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Diagnosis and Treatment > Medication

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Takuya Higashitani Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan

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Shigehiro Karashima Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan

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Daisuke Aono Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan

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Seigoh Konishi Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan
Department of Internal Medicine, Keiju Medical Center, Nanao, Ishikawa, Japan

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Mitsuhiro Kometani Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan

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Rie Oka Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan

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Masashi Demura Department of Hygiene, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan

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Kenji Furukawa Health Care Center, Japan Advanced Institute of Science and Technology, Nomi, Ishikawa, Japan

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Yuto Yamazaki Department of Pathology, Tohoku University Hospital, Sendai, Miyagi, Japan

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Hironobu Sasano Department of Pathology, Tohoku University Hospital, Sendai, Miyagi, Japan

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Takashi Yoneda Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan
Department of Health Promotion and Medicine of the Future, Kanazawa University, Kanazawa, Ishikawa, Japan

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Yoshiyu Takeda Division of Endocrinology and Hypertension, Department of Cardiovascular and Internal Medicine, Graduate School of Medical Science, Kanazawa University, Kanazawa, Ishikawa, Japan

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Summary

Renovascular hypertension (RVHT) is an important and potentially treatable form of resistant hypertension. Hypercortisolemia could also cause hypertension and diabetes mellitus. We experienced a case wherein adrenalectomy markedly improved blood pressure and plasma glucose levels in a patient with RVHT and low-level autonomous cortisol secretion. A 62-year-old Japanese man had been treated for hypertension and diabetes mellitus for 10 years. He was hospitalized because of a disturbance in consciousness. His blood pressure (BP) was 236/118 mmHg, pulse rate was 132 beats/min, and plasma glucose level was 712 mg/dL. Abdominal CT scanning revealed the presence of bilateral adrenal masses and left atrophic kidney. Abdominal magnetic resonance angiography demonstrated marked stenosis of the left main renal artery. The patient was subsequently diagnosed with atherosclerotic RVHT with left renal artery stenosis. His left adrenal lobular mass was over 40 mm and it was clinically suspected the potential for cortisol overproduction. Therefore, laparoscopic left nephrectomy and adrenalectomy were simultaneously performed, resulting in improved BP and glucose levels. Pathological studies revealed the presence of multiple cortisol-producing adrenal nodules and aldosterone-producing cell clusters in the adjacent left adrenal cortex. In the present case, the activated renin-angiotensin-aldosterone system and cortisol overproduction resulted in severe hypertension, which was managed with simultaneous unilateral nephrectomy and adrenalectomy.

Learning points:

  • Concomitant activation of the renin-angiotensin-aldosterone system and cortisol overproduction may contribute to the development of severe hypertension and lead to lethal cardiovascular complications.

  • Treatment with simultaneous unilateral nephrectomy and adrenalectomy markedly improves BP and blood glucose levels.

  • CYP11B2 immunohistochemistry staining revealed the existence of aldosterone-producing cell clusters (APCCs) in the adjacent non-nodular adrenal gland, suggesting that APCCs may contribute to aldosterone overproduction in patients with RVHT.

