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2. Type 2 diabetes after a pregnancy with gestational diabetes among first nations women in Australia: The PANDORA study.

Author

Wood A.J., Boyle J.A., Barr E.L.M., Barzi F., Hare M.J.L., Titmuss A., Longmore D.K., Death E., Kelaart J., Kirkwood M., Graham S., Connors C., Moore E., O'Dea K., Oats J.J.N., McIntyre H.D., Zimmet P.Z., Lu Z.X., Brown A., Shaw J.E., Maple-Brown L.J., Wood A.J., Boyle J.A., Barr E.L.M., Barzi F., Hare M.J.L., Titmuss A., Longmore D.K., Death E., Kelaart J., Kirkwood M., Graham S., Connors C., Moore E., O'Dea K., Oats J.J.N., McIntyre H.D., Zimmet P.Z., Lu Z.X., Brown A., Shaw J.E., and Maple-Brown L.J.

Abstract

Aims: To determine among First Nations and Europid pregnant women the cumulative incidence and predictors of postpartum type 2 diabetes and prediabetes and describe postpartum cardiovascular disease (CVD) risk profiles. Method(s): PANDORA is a prospective longitudinal cohort of women recruited in pregnancy. Ethnic-specific rates of postpartum type 2 diabetes and prediabetes were reported for women with diabetes in pregnancy (DIP), gestational diabetes (GDM) or normoglycaemia in pregnancy over a short follow-up of 2.5 years (n = 325). Pregnancy characteristics and CVD risk profiles according to glycaemic status, and factors associated with postpartum diabetes/prediabetes were examined in First Nations women. Result(s): The cumulative incidence of postpartum type 2 diabetes among women with DIP or GDM were higher for First Nations women (48%, 13/27, women with DIP, 13%, 11/82, GDM), compared to Europid women (nil DIP or GDM p < 0.001). Characteristics associated with type 2 diabetes/prediabetes among First Nations women with GDM/DIP included, older age, multiparity, family history of diabetes, higher glucose values, insulin use and body mass index (BMI). Conclusion(s): First Nations women experience a high incidence of postpartum type 2 diabetes after GDM/DIP, highlighting the need for culturally responsive policies at an individual and systems level, to prevent diabetes and its complications.Copyright © 2021 The Author(s)

Published
2021

3. Familial Hypocalciuric Hypercalcemia in Pregnancy: Diagnostic Pitfalls.

Author

Jones A.R., Brown J., Yang J., Meyer C., Milat F., Allan C.A., Hare M.J.L., Jones A.R., Brown J., Yang J., Meyer C., Milat F., Allan C.A., and Hare M.J.L.

Abstract

Familial hypocalciuric hypercalcemia (FHH) is a group of autosomal dominant disorders caused by dysfunction of the calcium sensing receptor (CaSR) and its downstream signaling proteins, leading to generally asymptomatic hypercalcemia. During pregnancy, distinguishing FHH from primary hyperparathyroidism (PHPT) is important, as the latter is associated with adverse outcomes and can be treated surgically during pregnancy, whereas the former is benign. This case report highlights the difficulties in diagnosing FHH during pregnancy. A 32-year-old woman was found to have asymptomatic hypercalcemia at 14-weeks' gestation. Investigations showed a corrected calcium (cCa) of 2.61 mmol/L (2.10 to 2.60), ionized Ca (iCa) of 1.40 mmol/L (1.15 to 1.28), 25OHD of 33 nmol/L (75 to 250), and PTH of 9.5 pmol/L (1.5 to 7.0). The patient was treated with 2000 IU cholecalciferol daily with normalization of 25OHD. The urine calcium / creatinine clearance ratio (CCCR) was 0.0071, and neck US did not visualize a parathyroid adenoma. Upon a retrospective review of the patient's biochemistry from 2 years prior, hypercalcemia was found that was not investigated. The patient was monitored with serial iCa levels and obstetric US. She delivered a healthy boy at 38-weeks' gestation. Postnatal iCa was 1.48 mmol/L and remained elevated. Her son had elevated iCa at birth of 1.46 mmol/L (1.15 to 1.33), which rose to 1.81 mmol/L by 2 weeks. He was otherwise well. Given the familial hypercalcemia, a likely diagnosis of FHH was made. Genetic testing of the son revealed a missense mutation, NM_000388.3(CASR):c.2446A > G, in exon 7 of the CaSR, consistent with FHH type 1. To our knowledge, there are only three existing reports of FHH in pregnancy. When differentiating between FHH and PHPT in pregnancy, interpretation of biochemistry requires an understanding of changes in Ca physiology, and urine CCCR may be unreliable. If the decision is made to observe, clinical symptoms, calcium levels, and fetal US s

Published
2020

4. Moderate weight change following diabetes diagnosis and 10 year incidence of cardiovascular disease and mortality.

Author

Wareham N.J., Long G.H., Hare M.J.L., Irving G., Boothby C.E., Griffin S.J., Strelitz J., Ahern A.L., Wareham N.J., Long G.H., Hare M.J.L., Irving G., Boothby C.E., Griffin S.J., Strelitz J., and Ahern A.L.

