of spontaneous diabetes in granzyme B-deficient mice was the same as wild-type NOD mice. We observed a delayed onset of diabetes in granzyme B-deficient CD8-dependent NOD8.3 mice (median onset 102.5 days in granzyme B-deficient versus 57.50 days in wild-type NOD8.3 mice), which may be due to the delayed onset of insulitis or inefficient priming at an earlier age in this accelerated model of diabetes. Our data indicate that granzyme B is dispensable for beta cell destruction in type 1 diabetes, but is required for efficient early activation of CTL.

Published

2012

14. Islet beta-Cells Deficient in Bcl-xL Develop but Are Abnormally Sensitive to Apoptotic Stimuli

Author

Carrington, EM, McKenzie, MD, Jansen, E, Myers, M, Fynch, S, Kos, C, Strasser, A, Kay, TW, Scott, CL, Allison, J, Carrington, EM, McKenzie, MD, Jansen, E, Myers, M, Fynch, S, Kos, C, Strasser, A, Kay, TW, Scott, CL, and Allison, J

Abstract

OBJECTIVE: Bcl-xL is an antiapoptotic member of the Bcl-2 family of proteins and a potent regulator of cell death. We investigated the importance of Bcl-xL for beta-cells by deleting the Bcl-x gene specifically in beta-cells and analyzing their survival in vivo and in culture. RESEARCH DESIGN AND METHODS: Islets with beta-cells lacking the Bcl-x gene were assessed in vivo by histology and by treatment of mice with low-dose streptozotocin (STZ). Islets were isolated by collagenase digestion and treated in culture with the apoptosis inducers staurosporine, thapsigargin, gamma-irradiation, proinflammatory cytokines, or Fas ligand. Cell death was assessed by flow cytometric analysis of subgenomic DNA. RESULTS: Bcl-xL-deficient beta-cells developed but were abnormally sensitive to apoptosis induced in vivo by low-dose STZ. Although a small proportion of beta-cells still expressed Bcl-xL, these did not have a survival advantage over their Bcl-xL-deficient neighbors. Islets appeared normal after collagenase isolation and whole-islet culture. They were, however, abnormally sensitive in culture to a number of different apoptotic stimuli including cytotoxic drugs, proinflammatory cytokines, and Fas ligand. CONCLUSIONS: Bcl-xL expression in beta-cells is dispensible during islet development in the mouse. Bcl-xL is, however, an important regulator of beta-cell death under conditions of synchronous stress. Bcl-xL expression at physiological levels may partially protect beta-cells from apoptotic stimuli, including apoptosis because of mediators implicated in type 1 diabetes and death or degeneration of transplanted islets.

Published

2009

15. Lack of expression of Gp-130 makes pancreatic beta cell lines unresponsive to the IL-6 family of cytokines.

Author

Naselli, G, Deaizpurua, HJ, Thomas, HE, Johnston, AM, Kay, TW, Naselli, G, Deaizpurua, HJ, Thomas, HE, Johnston, AM, and Kay, TW

Abstract

Cytokine receptors from the IL-6 receptor family are comprised of ligand specific alpha chains and a common signalling chain, gp-130, which is also required for high affinity binding. A cDNA library generated from the beta-TC3 SV40 T-antigen transformed insulinoma cell line was screened for members of this receptor family potentially relevant to both beta cell development and autoimmunity. Degenerate oligonucleotide primers to a consensus region of these receptors were used and the IL-11 receptor alpha chain was identified. Despite confirmation of IL-11 receptor mRNA expression, iodinated bioactive IL-11 did not bind specifically to beta-TC3 cells and gp-130-dependent cytokines did not elicit signalling events in beta cell lines. This was explained by absence of gp-130 protein or mRNA in the beta cell lines tested and in primary islets. We conclude from these results that the previously recognised effects of IL-6 family member cytokines on pancreatic islets must be indirect via other non-beta cells within the islet, rather than due to direct effects on beta cells themselves.

Published

2001

16. Granulocyte macrophage colony-stimulating factor: A new putative therapeutic target in multiple sclerosis

Author

McQualter, JL, Darwiche, R, Ewing, C, Onuki, M, Kay, TW, Hamilton, JA, Reid, HH, Bernard, CCA, McQualter, JL, Darwiche, R, Ewing, C, Onuki, M, Kay, TW, Hamilton, JA, Reid, HH, and Bernard, CCA

Abstract

Experimental autoimmune encephalomyelitis (EAE), a model for multiple sclerosis, can be induced by immunization with a number of myelin antigens. In particular, myelin oligodendrocyte glycoprotein, a central nervous system (CNS)-specific antigen expressed on the myelin surface, is able to induce a paralytic MS-like disease with extensive CNS inflammation and demyelination in several strains of animals. Although not well understood, the egress of immune cells into the CNS in EAE is governed by a complex interplay between pro and antiinflammatory cytokines and chemokines. The hematopoietic growth factor, granulocyte macrophage colony-stimulating factor (GM-CSF), is considered to play a central role in maintaining chronic inflammation. The present study was designed to investigate the previously unexplored role of GM-CSF in autoimmune-mediated demyelination. GM-CSF(-/)- mice are resistant to EAE, display decreased antigen-specific proliferation of splenocytes, and fail to sustain immune cell infiltrates in the CNS, thus revealing key activities for GM-CSF in the development of inflammatory demyelinating lesions and control of migration and/or proliferation of leukocytes within the CNS. These results hold implications for the pathogenesis of inflammatory and demyelinating diseases and may provide the basis for more effective therapies for inflammatory diseases, and more specifically for multiple sclerosis.

Published

2001

17. Advanced glycation end products are direct modulators of β-cell function.

Author

Coughlan MT, Yap FY, Tong DC, Andrikopoulos S, Gasser A, Thallas-Bonke V, Webster DE, Miyazaki J, Kay TW, Slattery RM, Kaye DM, Drew BG, Kingwell BA, Fourlanos S, Groop PH, Harrison LC, Knip M, Forbes JM, Coughlan, Melinda T, and Yap, Felicia Y T

Subjects

ANIMAL experimentation, CELLS, TYPE 1 diabetes, ISLANDS of Langerhans, MICE, ORGANIC compounds, RATS

Abstract

Objective: Excess accumulation of advanced glycation end products (AGEs) contributes to aging and chronic diseases. We aimed to obtain evidence that exposure to AGEs plays a role in the development of type 1 diabetes (T1D).Research Design and Methods: The effect of AGEs was examined on insulin secretion by MIN6N8 cells and mouse islets and in vivo in three separate rodent models: AGE-injected or high AGE-fed Sprague-Dawley rats and nonobese diabetic (NODLt) mice. Rodents were also treated with the AGE-lowering agent alagebrium.Results: β-Cells exposed to AGEs displayed acute glucose-stimulated insulin secretory defects, mitochondrial abnormalities including excess superoxide generation, a decline in ATP content, loss of MnSOD activity, reduced calcium flux, and increased glucose uptake, all of which were improved with alagebrium treatment or with MnSOD adenoviral overexpression. Isolated mouse islets exposed to AGEs had decreased glucose-stimulated insulin secretion, increased mitochondrial superoxide production, and depletion of ATP content, which were improved with alagebrium or with MnTBAP, an SOD mimetic. In rats, transient or chronic exposure to AGEs caused progressive insulin secretory defects, superoxide generation, and β-cell death, ameliorated with alagebrium. NODLt mice had increased circulating AGEs in association with an increase in islet mitochondrial superoxide generation, which was prevented by alagebrium, which also reduced the incidence of autoimmune diabetes. Finally, at-risk children who progressed to T1D had higher AGE concentrations than matched nonprogressors.Conclusions: These findings demonstrate that AGEs directly cause insulin secretory defects, most likely by impairing mitochondrial function, which may contribute to the development of T1D. [ABSTRACT FROM AUTHOR]

Published

2011

18. Interleukin-1β produced in response to islet autoantigen presentation differentiates T-helper 17 cells at the expense of regulatory T-cells: Implications for the timing of tolerizing immunotherapy.