Taxonomy:
Clinical Overview, Gland/Organ, Adrenal, Topic, Adrenal, Hormone, Aldosterone, Cortisol, Renin, Condition/ Syndrome, Diabetes mellitus type 2, Hyperaldosteronism, Hyperosmolar hyperglycaemic state, Hypertension, Macronodular Adrenal Hyperplasia, Patient Demographics, Age, Adult, Gender, Male, Ethnicity, Asian - Japanese, Country of Treatment, Japan, Diagnosis and Treatment, Signs and Symptoms, Arteriosclerosis, Collapse, Dyslipidaemia, Hypercortisolaemia, Hypertension, Renal failure, Investigation, ACTH stimulation, Adrenal scintigraphy, Adrenal venous sampling, Aldosterone (blood), Angiography, Blood pressure, Cortisol, Creatinine, Creatinine (serum), CT scan, Dexamethasone suppression, Estimated glomerular filtration rate, Glucose (blood), Glucose (blood, fasting), Haematoxylin and eosin staining, Histopathology, HOMA, Immunohistochemistry, Insulin tolerance, MRI, PET scan, Renin plasma activity, Total cholesterol, Triglycerides, Urinalysis, Intervention, Adrenalectomy, Laparoscopic adrenalectomy, Medication, Alpha-blockers, Atorvastatin, Doxazosin, DPP4 inhibitors, Insulin, Insulin Aspart, Linagliptin, Meglitinides, Nifedipine, Repaglinide, Related Disciplines, Urology, Publication Details, Case Report Type, Novel treatment
DOI:
https://doi.org/10.1530/EDM-19-0163
Volume/Issue:
Volume 2020: Issue 1
Open access
Frank Gao Department of Endocrinology and Diabetes, The Alfred Hospital, Melbourne, Australia

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Stephen Hall Department of Medicine, Monash University and Cabrini Health, Melbourne, Australia

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Leon A Bach Department of Endocrinology and Diabetes, The Alfred Hospital, Melbourne, Australia
Department of Medicine (Alfred), Monash University, Melbourne, Australia

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Summary

Sodium/glucose co-transporter 2 (SGLT2) inhibitors are novel oral hypoglycaemic agents that are increasingly used in the management of type 2 diabetes mellitus (T2DM). They are now recommended as second-line pharmacotherapy (in conjunction with metformin) in patients with type 2 diabetes and established atherosclerotic heart disease, heart failure or chronic kidney disease due to their favourable effects on cardiovascular and renal outcomes. We report a case of a 69-year-old man who developed muscle pain, weakness and wasting after commencing the SGLT2 inhibitor empagliflozin. This persisted for 1 year before he underwent resistance testing, which confirmed muscle weakness. His symptoms resolved within weeks of ceasing empagliflozin, with improvement in muscle strength on clinical assessment and resistance testing and reversal of MRI changes. No other cause of myopathy was identified clinically, on biochemical assessment or imaging, suggesting that empagliflozin was the cause of his myopathy.

Learning points:

  • Empagliflozin, a commonly used SGLT2 inhibitor, was associated with myopathy.

  • A high degree of suspicion is required to diagnose drug-induced myopathy, with a temporal relationship between starting the medication and symptom onset being the main indicator.

  • Recognition of drug-induced myopathy is essential, as discontinuation of the offending drug typically improves symptoms.

Taxonomy:
Clinical Overview, Gland/Organ, Pancreas, Topic, Diabetes, Hormone, Insulin, Condition/ Syndrome, Diabetes mellitus type 2, Iatrogenic disorder, Myositis, Patient Demographics, Age, Adult, Gender, Male, Ethnicity, White, Country of Treatment, Australia, Diagnosis and Treatment, Signs and Symptoms, Diabetes mellitus type 2, Fatigue, Muscle atrophy, Myalgia, Myasthaenia, Myopathy, Oedema, Polyuria, Weight loss, Investigation, Exercise tolerance, MRI, Medication, Atorvastatin, Empagliflozin, Insulin, Insulin Aspart, SGLT2 inhibitors, Publication Details, Case Report Type, Unusual effects of medical treatment
DOI:
https://doi.org/10.1530/EDM-20-0017
Volume/Issue:
Volume 2020: Issue 1
Open access
Shivani Patel Department of Diabetes and Endocrinology, St Vincent’s Hospital Sydney, Darlinghurst, New South Wales, Australia
Diabetes and Metabolism, Garvan Institute of Medical Research, Sydney, New South Wales, Australia

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Venessa Chin The Kinghorn Cancer Centre, Sydney, New South Wales, Australia
St Vincent’s Clinical School, UNSW Sydney, Darlinghurst, New South Wales, Australia