Abstract

Aims/hypothesis: Adults with type 2 diabetes are at high risk of developing cardiovascular disease (CVD). Evidence of the impact of weight loss on incidence of CVD events among adults with diabetes is sparse and conflicting. We assessed weight change in the year following diabetes diagnosis and estimated associations with 10 year incidence of CVD events and all-cause mortality. Method(s): In a cohort analysis among 725 adults with screen-detected diabetes enrolled in the Anglo-Danish-Dutch Study of Intensive Treatment in People with Screen-Detected Diabetes in Primary Care (ADDITION)-Cambridge trial, we estimated HRs for weight change in the year following diabetes diagnosis and 10 year incidence of CVD (n = 99) and all-cause mortality (n = 95) using Cox proportional hazards regression. We used linear regression to estimate associations between weight loss and CVD risk factors. Models were adjusted for age, sex, baseline BMI, smoking, occupational socioeconomic status, cardio-protective medication use and treatment group. Result(s): Loss of >=5% body weight in the year following diabetes diagnosis was associated with improvements in HbA1c and blood lipids and a lower hazard of CVD at 10 years compared with maintaining weight (HR 0.52 [95% CI 0.32, 0.86]). The associations between weight gain vs weight maintenance and CVD (HR 0.41 [95% CI 0.15, 1.11]) and mortality (HR 1.63 [95% CI 0.83, 3.19]) were less clear. Conclusions/interpretation: Among adults with screen-detected diabetes, loss of >=5% body weight during the year after diagnosis was associated with a lower hazard of CVD events compared with maintaining weight. These results support the hypothesis that moderate weight loss may yield substantial long-term CVD reduction, and may be an achievable target outside of specialist-led behavioural treatment programmes.Copyright © 2019, The Author(s).

Published
2019

5. Cardiovascular Disease Risk in Diabetes Mellitus.

Author

Hare M.J.L., Shaw J.E., Hare M.J.L., and Shaw J.E.

Abstract

Cardiovascular disease is the leading cause of mortality and morbidity among people with diabetes mellitus. The epidemic of diabetes continues to contribute significantly to the global burden of cardiovascular disease with varying epidemiological trends in different regions and resource settings. Understanding and estimating cardiovascular risk is an essential component of diabetes care. Increasingly, assessment of absolute cardiovascular risk in individuals with diabetes is used to guide treatment targets and medical therapies. Numerous approaches to assessing cardiovascular risk in diabetes have been developed. These largely rely on traditional risk factor associations, but there is substantial ongoing research into novel biomarkers and genetics. This chapter provides an overview of cardiovascular risk in diabetes, including epidemiology, mechanisms and a particular focus on risk prediction.Copyright © 2019 S. Karger AG, Basel.

Published
2019

6. SGLT2 Inhibitors Increase the Risk of Diabetic Ketoacidosis Developing in the Community and during Hospital Admission.

Author

Lafontaine N., Wong R., Ekinci E.I., Fourlanos S., Shah S., Jones A.R., Hare M.J.L., Calder G.L., Epa D.S., George E.M., Giri R., Kotowicz M.A., Kyi M., Macisaac R.J., Nolan B.J., O'Neal D.N., Renouf D., Varadarajan S., Wong J., Xu S., Bach L.A., Hamblin P.S., Lafontaine N., Wong R., Ekinci E.I., Fourlanos S., Shah S., Jones A.R., Hare M.J.L., Calder G.L., Epa D.S., George E.M., Giri R., Kotowicz M.A., Kyi M., Macisaac R.J., Nolan B.J., O'Neal D.N., Renouf D., Varadarajan S., Wong J., Xu S., Bach L.A., and Hamblin P.S.

Abstract

Context Diabetic ketoacidosis (DKA) has been associated with the use of sodium glucose cotransporter 2 inhibitors (SGLT2is). Objective To determine the incidence, characteristics, and outcomes of DKA in SGLT2i users vs nonusers with type 2 diabetes. Design Retrospective, multicenter, controlled cohort study. Setting All public hospitals in Melbourne and Geelong (combined population of 5 million), Australia, from 1 September 2015 to 31 October 2017. Patients Consecutive cases of DKA that developed in the community, or during the course of hospital admission, in patients with type 2 diabetes Main Outcome Measures In SGLT2i users vs nonusers: (i) OR of DKA developing during hospital admission, and (ii) incidence of DKA. Results There were 162 cases of DKA (37 SGLT2i users and 125 non-SGLT2i users) with a physician-adjudicated diagnosis of type 2 diabetes. Of these, DKA developed during the course of inpatient admission in 14 (38%) SGLT2i users vs 2 (2%) non-SGLT2i users (OR, 37.4; 95% CI, 8.0 to 175.9; P < 0.0001). The incidence of DKA was 1.02 per 1000 (95% CI, 0.74 to 1.41 per 1000) in SGLT2i users vs 0.69 per 1000 (95% CI, 0.58 to 0.82 per 1000) in non-SGLT2i users (OR, 1.48; 95% CI, 1.02 to 2.15; P = 0.037). Fifteen SGLT2i users (41%) had peak blood glucose <250 mg/dL (14 mmol/L) compared with one (0.8%) non-SGLT2i user (P < 0.001). Conclusions SGLT2i users were more likely to develop DKA as an inpatient compared with non-SGLT2i users. SGLT2i use was associated with a small but significant increased risk of DKA.Copyright © 2019 Endocrine Society.

Published
2019

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