Author

Bertin-Maghit S, Pang D, O'Sullivan B, Best S, Duggan E, Paul S, Thomas H, Kay TW, Harrison LC, Steptoe R, Thomas R, Bertin-Maghit, Sebastien, Pang, Dimeng, O'Sullivan, Brendan, Best, Shannon, Duggan, Emily, Paul, Sanjoy, Thomas, Helen, Kay, Thomas W H, and Harrison, Leonard C

Abstract

Objective: The effectiveness of tolerizing immunotherapeutic strategies, such as anti-CD40L or dendritic cells (DCs), is greater when administered to young nonobese diabetic (NOD) mice than at peak insulitis. RelB(lo) DCs, generated in the presence of an nuclear factor-κB inhibitor, induce T-regulatory (Treg) cells and suppress inflammation in a model of rheumatoid arthritis. Interleukin (IL)-1β is overexpressed in humans and mice at risk of type 1 diabetes, dysregulates Treg cells, and accelerates diabetes in NOD mice. We investigated the relationship between IL-1β production and the response to RelB(lo) DCs in the prediabetic period.Research Design and Methods: We injected RelB(lo) DCs subcutaneously into 4- or 14-week-old NOD mice and tracked the incidence of diabetes and effect on Treg cell function. We measured the expression of proinflammatory cytokines by stimulated splenocytes and unstimulated islets from mice of different ages and strains and proliferative and cytokine responses of T effectors to Treg in vitro.Results: Tolerizing RelB(lo) DCs significantly inhibited diabetes progression when administered to 4-week-old but not 14-week-old mice. IL-1β production by NOD splenocytes and mRNA expression by islets increased from 6 to 16 weeks of age when major histocompatibility complex (MHC)-restricted islet antigen presentation to autoreactive T-cells occurred. IL-1 reduced the capacity of Treg cells to suppress effector cells and promoted their conversion to Th17 cells. RelB(lo) DCs exacerbated the IL-1-dependent decline in Treg function and promoted Th17 conversion.Conclusions: IL-1β, generated by islet-autoreactive cells in MHC-susceptible mice, accelerates diabetes by differentiating Th17 at the expense of Treg. Tolerizing DC therapies can regulate islet autoantigen priming and prevent diabetes, but progression past the IL-1β/IL-17 checkpoint signals the need for other strategies. [ABSTRACT FROM AUTHOR]

Published

2011

19. Islet beta-cells deficient in Bcl-xL develop but are abnormally sensitive to apoptotic stimuli.

Author

Carrington EM, McKenzie MD, Jansen E, Myers M, Fynch S, Kos C, Strasser A, Kay TW, Scott CL, Allison J, Carrington, Emma M, McKenzie, Mark D, Jansen, Elisa, Myers, Michelle, Fynch, Stacey, Kos, Cameron, Strasser, Andreas, Kay, Thomas W, Scott, Clare L, and Allison, Janette

Abstract

Objective: Bcl-xL is an antiapoptotic member of the Bcl-2 family of proteins and a potent regulator of cell death. We investigated the importance of Bcl-xL for beta-cells by deleting the Bcl-x gene specifically in beta-cells and analyzing their survival in vivo and in culture.Research Design and Methods: Islets with beta-cells lacking the Bcl-x gene were assessed in vivo by histology and by treatment of mice with low-dose streptozotocin (STZ). Islets were isolated by collagenase digestion and treated in culture with the apoptosis inducers staurosporine, thapsigargin, gamma-irradiation, proinflammatory cytokines, or Fas ligand. Cell death was assessed by flow cytometric analysis of subgenomic DNA.Results: Bcl-xL-deficient beta-cells developed but were abnormally sensitive to apoptosis induced in vivo by low-dose STZ. Although a small proportion of beta-cells still expressed Bcl-xL, these did not have a survival advantage over their Bcl-xL-deficient neighbors. Islets appeared normal after collagenase isolation and whole-islet culture. They were, however, abnormally sensitive in culture to a number of different apoptotic stimuli including cytotoxic drugs, proinflammatory cytokines, and Fas ligand.Conclusions: Bcl-xL expression in beta-cells is dispensible during islet development in the mouse. Bcl-xL is, however, an important regulator of beta-cell death under conditions of synchronous stress. Bcl-xL expression at physiological levels may partially protect beta-cells from apoptotic stimuli, including apoptosis because of mediators implicated in type 1 diabetes and death or degeneration of transplanted islets. [ABSTRACT FROM AUTHOR]

Published

2009

20. Cytotoxic T-cells from T-cell receptor transgenic NOD8.3 mice destroy beta-cells via the perforin and Fas pathways.

Author

Dudek NL, Thomas HE, Mariana L, Sutherland RM, Allison J, Estella E, Angstetra E, Trapani JA, Santamaria P, Lew AM, Kay TW, Dudek, Nadine L, Thomas, Helen E, Mariana, Lina, Sutherland, Robyn M, Allison, Janette, Estella, Eugene, Angstetra, Eveline, Trapani, Joseph A, and Santamaria, Pere

Abstract

Cytotoxic T-cells are the major mediators of beta-cell destruction in type 1 diabetes, but the molecular mechanisms are not definitively established. We have examined the contribution of perforin and Fas ligand to beta-cell destruction using islet-specific CD8(+) T-cells from T-cell receptor transgenic NOD8.3 mice. NOD8.3 T-cells killed Fas-deficient islets in vitro and in vivo. Perforin-deficient NOD8.3 T-cells were able to destroy wild-type but not Fas-deficient islets in vitro. These results imply that NOD8.3 T-cells use both pathways and that Fas is required for beta-cell killing only when perforin is missing. Consistent with this theory, transgenic NOD8.3 mice with beta-cells that do not respond to Fas ligation were not protected from diabetes. We next investigated the mechanism of protection provided by overexpression of suppressor of cytokine signaling-1 (SOCS-1) in beta-cells of NOD8.3 mice. SOCS-1 islets remained intact when grafted into NOD8.3 mice and were less efficiently killed in vitro. However, addition of exogenous peptide rendered SOCS-1 islets susceptible to 8.3 T-cell-mediated lysis. Therefore, NOD8.3 T-cells use both perforin and Fas pathways to kill beta-cells and the surprising blockade of NOD8.3 T-cell-mediated beta-cell death by SOCS-1 overexpression may be due in part to reduced target cell recognition. [ABSTRACT FROM AUTHOR]

Published

2006

21. RELATIVE SENSITIVITY OF FETAL AND NEWBORN MICE TO INDUCTION OF HAPTEN-SPECIFIC B-CELL TOLERANCE

Author

PIKE, BL, KAY, TW, NOSSAL, GJV, PIKE, BL, KAY, TW, and NOSSAL, GJV

Abstract

Mice were rendered tolerant to the hapten fluorescein (FLU) by a single injection of FLU-human gamma globulin (FLU5HGG) 2-3 d after birth or via the maternal circulation at 14.5 d of fetal life. After 7-9 d, the degree of functional nonresponsiveness induced in vivo among splenic FLU-specific B cells of tolerized mice was assessed by limiting-dilution analysis in vitro, and the serum levels of trace-labeled tolerogen were determined. When tolerogen was introduced before the appearance of any B cells, and was thus present during the pre-B to B cell transition stage, a concentration of 5.4 x 10(-13) M effectively silenced 50% of the clonable anti-FLU PFC precursors; but a similar reduction on newborns required a minimal tolerogen concentration of 1.3 x 10(-10) M, > 300-fold less than has previously been shown to equally affect adult B cells, but at least 240-fold more than in the in utero situation. Neonatally induced tolerance using a relatively high tolerogen dose lasted approximately 12 wk.

Published

1980

22. Heel ulcers in patients with long‐standing diabetes who wear antiembolism stockings

Author

F. I. R. Martin and Kay Tw

Subjects

Male, medicine.medical_specialty, Heel, Clothing, Foot Diseases, Diabetes mellitus, Skin Ulcer, medicine, Humans, In patient, Heel ulcers, Aged, Postoperative Care, Vascular disease, business.industry, General Medicine, Middle Aged, medicine.disease, Surgery, Peripheral, Diabetes Mellitus, Type 1, Peripheral neuropathy, medicine.anatomical_structure, Female, business, Venous thromboembolism

Abstract

Four patients with long-standing insulin-dependent diabetes mellitus developed heel ulceration while wearing correctly fitted antiembolism stockings after major surgery. These patients all had evidence of peripheral vascular disease and peripheral neuropathy. Heel ulceration appears to be a significant side-effect of this form of prophylaxis against venous thromboembolism in patients with long-standing diabetes mellitus. The use of antiembolism stockings in such patients, who are likely to have vascular and neurological impairment, should be undertaken with great care, if at all.