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Jerry R Greenfield Department of Diabetes and Endocrinology, St Vincent’s Hospital Sydney, Darlinghurst, New South Wales, Australia
Diabetes and Metabolism, Garvan Institute of Medical Research, Sydney, New South Wales, Australia
St Vincent’s Clinical School, UNSW Sydney, Darlinghurst, New South Wales, Australia

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Summary

Durvalumab is a programmed cell death ligand 1 inhibitor, which is now approved in Australia for use in non-small-cell lung and urothelial cancers. Autoimmune diabetes is a rare immune-related adverse effect associated with the use of immune checkpoint inhibitor therapy. It is now being increasingly described reflecting the wider use of immune checkpoint inhibitor therapy. We report the case of a 49-year-old female who presented with polyuria, polydipsia and weight loss, 3 months following the commencement of durvalumab. On admission, she was in severe diabetic ketoacidosis with venous glucose: 20.1 mmol/L, pH: 7.14, bicarbonate 11.2 mmol/L and serum beta hydroxybutyrate: >8.0 mmol/L. She had no personal or family history of diabetes or autoimmune disease. Her HbA1c was 7.8% and her glutamic acid decarboxylase (GAD) antibodies were mildly elevated at 2.2 mU/L (reference range: <2 mU/L) with negative zinc transporter 8 (ZnT8) and islet cell (ICA) antibodies. Her fasting C-peptide was low at 86 pmol/L (reference range: 200–1200) with a corresponding serum glucose of 21.9 mmol/L. She was promptly stabilised with an insulin infusion in intensive care and discharged on basal bolus insulin. Durvalumab was recommenced once her glycaemic control had stabilised. Thyroid function tests at the time of admission were within normal limits with negative thyroid autoantibodies. Four weeks post discharge, repeat thyroid function tests revealed hypothyroidism, with an elevated thyroid-stimulating hormone (TSH) at 6.39 mIU/L (reference range: 0.40–4.80) and low free T4: 5.9 pmol/L (reference range: 8.0–16.0). These findings persisted with repeat testing despite an absence of clinical symptoms. Treatment with levothyroxine was commenced after excluding adrenal insufficiency (early morning cortisol: 339 nmol/L) and hypophysitis (normal pituitary on MRI).

Learning points:

  • Durvalumab use is rarely associated with fulminant autoimmune diabetes, presenting with severe DKA.

  • Multiple endocrinopathies can co-exist with the use of a single immune checkpoint inhibitors; thus, patients should be regularly monitored.

  • Regular blood glucose levels should be performed on routine pathology on all patients on immune checkpoint inhibitor.

  • Clinician awareness of immunotherapy-related diabetes needs to increase in an attempt to detect hyperglycaemia early and prevent DKA.

Taxonomy:
Clinical Overview, Gland/Organ, Pancreas, Thyroid, Topic, Thyroid, Hormone, Cortisol, Insulin, Thyroxine (T4), TSH, Condition/ Syndrome, Autoimmune disorders, Diabetes mellitus type 1, Diabetic ketoacidosis, Hyperglycaemia, Hypothyroidism, Patient Demographics, Age, Adult, Gender, Female, Ethnicity, White, Country of Treatment, Australia, Diagnosis and Treatment, Signs and Symptoms, Diabetes mellitus type 1, Diabetic ketoacidosis, Fatigue, Hyperglycaemia, Hypothyroidism, Polydipsia, Polyuria, Vision - blurred, Weight loss, Investigation, Beta-hydroxybutyrate, Bicarbonate, Cortisol (9am), C-peptide (blood), FT4, GADA, Glucose (blood), Haemoglobin A1c, pH (blood), Thyroid function, TSH, Medication, Insulin, Insulin Aspart, Insulin glargine, Levothyroxine, Related Disciplines, Oncology, Publication Details, Case Report Type, Unusual effects of medical treatment
DOI:
https://doi.org/10.1530/EDM-19-0098
Volume/Issue:
Volume 2019: Issue 1
Open access
Jose León Mengíbar Endocrinology and Nutrition Department, Parc Taulí University Hospital, Sabadell, Barcelona, Spain

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Ismael Capel Endocrinology and Nutrition Department, Parc Taulí University Hospital, Sabadell, Barcelona, Spain

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Teresa Bonfill Medical Oncology Department, Parc Taulí University Hospital, Sabadell, Barcelona, Spain

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Isabel Mazarico Endocrinology and Nutrition Department, Parc Taulí University Hospital, Sabadell, Barcelona, Spain

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Laia Casamitjana Espuña Endocrinology and Nutrition Department, Parc Taulí University Hospital, Sabadell, Barcelona, Spain

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Assumpta Caixàs Endocrinology and Nutrition Department, Parc Taulí University Hospital, Sabadell, Barcelona, Spain

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Mercedes Rigla Endocrinology and Nutrition Department, Parc Taulí University Hospital, Sabadell, Barcelona, Spain

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Summary

Durvalumab, a human immunoglobulin G1 kappa monoclonal antibody that blocks the interaction of programmed cell death ligand 1 (PD-L1) with the PD-1 and CD80 (B7.1) molecules, is increasingly used in advanced neoplasias. Durvalumab use is associated with increased immune-related adverse events. We report a case of a 55-year-old man who presented to our emergency room with hyperglycaemia after receiving durvalumab for urothelial high-grade non-muscle-invasive bladder cancer. On presentation, he had polyuria, polyphagia, nausea and vomiting, and laboratory test revealed diabetic ketoacidosis (DKA). Other than durvalumab, no precipitating factors were identified. Pre-durvalumab blood glucose was normal. The patient responded to treatment with intravenous fluids, insulin and electrolyte replacement. Simultaneously, he presented a thyroid hormone pattern that evolved in 10 weeks from subclinical hyperthyroidism (initially attributed to iodinated contrast used in a previous computerised tomography) to overt hyperthyroidism and then to severe primary hypothyroidism (TSH: 34.40 µU/mL, free thyroxine (FT4): <0.23 ng/dL and free tri-iodothyronine (FT3): 0.57 pg/mL). Replacement therapy with levothyroxine was initiated. Finally, he was tested positive for anti-glutamic acid decarboxylase (GAD65), anti-thyroglobulin (Tg) and antithyroid peroxidase (TPO) antibodies (Abs) and diagnosed with type 1 diabetes mellitus (DM) and silent thyroiditis caused by durvalumab. When durvalumab was stopped, he maintained the treatment of multiple daily insulin doses and levothyroxine. Clinicians need to be alerted about the development of endocrinopathies, such as DM, DKA and primary hypothyroidism in the patients receiving durvalumab.

Learning points:

  • Patients treated with anti-PD-L1 should be screened for the most common immune-related adverse events (irAEs).

  • Glucose levels and thyroid function should be monitored before and during the treatment.

  • Durvalumab is mainly associated with thyroid and endocrine pancreas dysfunction.

  • In the patients with significant autoimmune background, risk–benefit balance of antineoplastic immunotherapy should be accurately assessed.