Published

1986

23. Evidence-Informed Clinical Practice Recommendations for Treatment of Type 1 Diabetes Complicated by Problematic Hypoglycemia

Author

Peter A. Senior, Pratik Choudhary, Bernhard J. Hering, Bart Keymeulen, Paola Maffi, Frantisek Saudek, Marie-Christine Vantyghem, Roger Lehmann, Thomas W.H. Kay, Nobuya Inagaki, Michael R. Rickels, Choudhary, P, Rickels, Mr, Senior, Pa, Vantyghem, Mc, Maffi, P, Kay, Tw, Keymeulen, B, Inagaki, N, Saudek, F, Lehmann, R, Hering, Bj, Pathology/molecular and cellular medicine, and Diabetes Pathology & Therapy

Subjects

Blood Glucose, medicine.medical_specialty, endocrine system diseases, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Psychological intervention, 030209 endocrinology & metabolism, Hypoglycemia, Pancreas transplantation, 03 medical and health sciences, Insulin Infusion Systems, 0302 clinical medicine, Patient Education as Topic, Diabetes mellitus, Internal Medicine, medicine, Humans, Hypoglycemic Agents, Insulin, 030212 general & internal medicine, Intensive care medicine, Glycemic, Advanced and Specialized Nursing, Type 1 diabetes, Evidence-Based Medicine, business.industry, Blood Glucose Self-Monitoring, nutritional and metabolic diseases, Evidence-based medicine, Type 1 Diabetes at a Crossroads, Awareness, medicine.disease, 3. Good health, Surgery, Diabetes Mellitus, Type 1, Pancreas Transplantation, business, Algorithms

Abstract

Problematic hypoglycemia, defined as two or more episodes per year of severe hypoglycemia or as one episode associated with impaired awareness of hypoglycemia, extreme glycemic lability, or major fear and maladaptive behavior, is a challenge, especially for patients with long-standing type 1 diabetes. Individualized therapy for such patients should include a composite target: optimal glucose control without problematic hypoglycemia. Therefore, we propose a tiered, four-stage algorithm based on evidence of efficacy given the limitations of educational, technological, and transplant interventions. All patients with problematic hypoglycemia should undergo structured or hypoglycemia-specific education programs (stage 1). Glycemic and hypoglycemia treatment targets should be individualized and reassessed every 3–6 months. If targets are not met, one diabetes technology—continuous subcutaneous insulin infusion or continuous glucose monitoring—should be added (stage 2). For patients with continued problematic hypoglycemia despite education (stage 1) and one diabetes technology (stage 2), sensor-augmented insulin pumps preferably with an automated low-glucose suspend feature and/or very frequent contact with a specialized hypoglycemia service can reduce hypoglycemia (stage 3). For patients whose problematic hypoglycemia persists, islet or pancreas transplant should be considered (stage 4). This algorithm provides an evidence-informed approach to resolving problematic hypoglycemia; it should be used as a guide, with individual patient circumstances directing suitability and acceptability to ensure the prudent use of technology and scarce transplant resources. Standardized reporting of hypoglycemia outcomes and inclusion of patients with problematic hypoglycemia in studies of new interventions may help to guide future therapeutic strategies.

Published

2015

24. Altering β Cell Antigen Exposure to Exhausted CD8+ T Cells Prevents Autoimmune Diabetes in Mice.

Author

De George DJ, Jhala G, Selck C, Trivedi P, Brodnicki TC, Mackin L, Kay TW, Thomas HE, and Krishnamurthy B

Subjects

Animals, Mice, Granzymes metabolism, Interferon-gamma immunology, Interferon-gamma metabolism, Antigen Presentation immunology, Female, CD8-Positive T-Lymphocytes immunology, Insulin-Secreting Cells immunology, Mice, Inbred NOD, Diabetes Mellitus, Type 1 immunology

Abstract

Chronic destruction of insulin-producing pancreatic β cells by T cells results in autoimmune diabetes. Similar to other chronic T cell-mediated pathologies, a role for T cell exhaustion has been identified in diabetes in humans and NOD mice. The development and differentiation of exhausted T cells depends on exposure to Ag. In this study, we manipulated β cell Ag presentation to target exhausted autoreactive T cells by inhibiting IFN-γ-mediated MHC class I upregulation or by ectopically expressing the β cell Ag IGRP under the MHC class II promotor in the NOD8.3 model. Islet PD-1+TIM3+CD8+ (terminally exhausted [TEX]) cells were primary producers of islet granzyme B and CD107a, suggestive of cells that have entered the exhaustion program yet maintained cytotoxic capacity. Loss of IFN-γ-mediated β cell MHC class I upregulation correlated with a significant reduction in islet TEX cells and diabetes protection in NOD8.3 mice. In NOD.TII/8.3 mice with IGRP expression induced in APCs, IGRP-reactive T cells remained exposed to high levels of IGRP in the islets and periphery. Consequently, functionally exhausted TEX cells, with reduced granzyme B expression, were significantly increased in these mice and this correlated with diabetes protection. These results indicate that intermediate Ag exposure in wild-type NOD8.3 islets allows T cells to enter the exhaustion program without becoming functionally exhausted. Moreover, Ag exposure can be manipulated to target this key cytotoxic population either by limiting the generation of cytotoxic TIM3+ cells or by driving their functional exhaustion, with both resulting in diabetes protection., (Copyright © 2024 by The American Association of Immunologists, Inc.)

Published

2024

25. TIGIT acts as an immune checkpoint upon inhibition of PD1 signaling in autoimmune diabetes.

Author

Trivedi P, Jhala G, De George DJ, Chiu C, Selck C, Ge T, Catterall T, Elkerbout L, Boon L, Joller N, Kay TW, Thomas HE, and Krishnamurthy B

Subjects

Animals, Humans, Mice, Immune Checkpoint Proteins, Ligands, Mice, Inbred NOD, Receptors, Immunologic metabolism, Diabetes Mellitus, Type 1

Abstract

Introduction: Chronic activation of self-reactive T cells with beta cell antigens results in the upregulation of immune checkpoint molecules that keep self-reactive T cells under control and delay beta cell destruction in autoimmune diabetes. Inhibiting PD1/PD-L1 signaling results in autoimmune diabetes in mice and humans with pre-existing autoimmunity against beta cells. However, it is not known if other immune checkpoint molecules, such as TIGIT, can also negatively regulate self-reactive T cells. TIGIT negatively regulates the CD226 costimulatory pathway, T-cell receptor (TCR) signaling, and hence T-cell function., Methods: The phenotype and function of TIGIT expressing islet infiltrating T cells was studied in non-obese diabetic (NOD) mice using flow cytometry and single cell RNA sequencing. To determine if TIGIT restrains self-reactive T cells, we used a TIGIT blocking antibody alone or in combination with anti-PDL1 antibody., Results: We show that TIGIT is highly expressed on activated islet infiltrating T cells in NOD mice. We identified a subset of stem-like memory CD8+ T cells expressing multiple immune checkpoints including TIGIT, PD1 and the transcription factor EOMES, which is linked to dysfunctional CD8+ T cells. A known ligand for TIGIT, CD155 was expressed on beta cells and islet infiltrating dendritic cells. However, despite TIGIT and its ligand being expressed, islet infiltrating PD1+TIGIT+CD8+ T cells were functional. Inhibiting TIGIT in NOD mice did not result in exacerbated autoimmune diabetes while inhibiting PD1-PDL1 resulted in rapid autoimmune diabetes, indicating that TIGIT does not restrain islet infiltrating T cells in autoimmune diabetes to the same degree as PD1. Partial inhibition of PD1-PDL1 in combination with TIGIT inhibition resulted in rapid diabetes in NOD mice., Discussion: These results suggest that TIGIT and PD1 act in synergy as immune checkpoints when PD1 signaling is partially impaired. Beta cell specific stem-like memory T cells retain their functionality despite expressing multiple immune checkpoints and TIGIT is below PD1 in the hierarchy of immune checkpoints in autoimmune diabetes., Competing Interests: Author LB was employed by the company JJP Biologics. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. The author(s) declared that they were an editorial board member of Frontiers, at the time of submission. This had no impact on the peer review process and the final decision., (Copyright © 2024 Trivedi, Jhala, De George, Chiu, Selck, Ge, Catterall, Elkerbout, Boon, Joller, Kay, Thomas and Krishnamurthy.)

Published

2024

26. Intracutaneous Transplantation of Islets Within a Biodegradable Temporizing Matrix as an Alternative Site for Islet Transplantation.

Author

Rojas-Canales D, Walters SN, Penko D, Cultrone D, Bailey J, Chtanova T, Nitschke J, Johnston J, Kireta S, Loudovaris T, Kay TW, Kuchel TR, Hawthorne W, O'Connell PJ, Korbutt G, Greenwood JE, Grey ST, Drogemuller CJ, and Coates PT

Subjects

Swine, Humans, Animals, Mice, Graft Survival, Collagen, Islets of Langerhans Transplantation methods, Islets of Langerhans blood supply, Diabetes Mellitus, Type 1 surgery

Abstract

Intrahepatic islet transplantation for type 1 diabetes is limited by the need for multiple infusions and poor islet viability posttransplantation. The development of alternative transplantation sites is necessary to improve islet survival and facilitate monitoring and retrieval. We tested a clinically proven biodegradable temporizing matrix (BTM), a polyurethane-based scaffold, to generate a well-vascularized intracutaneous "neodermis" within the skin for islet transplantation. In murine models, BTM did not impair syngeneic islet renal-subcapsular transplant viability or function, and it facilitated diabetes cure for over 150 days. Furthermore, BTM supported functional neonatal porcine islet transplants into RAG-1-/- mice for 400 days. Hence, BTM is nontoxic for islets. Two-photon intravital imaging used to map vessel growth through time identified dense vascular networks, with significant collagen deposition and increases in vessel mass up to 30 days after BTM implantation. In a preclinical porcine skin model, BTM implants created a highly vascularized intracutaneous site by day 7 postimplantation. When syngeneic neonatal porcine islets were transplanted intracutaneously, the islets remained differentiated as insulin-producing cells, maintained normal islet architecture, secreted c-peptide, and survived for over 100 days. Here, we show that BTM facilitates formation of an islet-supportive intracutaneous neodermis in a porcine preclinical model, as an alternative islet-transplant site., Article Highlights: Human and porcine pancreatic islets were transplanted into a fully vascularized biodegradable temporizing matrix (Novosorb) that creates a unique intracutaneous site outside of the liver in a large-animal preclinical model. The intracutaneous prevascularized site supported pancreatic islet survival for 3 months in a syngeneic porcine-transplant model. Pancreatic (human and porcine) islet survival and function were demonstrated in an intracutaneous site outside of the liver for the first time in a large-animal preclinical model., (© 2023 by the American Diabetes Association.)

Published

2023

27. Diabetes induced by checkpoint inhibition in nonobese diabetic mice can be prevented or reversed by a JAK1/JAK2 inhibitor.

Author

Ge T, Phung AL, Jhala G, Trivedi P, Principe N, De George DJ, Pappas EG, Litwak S, Sanz-Villanueva L, Catterall T, Fynch S, Boon L, Kay TW, Chee J, Krishnamurthy B, and Thomas HE

Abstract

Objectives: Immune checkpoint inhibitors have achieved clinical success in cancer treatment, but this treatment causes immune-related adverse events, including type 1 diabetes (T1D). Our aim was to test whether a JAK1/JAK2 inhibitor, effective at treating spontaneous autoimmune diabetes in nonobese diabetic (NOD) mice, can prevent diabetes secondary to PD-L1 blockade., Methods: Anti-PD-L1 antibody was injected into NOD mice to induce diabetes, and JAK1/JAK2 inhibitor LN3103801 was administered by oral gavage to prevent diabetes. Flow cytometry was used to study T cells and beta cells. Mesothelioma cells were inoculated into BALB/c mice to induce a transplantable tumour model., Results: Anti-PD-L1-induced diabetes was associated with increased immune cell infiltration in the islets and upregulated MHC class I on islet cells. Anti-PD-L1 administration significantly increased islet T cell proliferation and islet-specific CD8 + T cell numbers in peripheral lymphoid organs. JAK1/JAK2 inhibitor treatment blocked IFNγ-mediated MHC class I upregulation on beta cells and T cell proliferation mediated by cytokines that use the common γ chain receptor. As a result, anti-PD-L1-induced diabetes was prevented by JAK1/JAK2 inhibitor administered before or after checkpoint inhibitor therapy. Diabetes was also reversed when the JAK1/JAK2 inhibitor was administered after the onset of anti-PD-L1-induced hyperglycaemia. Furthermore, JAK1/JAK2 inhibitor intervention after checkpoint inhibitors did not reverse or abrogate the antitumour effects in a transplantable tumour model., Conclusion: A JAK1/JAK2 inhibitor can prevent and reverse anti-PD-L1-induced diabetes by blocking IFNγ and γc cytokine activities. Our study provides preclinical validation of JAK1/JAK2 inhibitor use in checkpoint inhibitor-induced diabetes., Competing Interests: TWHK has an Investigator‐Initiated Clinical Trial agreement with Eli Lilly. However, Eli Lilly had no role in the current study design, data collection and analysis, decision to publish or preparation of the manuscript. The authors declare that there are no other relationships or activities that might bias, or be perceived to bias, their work., (© 2022 The Authors. Clinical & Translational Immunology published by John Wiley & Sons Australia, Ltd on behalf of Australian and New Zealand Society for Immunology, Inc.)

Published

2022

28. Desmoglein-2 is important for islet function and β-cell survival.

Author

Myo Min KK, Rojas-Canales D, Penko D, DeNichilo M, Cockshell MP, Ffrench CB, Thompson EJ, Asplund O, Drogemuller CJ, Prasad RB, Groop L, Grey ST, Thomas HE, Loudovaris T, Kay TW, Mahoney MG, Jessup CF, Coates PT, and Bonder CS

Subjects

Animals, Humans, Mice, Cell Survival, Desmogleins metabolism, Insulin metabolism, Streptozocin, Diabetes Mellitus, Experimental genetics, Diabetes Mellitus, Experimental metabolism, Diabetes Mellitus, Type 1 metabolism, Islets of Langerhans metabolism

Abstract

Type 1 diabetes is a complex disease characterized by the lack of endogenous insulin secreted from the pancreatic β-cells. Although β-cell targeted autoimmune processes and β-cell dysfunction are known to occur in type 1 diabetes, a complete understanding of the cell-to-cell interactions that support pancreatic function is still lacking. To characterize the pancreatic endocrine compartment, we studied pancreata from healthy adult donors and investigated a single cell surface adhesion molecule, desmoglein-2 (DSG2). Genetically-modified mice lacking Dsg2 were examined for islet cell mass, insulin production, responses to glucose, susceptibility to a streptozotocin-induced mouse model of hyperglycaemia, and ability to cure diabetes in a syngeneic transplantation model. Herein, we have identified DSG2 as a previously unrecognized adhesion molecule that supports β-cells. Furthermore, we reveal that DSG2 is within the top 10 percent of all genes expressed by human pancreatic islets and is expressed by the insulin-producing β-cells but not the somatostatin-producing δ-cells. In a Dsg2 loss-of-function mice (Dsg2 lo/lo ), we observed a significant reduction in the number of pancreatic islets and islet size, and consequently, there was less total insulin content per islet cluster. Dsg2 lo/lo mice also exhibited a reduction in blood vessel barrier integrity, an increased incidence of streptozotocin-induced diabetes, and islets isolated from Dsg2 lo/lo mice were more susceptible to cytokine-induced β-cell apoptosis. Following transplantation into diabetic mice, islets isolated from Dsg2 lo/lo mice were less effective than their wildtype counterparts at curing diabetes. In vitro assays using the Beta-TC-6 murine β-cell line suggest that DSG2 supports the actin cytoskeleton as well as the release of cytokines and chemokines. Taken together, our study suggests that DSG2 is an under-appreciated regulator of β-cell function in pancreatic islets and that a better understanding of this adhesion molecule may provide new opportunities to combat type 1 diabetes., (© 2022. The Author(s).)

Published

2022

29. Investigating the efficacy of baricitinib in new onset type 1 diabetes mellitus (BANDIT)-study protocol for a phase 2, randomized, placebo controlled trial.

Author

Waibel M, Thomas HE, Wentworth JM, Couper JJ, MacIsaac RJ, Cameron FJ, So M, Krishnamurthy B, Doyle MC, and Kay TW

Subjects

Animals, Azetidines, C-Peptide, Clinical Trials, Phase II as Topic, Double-Blind Method, Glucose therapeutic use, Humans, Janus Kinases therapeutic use, Mice, Multicenter Studies as Topic, Purines, Pyrazoles, Randomized Controlled Trials as Topic, STAT Transcription Factors therapeutic use, Signal Transduction, Sulfonamides, Treatment Outcome, Diabetes Mellitus, Type 1 diagnosis, Diabetes Mellitus, Type 1 drug therapy

Abstract

Background: Type 1 diabetes (T1D) places an extraordinary burden on individuals and their families, as well as on the healthcare system. Despite recent advances in glucose sensors and insulin pump technology, only a minority of patients meet their glucose targets and face the risk of both acute and long-term complications, some of which are life-threatening. The JAK-STAT pathway is critical for the immune-mediated pancreatic beta cell destruction in T1D. Our pre-clinical data show that inhibitors of JAK1/JAK2 prevent diabetes and reverse newly diagnosed diabetes in the T1D non-obese diabetic mouse model. The goal of this study is to determine if the JAK1/JAK2 inhibitor baricitinib impairs type 1 diabetes autoimmunity and preserves beta cell function., Methods: This will be as a multicentre, two-arm, double-blind, placebo-controlled randomized trial in individuals aged 10-30 years with recent-onset T1D. Eighty-three participants will be randomized in a 2:1 ratio within 100 days of diagnosis to receive either baricitinib 4mg/day or placebo for 48 weeks and then monitored for a further 48 weeks after stopping study drug. The primary outcome is the plasma C-peptide 2h area under the curve following ingestion of a mixed meal. Secondary outcomes include HbA1c, insulin dose, continuous glucose profile and adverse events. Mechanistic assessments will characterize general and diabetes-specific immune responses., Discussion: This study will determine if baricitinib slows the progressive, immune-mediated loss of beta cell function that occurs after clinical presentation of T1D. Preservation of beta cell function would be expected to improve glucose control and prevent diabetes complications, and justify additional trials of baricitinib combined with other therapies and of its use in at-risk populations to prevent T1D., Trial Registration: ANZCTR ACTRN12620000239965 . Registered on 26 February 2020., Clinicaltrials: gov NCT04774224. Registered on 01 March 2021., (© 2022. The Author(s).)

Published

2022

30. Australian experience with total pancreatectomy with islet autotransplantation to treat chronic pancreatitis.

Author

Bampton TJ, Holmes-Walker DJ, Drogemuller CJ, Radford T, Anderson P, Etherton C, Russell CH, Khurana S, Torpy DJ, Couper JJ, Couper RLT, Macintyre P, Neo EL, Benitez-Aguirre P, Thomas G, Loudovaris T, Thomas HE, Palmer LJ, Wu D, Rogers NM, Williams L, Hawthorne WJ, O'Connell PJ, Kay TW, Pleass H, Chen JW, and Coates PT

Subjects

Australia epidemiology, Humans, Pain Management, Transplantation, Autologous, Pancreatectomy, Pancreatitis, Chronic surgery

Abstract

Background: This study aimed to describe the clinical outcomes of total pancreatectomy with islet autotransplantation (TP-IAT) in Australia., Methods: Individuals selected for TP-IAT surgery according to the Minnesota Criteria (Appendix) without evidence of diabetes were evaluated including time to transplantation from pancreatectomy, islet numbers infused and post-transplantation HbA1c, C-peptide, total daily insulin and analgesic requirement., Results: Sixteen individuals underwent TP-IAT from Australia and New Zealand between 2010 and 2020. Two recipients are deceased. The median islet equivalents/kg infused was 4244 (interquartile range (IQR) 2290-7300). The median C-peptide 1 month post-TP-IAT was 384 (IQR 210-579) pmol/L and at median 29.5 (IQR 14.5-46.5) months from transplant was 395 (IQR 139-862) pmol/L. Insulin independence was achieved in eight of 15 (53.3%) surviving recipients. A higher islet equivalents transplanted was most strongly associated with the likelihood of insulin independence (P < 0.05). Of the 15 surviving recipients, 14 demonstrated substantial reduction in analgesic requirement., Conclusion: The TP-IAT programme in Australia has been a successful new therapy for the management of individuals with chronic pancreatitis including hereditary forms refractory to medical treatment to improve pain management with 50% insulin independence rates., (© 2021 Royal Australasian College of Surgeons.)

Published

2021

31. South Australian experience with paediatric total pancreatectomy and islet autotransplantation for PRSS1-associated hereditary pancreatitis.

Author

Eldredge J, Couper MR, Moore DJ, Khurana S, Chen JW, Couper JJ, Drogemuller CJ, Radford T, Kay TW, Loudovaris T, Wilks M, Coates PT, and Couper RT

Subjects

Adolescent, Child, Female, Humans, Incidence, Islets of Langerhans Transplantation methods, Male, Mutation, Pancreatectomy statistics & numerical data, Pancreatitis, Chronic epidemiology, Pancreatitis, Chronic etiology, South Australia epidemiology, Transplantation, Autologous, Treatment Outcome, Pancreatectomy methods, Pancreatitis, Chronic genetics, Pancreatitis, Chronic surgery, Trypsin genetics

Published

2021

32. Harnessing CD8 + T-cell exhaustion to treat type 1 diabetes.

Author

Kwong CJ, Selck C, Tahija K, McAnaney LJ, Le DV, Kay TW, Thomas HE, and Krishnamurthy B

Subjects

Autoimmunity, CD8-Positive T-Lymphocytes, Humans, Insulin, Diabetes Mellitus, Type 1 therapy, Insulin-Secreting Cells

Abstract

Although immune interventions have shown great promise in type 1 diabetes mellitus (T1D) clinical trials, none are yet in routine clinical use or able to achieve insulin independence in patients. In addition to this, the principles of T1D treatment remain essentially unchanged since the isolation of insulin, almost a century ago. T1D is characterized by insulin deficiency as a result of destruction of insulin-producing beta cells mediated by autoreactive T cells. Therapies that target beta-cell antigen-specific T cells are needed to prevent T1D. CD8 + T-cell exhaustion is an emerging area of research in chronic infection, cancer immunotherapy, and more recently, autoimmunity. Recent data suggest that exhausted T-cell populations are associated with improved markers of T1D. T-cell exhaustion is both characterized and mediated by inhibitory receptors. This review aims to identify which inhibitory receptors may prove useful to induce T-cell exhaustion to treat T1D and identify limitations and gaps in the current literature., (© 2021 Australian and New Zealand Society for Immunology, Inc.)

Published

2021

33. Machine learning workflows identify a microRNA signature of insulin transcription in human tissues.

Author

Wong WKM, Joglekar MV, Saini V, Jiang G, Dong CX, Chaitarvornkit A, Maciag GJ, Gerace D, Farr RJ, Satoor SN, Sahu S, Sharangdhar T, Ahmed AS, Chew YV, Liuwantara D, Heng B, Lim CK, Hunter J, Januszewski AS, Sørensen AE, Akil ASA, Gamble JR, Loudovaris T, Kay TW, Thomas HE, O'Connell PJ, Guillemin GJ, Martin D, Simpson AM, Hawthorne WJ, Dalgaard LT, Ma RCW, and Hardikar AA

Abstract

Dicer knockout mouse models demonstrated a key role for microRNAs in pancreatic β-cell function. Studies to identify specific microRNA(s) associated with human (pro-)endocrine gene expression are needed. We profiled microRNAs and key pancreatic genes in 353 human tissue samples. Machine learning workflows identified microRNAs associated with (pro-)insulin transcripts in a discovery set of islets (n = 30) and insulin-negative tissues (n = 62). This microRNA signature was validated in remaining 261 tissues that include nine islet samples from individuals with type 2 diabetes. Top eight microRNAs (miR-183-5p, -375-3p, 216b-5p, 183-3p, -7-5p, -217-5p, -7-2-3p, and -429-3p) were confirmed to be associated with and predictive of (pro-)insulin transcript levels. Use of doxycycline-inducible microRNA-overexpressing human pancreatic duct cell lines confirmed the regulatory roles of these microRNAs in (pro-)endocrine gene expression. Knockdown of these microRNAs in human islet cells reduced (pro-)insulin transcript abundance. Our data provide specific microRNAs to further study microRNA-mRNA interactions in regulating insulin transcription., Competing Interests: A patent application (WO2019000017A1) was filed., (© 2021 The Authors.)

Published

2021

34. The JAK1 Selective Inhibitor ABT 317 Blocks Signaling Through Interferon-γ and Common γ Chain Cytokine Receptors to Reverse Autoimmune Diabetes in NOD Mice.

Author

Ge T, Jhala G, Fynch S, Akazawa S, Litwak S, Pappas EG, Catterall T, Vakil I, Long AJ, Olson LM, Krishnamurthy B, Kay TW, and Thomas HE

Subjects

Animals, Insulin-Secreting Cells drug effects, Insulin-Secreting Cells immunology, Janus Kinase Inhibitors pharmacokinetics, Male, Mice, Inbred C57BL, Mice, Inbred NOD, Signal Transduction drug effects, Spleen immunology, Diabetes Mellitus, Type 1 immunology, Interferon-gamma immunology, Interleukin Receptor Common gamma Subunit immunology, Janus Kinase 1 antagonists & inhibitors, Janus Kinase Inhibitors pharmacology

Abstract

Cytokines that signal through the JAK-STAT pathway, such as interferon-γ (IFN-γ) and common γ chain cytokines, contribute to the destruction of insulin-secreting β cells by CD8 + T cells in type 1 diabetes (T1D). We previously showed that JAK1/JAK2 inhibitors reversed autoimmune insulitis in non-obese diabetic (NOD) mice and also blocked IFN-γ mediated MHC class I upregulation on β cells. Blocking interferons on their own does not prevent diabetes in knockout NOD mice, so we tested whether JAK inhibitor action on signaling downstream of common γ chain cytokines, including IL-2, IL-7 IL-15, and IL-21, may also affect the progression of diabetes in NOD mice. Common γ chain cytokines activate JAK1 and JAK3 to regulate T cell proliferation. We used a JAK1-selective inhibitor, ABT 317, to better understand the specific role of JAK1 signaling in autoimmune diabetes. ABT 317 reduced IL-21, IL-2, IL-15 and IL-7 signaling in T cells and IFN-γ signaling in β cells, but ABT 317 did not affect GM-CSF signaling in granulocytes. When given in vivo to NOD mice, ABT 317 reduced CD8 + T cell proliferation as well as the number of KLRG + effector and CD44 hi CD62L lo effector memory CD8 + T cells in spleen. ABT 317 also prevented MHC class I upregulation on β cells. Newly diagnosed diabetes was reversed in 94% NOD mice treated twice daily with ABT 317 while still on treatment at 40 days and 44% remained normoglycemic after a further 60 days from discontinuing the drug. Our results indicate that ABT 317 blocks common γ chain cytokines in lymphocytes and interferons in lymphocytes and β cells and are thus more effective against diabetes pathogenesis than IFN-γ receptor deficiency alone. Our studies suggest use of this class of drug for the treatment of type 1 diabetes., Competing Interests: At the time of the study, AL and LO were both employees of Abbvie. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2020 Ge, Jhala, Fynch, Akazawa, Litwak, Pappas, Catterall, Vakil, Long, Olson, Krishnamurthy, Kay and Thomas.)

Published

2020

35. Comment on Trinh et al. Successful Treatment of Immune Checkpoint Inhibitor-Induced Diabetes With Infliximab. Diabetes Care 2019;42:e153-e154.

Author

Galligan A, Krishnamurthy B, and Kay TW

Published

2020

36. Replica moulded poly(dimethylsiloxane) microwell arrays induce localized endothelial cell immobilization for coculture with pancreatic islets.

Author

Burzava ALS, Forget A, Harding FJ, Cockshell MP, Penko D, Rouzaud C, Ahmadi V, Marina PF, Rojas-Canales D, Bonder CS, Coates PTH, Waibel M, Thomas HE, Kay TW, Loudovaris T, Blencowe A, and Voelcker NH

Subjects

Humans, Islets of Langerhans, Printing, Three-Dimensional, Surface Properties, Cell Adhesion, Cells, Immobilized physiology, Coculture Techniques methods, Dimethylpolysiloxanes metabolism, Endothelial Cells physiology, Glucagon-Secreting Cells physiology, Insulin-Secreting Cells physiology

Abstract

PolyJet three-dimensional (3D) printing allows for the rapid manufacturing of 3D moulds for the fabrication of cross-linked poly(dimethylsiloxane) microwell arrays (PMAs). As this 3D printing technique has a resolution on the micrometer scale, the moulds exhibit a distinct surface roughness. In this study, the authors demonstrate by optical profilometry that the topography of the 3D printed moulds can be transferred to the PMAs and that this roughness induced cell adhesive properties to the material. In particular, the topography facilitated immobilization of endothelial cells on the internal walls of the microwells. The authors also demonstrate that upon immobilization of endothelial cells to the microwells, a second population of cells, namely, pancreatic islets could be introduced, thus producing a 3D coculture platform.

Published

2019

37. Mortality in People With Type 1 Diabetes, Severe Hypoglycemia, and Impaired Awareness of Hypoglycemia Referred for Islet Transplantation.

Author

Lee MH, Ward GM, MacIsaac RJ, Howe K, Holmes-Walker DJ, Anderson P, Radford T, Coates PT, Kay TW, O'Connell PJ, and Goodman DJ

Abstract

Competing Interests: M.H.L., G.M.W., R.J.M., K.H., D.J.H., P.A., T.R., P.T.C., T.W.K., and D.G. declare no competing financial interests. P.J.O. consults for CSL, Vitaeris and eGenesis; and has received research grants from CSL.

Published

2018

38. Characterization of the Human Pancreas Side Population as a Potential Reservoir of Adult Stem Cells.

Author

Augstein P, Loudovaris T, Bandala-Sanchez E, Heinke P, Naselli G, Lee L, Hawthorne WJ, Góñez LJ, Neale AM, Vaillant F, Thomas HE, Kay TW, Banakh I, and Harrison LC

Subjects

AC133 Antigen metabolism, Adolescent, Adult, Adult Stem Cells metabolism, Aged, CA-19-9 Antigen metabolism, Cells, Cultured, Female, Humans, Islets of Langerhans cytology, Islets of Langerhans metabolism, Male, Middle Aged, Pancreas, Exocrine cytology, Pancreas, Exocrine metabolism, Side-Population Cells metabolism, Young Adult, Adult Stem Cells cytology, Cell Separation methods, Pancreas cytology, Side-Population Cells cytology

Abstract

Objectives: The side population (SP) contains cells with stem cell/progenitor properties. Previously, we observed that the mouse pancreas SP expanded after pancreatic injury. We aimed to characterize the SP in human pancreas as a potential source of stem cells., Methods: Human organ donor pancreata were fractionated into islets and exocrine tissue, enriched by tissue culture and dispersed into single cells. Cells were phenotyped by flow cytometry, and the SP was defined by efflux of fluorescent dye Hoechst 33342 visualized by ultraviolet excitation. Cells were flow sorted, and their colony-forming potential measured on feeder cells in culture., Results: An SP was identified in islet and exocrine cells from human organ donors: 2 with type 1 diabetes, 3 with type 2 diabetes, and 28 without diabetes. Phenotyping revealed that exocrine SP cells had an epithelial origin, were enriched for carbohydrate antigen 19-9 ductal cells expressing stem cell markers CD133 and CD26, and had greater colony-forming potential than non-SP cells. The exocrine SP was increased in a young adult with type 1 diabetes and ongoing islet autoimmunity., Conclusions: The pancreatic exocrine SP is a potential reservoir of adult stem/progenitor cells, consistent with previous evidence that such cells are duct-derived and express CD133.

Published

2018

39. Loss of BIM increases mitochondrial oxygen consumption and lipid oxidation, reduces adiposity and improves insulin sensitivity in mice.

Author

Wali JA, Galic S, Tan CY, Gurzov EN, Frazier AE, Connor T, Ge J, Pappas EG, Stroud D, Varanasi LC, Selck C, Ryan MT, Thorburn DR, Kemp BE, Krishnamurthy B, Kay TW, McGee SL, and Thomas HE

Subjects

Animals, Bcl-2-Like Protein 11 genetics, Electron Transport Complex IV metabolism, Energy Metabolism, Glucose metabolism, Hepatocytes metabolism, Insulin Resistance, Liver metabolism, Membrane Potential, Mitochondrial, Mice, Oxidation-Reduction, Oxygen Consumption, Weight Loss, Adiposity, Bcl-2-Like Protein 11 physiology, Lipid Metabolism, Mitochondria metabolism

Abstract

BCL-2 proteins are known to engage each other to determine the fate of a cell after a death stimulus. However, their evolutionary conservation and the many other reported binding partners suggest an additional function not directly linked to apoptosis regulation. To identify such a function, we studied mice lacking the BH3-only protein BIM. BIM -/- cells had a higher mitochondrial oxygen consumption rate that was associated with higher mitochondrial complex IV activity. The consequences of increased oxygen consumption in BIM -/- mice were significantly lower body weights, reduced adiposity and lower hepatic lipid content. Consistent with reduced adiposity, BIM -/- mice had lower fasting blood glucose, improved insulin sensitivity and hepatic insulin signalling. Lipid oxidation was increased in BIM -/- mice, suggesting a mechanism for their metabolic phenotype. Our data suggest a role for BIM in regulating mitochondrial bioenergetics and metabolism and support the idea that regulation of metabolism and cell death are connected.

Published

2018

40. Transplantation sites for human and murine islets.

Author

Stokes RA, Cheng K, Lalwani A, Swarbrick MM, Thomas HE, Loudovaris T, Kay TW, Hawthorne WJ, O'Connell PJ, and Gunton JE

Subjects

Animals, Blood Glucose, Diabetes Mellitus, Experimental blood, Graft Survival, Humans, Mice, Mice, Inbred C57BL, Diabetes Mellitus, Experimental surgery, Islets of Langerhans Transplantation methods, Kidney surgery, Liver surgery, Portal Vein surgery, Quadriceps Muscle surgery, Spleen surgery

Abstract

Aims/hypothesis: Beta cell replacement is a potential cure for type 1 diabetes. In humans, islet transplants are currently infused into the liver via the portal vein, although this site has disadvantages. Here, we investigated alternative transplantation sites for human and murine islets in recipient mice, comparing the portal vein with quadriceps muscle and kidney, liver and spleen capsules., Methods: Murine islets were isolated from C57BL6/J mice and transplanted into syngeneic recipients. Human islets were isolated and transplanted into either severe combined immunodeficiency (SCID) or recombination-activating gene 1 (RAG-1) immunodeficient recipient mice. All recipient mice were 8-12 weeks of age and had been rendered diabetic (defined as blood glucose concentrations ≥20 mmol/l on two consecutive days before transplantation) by alloxan tetrahydrate treatment. Islets were transplanted into five different sites (portal vein, quadriceps muscle, kidney, liver and spleen capsules). Blood glucose concentrations were monitored twice weekly until mice were killed. Dose-response studies were also performed to determine the minimum number of islets required to cure diabetes ('cure' is defined for this study as random fed blood glucose of <15 mmol/l)., Results: For transplantation of murine islets into the different sites, the kidney yielded 100% success, followed by muscle (70%), portal vein (60%), spleen capsule (29%) and liver capsule (0%). For human islets, transplantation into the kidney cured diabetes in 75-80% of recipient mice. Transplantation into muscle and portal vein had intermediate success (both 29% at 2000 islet equivalents), while transplantation into liver and spleen capsule failed (0%). With increased islet mass, success rates for muscle grafts improved to 52-56%., Conclusions/interpretation: For both human and murine islets, equivalent or superior glucose lowering results were obtained for transplantation into skeletal muscle, compared with the portal vein. Unfortunately, kidney grafts are not feasible in human recipients. Skeletal muscle offers easier access and greater potential for protocol biopsies. This study suggests that human trials of muscle as a transplant site may be warranted.

Published

2017

41. Inhibition of Y1 receptor signaling improves islet transplant outcome.

Author

Loh K, Shi YC, Walters S, Bensellam M, Lee K, Dezaki K, Nakata M, Ip CK, Chan JY, Gurzov EN, Thomas HE, Waibel M, Cantley J, Kay TW, Yada T, Laybutt DR, Grey ST, and Herzog H

Subjects

Animals, Arginine analogs & derivatives, Arginine pharmacology, Cyclic AMP metabolism, Diabetes Mellitus, Experimental metabolism, Humans, Insulin metabolism, Insulin Secretion, Mice, Receptors, Neuropeptide Y antagonists & inhibitors, Receptors, Neuropeptide Y metabolism, Signal Transduction, Insulin-Secreting Cells metabolism, Islets of Langerhans metabolism, Islets of Langerhans Transplantation

Abstract

Failure to secrete sufficient quantities of insulin is a pathological feature of type-1 and type-2 diabetes, and also reduces the success of islet cell transplantation. Here we demonstrate that Y1 receptor signaling inhibits insulin release in β-cells, and show that this can be pharmacologically exploited to boost insulin secretion. Transplanting islets with Y1 receptor deficiency accelerates the normalization of hyperglycemia in chemically induced diabetic recipient mice, which can also be achieved by short-term pharmacological blockade of Y1 receptors in transplanted mouse and human islets. Furthermore, treatment of non-obese diabetic mice with a Y1 receptor antagonist delays the onset of diabetes. Mechanistically, Y1 receptor signaling inhibits the production of cAMP in islets, which via CREB mediated pathways results in the down-regulation of several key enzymes in glycolysis and ATP production. Thus, manipulating Y1 receptor signaling in β-cells offers a unique therapeutic opportunity for correcting insulin deficiency as it occurs in the pathological state of type-1 diabetes as well as during islet transplantation.Islet transplantation is considered one of the potential treatments for T1DM but limited islet survival and their impaired function pose limitations to this approach. Here Loh et al. show that the Y1 receptor is expressed in β- cells and inhibition of its signalling, both genetic and pharmacological, improves mouse and human islet function.

Published

2017

42. Islet Transplantation Provides Superior Glycemic Control With Less Hypoglycemia Compared With Continuous Subcutaneous Insulin Infusion or Multiple Daily Insulin Injections.

Author

Holmes-Walker DJ, Gunton JE, Hawthorne W, Payk M, Anderson P, Donath S, Loudovaris T, Ward GM, Kay TW, and OʼConnell PJ

Subjects

Adult, Australia, Biomarkers blood, Blood Glucose metabolism, Blood Glucose Self-Monitoring, Diabetes Mellitus, Type 1 blood, Diabetes Mellitus, Type 1 diagnosis, Drug Administration Schedule, Female, Glycated Hemoglobin metabolism, Humans, Hypoglycemia blood, Hypoglycemia chemically induced, Hypoglycemic Agents adverse effects, Infusions, Subcutaneous, Injections, Insulin adverse effects, Insulin Infusion Systems, Male, Middle Aged, Risk Factors, Time Factors, Treatment Outcome, Blood Glucose drug effects, Diabetes Mellitus, Type 1 therapy, Hypoglycemia prevention & control, Hypoglycemic Agents administration & dosage, Insulin administration & dosage, Islets of Langerhans Transplantation adverse effects

Abstract

Background: The aim was to compare efficacy of multiple daily injections (MDI), continuous subcutaneous insulin infusion (CSII) and islet transplantation to reduce hypoglycemia and glycemic variability in type 1 diabetes subjects with severe hypoglycemia., Methods: This was a within-subject, paired comparison of MDI and CSII and CSII with 12 months postislet transplantation in 10 type 1 diabetes subjects referred with severe hypoglycemia, suitable for islet transplantation. Individuals were assessed with HbA1c, Edmonton Hypoglycemia Score (HYPOscore), continuous glucose monitoring (CGM) and in 8 subjects measurements of glucose variability using standard deviation of glucose (SD glucose) from CGM and continuous overlapping net glycemic action using a 4 hour interval (CONGA4)., Results: After changing from MDI to CSII before transplantation, 10 subjects reduced median HYPOscore from 2028 to 1085 (P < 0.05) and hypoglycemia events from 24 to 8 per patient-year (P < 0.05). While HbA1c, mean glucose and median percent time hypoglycemic on CGM were unchanged with CSII, SD glucose and CONGA4 reduced significantly (P < 0.05). At 12 months posttransplant 9 of 10 were C-peptide positive, (5 insulin independent). Twelve months postislet transplantation, there were significant reductions in all baseline parameters versus CSII, respectively, HbA1c (6.4% cf 8.2%), median HYPOscore (0 cf 1085), mean glucose (7.1 cf 8.6 mmol L), SD glucose (1.7 cf 3.2 mmol/L), and CONGA4 (1.6 cf 3.0)., Conclusions: In subjects with severe hypoglycemia suitable for islet transplantation, CSII decreased hypoglycemia frequency and glycemic variability compared with MDI whereas islet transplantation resolved hypoglycemia and further improved glycemic variability regardless of insulin independence.

Published

2017

43. Repurposed JAK1/JAK2 Inhibitor Reverses Established Autoimmune Insulitis in NOD Mice.

Author

Trivedi PM, Graham KL, Scott NA, Jenkins MR, Majaw S, Sutherland RM, Fynch S, Lew AM, Burns CJ, Krishnamurthy B, Brodnicki TC, Mannering SI, Kay TW, and Thomas HE

Subjects

Animals, Blotting, Western, CD8-Positive T-Lymphocytes immunology, Chemokine CXCL10 immunology, Cytokines immunology, Diabetes Mellitus, Type 1 metabolism, Flow Cytometry, Histocompatibility Antigens Class II genetics, Histocompatibility Antigens Class II immunology, Humans, Immunohistochemistry, In Vitro Techniques, Insulin-Secreting Cells metabolism, Islets of Langerhans cytology, Islets of Langerhans drug effects, Islets of Langerhans immunology, Janus Kinase 1 antagonists & inhibitors, Janus Kinase 2 antagonists & inhibitors, Mice, Mice, Inbred NOD, Up-Regulation, Blood Glucose metabolism, CD8-Positive T-Lymphocytes drug effects, Diabetes Mellitus, Type 1 immunology, Histocompatibility Antigens Class II drug effects, Insulin-Secreting Cells drug effects, Pyrazoles pharmacology, Pyrimidines pharmacology

Abstract

Recent advances in immunotherapeutics have not yet changed the routine management of autoimmune type 1 diabetes. There is an opportunity to repurpose therapeutics used to treat other diseases to treat type 1 diabetes, especially when there is evidence for overlapping mechanisms. Janus kinase (JAK) 1/JAK2 inhibitors are in development or clinical use for indications including rheumatoid arthritis. There is good evidence for activation of the JAK1/JAK2 and signal transducer and activator of transcription (STAT) 1 pathway in human type 1 diabetes and in mouse models, especially in β-cells. We tested the hypothesis that using these drugs to block the JAK-STAT pathway would prevent autoimmune diabetes. The JAK1/JAK2 inhibitor AZD1480 blocked the effect of cytokines on mouse and human β-cells by inhibiting MHC class I upregulation. This prevented the direct interaction between CD8 + T cells and β-cells, and reduced immune cell infiltration into islets. NOD mice treated with AZD1480 were protected from autoimmune diabetes, and diabetes was reversed in newly diagnosed NOD mice. This provides mechanistic groundwork for repurposing clinically approved JAK1/JAK2 inhibitors for type 1 diabetes., (© 2017 by the American Diabetes Association.)

Published

2017

44. Cognate antigen engagement on parenchymal cells stimulates CD8 + T cell proliferation in situ.

Author

Sutherland RM, Londrigan SL, Brady JL, Carrington EM, Marchingo JM, Heinzel S, Hodgkin PD, Graham KL, Kay TW, Zhan Y, and Lew AM

Subjects

Animals, Antigen Presentation immunology, CD8-Positive T-Lymphocytes immunology, Female, Inflammation immunology, Interleukin-2 metabolism, Islets of Langerhans cytology, Islets of Langerhans immunology, Lymph Nodes immunology, Male, Mice, Mice, Transgenic, Models, Biological, Parenchymal Tissue immunology, Antigens immunology, CD8-Positive T-Lymphocytes cytology, Cell Proliferation, Ovalbumin immunology, Parenchymal Tissue cytology

Abstract

T-cell responses are initiated upon cognate presentation by professional antigen presenting cells in lymphoid tissue. T cells then migrate to inflamed tissues, but further T-cell stimulation in these parenchymal target sites is not well understood. Here we show that T-cell expansion within inflamed tissues is a distinct phase that is neither a classical primary nor classical secondary response. This response, which we term 'the mezzanine response', commences within days after initial antigen encounter, unlike the secondary response that usually occurs weeks after priming. A further distinction of this response is that T-cell proliferation is driven by parenchymal cell antigen presentation, without requiring professional antigen presenting cells, but with increased dependence on IL-2. The mezzanine response might, therefore, be a new target for inhibiting T-cell responses in allograft rejection and autoimmunity or for enhancing T-cell responses in the context of microbial or tumour immunity.

Published

2017

45. Re-addressing the 2013 consensus guidelines for the diagnosis of insulitis in human type 1 diabetes: is change necessary?

Author

Campbell-Thompson ML, Atkinson MA, Butler AE, Giepmans BN, von Herrath MG, Hyöty H, Kay TW, Morgan NG, Powers AC, Pugliese A, Richardson SJ, and In't Veld PA

Subjects

Humans, Insulin, Mice, Inbred NOD, Pancreatic Diseases, Diabetes Mellitus, Type 1, Islets of Langerhans

Published

2017

46. First Report of Successful Total Pancreatectomy and Islet Autotransplant in Australia.

Author

Geyer MC, Coates PT, Khurana S, Chen JW, Kay TW, Balamurugan AN, Couper JJ, Radford T, Drogemuller CJ, Loudovaris T, Pathi R, Wilks MJ, and Couper RT

Subjects

Australia, Child, Preschool, Humans, Male, Pancreatic Ducts pathology, Pancreatic Ducts surgery, Transplantation, Autologous, Treatment Outcome, Islets of Langerhans Transplantation methods, Pancreatectomy methods, Pancreatitis surgery

Published

2017

47. Disruption of Serinc1, which facilitates serine-derived lipid synthesis, fails to alter macrophage function, lymphocyte proliferation or autoimmune disease susceptibility.

Author

Chu EP, Elso CM, Pollock AH, Alsayb MA, Mackin L, Thomas HE, Kay TW, Silveira PA, Mansell AS, Gaus K, and Brodnicki TC

Subjects

Animals, Cell Separation, Diabetes Mellitus, Experimental immunology, Disease Models, Animal, Flow Cytometry, Lipid Metabolism immunology, Macrophages immunology, Mice, Mice, Knockout, Polymerase Chain Reaction, Serine metabolism, Autoimmune Diseases immunology, Disease Susceptibility immunology, Lymphocyte Activation immunology, Macrophage Activation immunology, Membrane Proteins immunology

Abstract

During immune cell activation, serine-derived lipids such as phosphatidylserine and sphingolipids contribute to the formation of protein signaling complexes within the plasma membrane. Altering lipid composition in the cell membrane can subsequently affect immune cell function and the development of autoimmune disease. Serine incorporator 1 (SERINC1) is a putative carrier protein that facilitates synthesis of serine-derived lipids. To determine if SERINC1 has a role in immune cell function and the development of autoimmunity, we characterized a mouse strain in which a retroviral insertion abolishes expression of the Serinc1 transcript. Expression analyses indicated that the Serinc1 transcript is readily detectable and expressed at relatively high levels in wildtype macrophages and lymphocytes. The ablation of Serinc1 expression in these immune cells, however, did not significantly alter serine-derived lipid composition or affect macrophage function and lymphocyte proliferation. Analyses of Serinc1-deficient mice also indicated that systemic ablation of Serinc1 expression did not affect viability, fertility or autoimmune disease susceptibility. These results suggest that Serinc1 is dispensable for certain immune cell functions and does not contribute to previously reported links between lipid composition in immune cells and autoimmunity., (Copyright © 2016 Elsevier Ltd. All rights reserved.)

Published

2017

48. Long-term effects of islet transplantation.

Author

Holmes-Walker DJ and Kay TW

Subjects

Humans, Hypoglycemia therapy, Islets of Langerhans Transplantation methods

Abstract

Purpose of Review: Islet transplantation has made great progress in recent years. This is a remarkable technical feat but raises the question of what the long-term benefits and risks are for type I diabetes recipients., Recent Findings: Graft survival continues to improve, and recent multicenter studies show that islet transplantation is particularly effective to prevent hypoglycemic events even in those who do not become insulin-independent and to achieve excellent glycemic control. Concerns include histocompatability leucocyte antigen (HLA) sensitization and other risks including from immunosuppression that islet transplantation shares with other forms of allotransplantation., Summary: Reversal of hypoglycemia unawareness and protection from severe hypoglycemia events are two of the main benefits of islet transplantation and they persist for the duration of graft function. Islet transplantation compares favorably with other therapies for those with hypoglycemia unawareness, although new technologies have not been tested head-to-head with transplantation. HLA sensitization increases with time after transplantation especially if immunosuppression is ceased and is a risk for those who may require future transplantation as well as being associated with loss of graft function.

Published

2016

49. Rotavirus acceleration of type 1 diabetes in non-obese diabetic mice depends on type I interferon signalling.

Author

Pane JA, Fleming FE, Graham KL, Thomas HE, Kay TW, and Coulson BS

Subjects

Animals, Diabetes Mellitus, Experimental genetics, Diabetes Mellitus, Experimental pathology, Diabetes Mellitus, Experimental virology, Diabetes Mellitus, Type 1 genetics, Diabetes Mellitus, Type 1 pathology, Diabetes Mellitus, Type 1 virology, Interferon Type I genetics, Mice, Mice, Inbred NOD, Mice, Knockout, Receptor, Interferon alpha-beta genetics, Receptor, Interferon alpha-beta immunology, Rotavirus Infections genetics, Rotavirus Infections pathology, Signal Transduction genetics, Th1 Cells immunology, Th1 Cells pathology, Diabetes Mellitus, Experimental immunology, Diabetes Mellitus, Type 1 immunology, Interferon Type I immunology, Rotavirus immunology, Rotavirus Infections immunology, Signal Transduction immunology

Abstract

Rotavirus infection is associated with childhood progression to type 1 diabetes. Infection by monkey rotavirus RRV accelerates diabetes onset in non-obese diabetic (NOD) mice, which relates to regional lymph node infection and a T helper 1-specific immune response. When stimulated ex vivo with RRV, plasmacytoid dendritic cells (pDCs) from naïve NOD mice secrete type I interferon, which induces the activation of bystander lymphocytes, including islet-autoreactive T cells. This is our proposed mechanism for diabetes acceleration by rotaviruses. Here we demonstrate bystander lymphocyte activation in RRV-infected NOD mice, which showed pDC activation and strong upregulation of interferon-dependent gene expression, particularly within lymph nodes. The requirement for type I interferon signalling was analysed using NOD mice lacking a functional type I interferon receptor (NOD.IFNAR1(-/-) mice). Compared with NOD mice, NOD.IFNAR1(-/-) mice showed 8-fold higher RRV titers in lymph nodes and 3-fold higher titers of total RRV antibody in serum. However, RRV-infected NOD.IFNAR1(-/-) mice exhibited delayed pDC and lymphocyte activation, no T helper 1 bias in RRV-specific antibodies and unaltered diabetes onset when compared with uninfected controls. Thus, the type I interferon signalling induced by RRV infection is required for bystander lymphocyte activation and accelerated type 1 diabetes onset in genetically susceptible mice.

Published

2016

50. Perinatal tolerance to proinsulin is sufficient to prevent autoimmune diabetes.

Author

Jhala G, Chee J, Trivedi PM, Selck C, Gurzov EN, Graham KL, Thomas HE, Kay TW, and Krishnamurthy B

Subjects

Animals, Antigen-Presenting Cells cytology, Autoantigens, CD8-Positive T-Lymphocytes cytology, Glucose-6-Phosphatase metabolism, Immune Tolerance, Mice, Mice, Inbred C57BL, Mice, Inbred NOD, Mice, Transgenic, Diabetes Mellitus, Type 1 drug therapy, Diabetes Mellitus, Type 1 prevention & control, Proinsulin therapeutic use

Abstract

High-affinity self-reactive thymocytes are purged in the thymus, and residual self-reactive T cells, which are detectable in healthy subjects, are controlled by peripheral tolerance mechanisms. Breakdown in these mechanisms results in autoimmune disease, but antigen-specific therapy to augment natural mechanisms can prevent this. We aimed to determine when antigen-specific therapy is most effective. Islet autoantigens, proinsulin (PI), and islet-specific glucose-6-phosphatase catalytic subunit-related protein (IGRP) were expressed in the antigen-presenting cells (APCs) of autoimmune diabetes-prone nonobese diabetic (NOD) mice in a temporally controlled manner. PI expression from gestation until weaning was sufficient to completely protect NOD mice from diabetes, insulitis, and development of insulin autoantibodies. Insulin-specific T cells were significantly diminished, were naive, and did not express IFN-γ when challenged. This long-lasting effect from a brief period of treatment suggests that autoreactive T cells are not produced subsequently. We tracked IGRP 206-214 -specific CD8 + T cells in NOD mice expressing IGRP in APCs. When IGRP was expressed only until weaning, IGRP 206-214 -specific CD8 + T cells were not detected later in life. Thus, anti-islet autoimmunity is determined during early life, and autoreactive T cells are not generated in later life. Bolstering tolerance to islet antigens in the perinatal period is sufficient to impart lasting protection from diabetes.

Published

2016