Taxonomy:
Clinical Overview, Gland/Organ, Pancreas, Topic, Diabetes, Hormone, Insulin, Thyroxine (T4), Triiodothyronine (T3), TSH, Condition/ Syndrome, Autoimmune disorders, Diabetes mellitus type 1, Diabetic ketoacidosis, Hyperglycaemia, Hyperkalaemia, Hyperthyroidism, Hyponatraemia, Hypothyroidism, Thyroiditis, Patient Demographics, Age, Adult, Gender, Male, Ethnicity, White, Country of Treatment, Spain, Diagnosis and Treatment, Signs and Symptoms, Constipation, Diabetes mellitus type 1, Diabetic ketoacidosis, Dizziness, Fatigue, Hyperglycaemia, Hyperkalaemia, Hyperthyroidism, Hyponatraemia, Hypothyroidism, Myasthaenia, Nausea, Oedema, Polydipsia, Polyphagia, Polyuria, Vomiting, Weight gain, Xeroderma, Investigation, ACTH stimulation, Anion gap, Beta-hydroxybutyrate, Bicarbonate, Cortisol, C-peptide (blood), CT scan, FT3, FT4, GADA, Glucose (blood), Glucose (blood, fasting), Haemoglobin A1c, pH (blood), Thyroid antibodies, Thyroid function, TSH, Intervention, Fluid repletion, Medication, Insulin, Insulin Aspart, Insulin glargine, Levothyroxine, Publication Details, Case Report Type, Unusual effects of medical treatment
DOI:
https://doi.org/10.1530/EDM-19-0045
Volume/Issue:
Volume 2019: Issue 1
Open access
Harmony Thompson Department of Endocrinology and Diabetes, Canterbury District Health Board, Christchurch, New Zealand

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Helen Lunt Department of Endocrinology and Diabetes, Canterbury District Health Board, Christchurch, New Zealand
Department of Medicine, University of Otago Christchurch, Christchurch, New Zealand

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Cate Fleckney Department of Endocrinology and Diabetes, Canterbury District Health Board, Christchurch, New Zealand

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Steven Soule Department of Endocrinology and Diabetes, Canterbury District Health Board, Christchurch, New Zealand
Department of Medicine, University of Otago Christchurch, Christchurch, New Zealand

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Summary

An adolescent with type 1 diabetes and a history of self-harm, which included intentional overdoses and insulin omission, presented with an insulin degludec overdose. She had been commenced on the ultra-long-acting insulin, degludec, with the aim of reducing ketoacidosis episodes in response to intermittent refusal to take insulin. Insulin degludec was administered under supervision as an outpatient. Because it was anticipated that she would attempt a degludec overdose at some stage, the attending clinicians implemented a proactive management plan for this (and related) scenarios. This included long-term monitoring of interstitial glucose using the Abbott Freestyle Libre flash glucose monitor. The patient took a witnessed overdose of 242 units of degludec (usual daily dose, 32 units). She was hospitalised an hour later. Inpatient treatment was guided primarily by interstitial glucose results, with capillary and venous glucose tests used as secondary measures to assess the accuracy of interstitial glucose values. Four days of inpatient treatment was required. The patient was managed with high glycaemic loads of food and also intermittent intravenous dextrose. No hypoglycaemia was documented during the admission. In summary, while a degludec overdose may require several days of inpatient management, in situations where proactive management is an option and the dose administered is relatively modest, it may be possible to avoid significant hypoglycaemia. In addition, this case demonstrates that inpatient interstitial glucose monitoring may have a role in managing insulin overdose, especially in situations where the effect of the insulin overdose on glucose levels is likely to be prolonged.

Learning points:

  • Degludec overdoses have a prolonged effect on blood glucose levels, but if the clinical situation allows for early detection and management, treatment may prove easier than that which is typically needed following overdoses of a similar dose of shorter acting insulins.

  • Inpatient real-time interstitial monitoring helped guide management, which in this context included the prescription of high dietary carbohydrate intake (patient led) and intravenous 10% dextrose (nurse led).

  • Use of inpatient interstitial glucose monitoring to guide therapy might be considered ‘off label’ use, thus, both staff and also patients should be aware of the limitations, as well as the benefits, of interstitial monitoring systems.

  • The Libre flash glucose monitor provided nurses with low cost, easy-to-use interstitial glucose results, but it is nevertheless advisable to check these results against conventional glucose tests, for example, capillary ‘finger-stick’ or venous glucose tests.

Taxonomy:
Clinical Overview, Gland/Organ, Pancreas, Topic, Diabetes, Hormone, Insulin, Condition/ Syndrome, Diabetes mellitus type 1, Patient Demographics, Age, Adolescent/young adult, Gender, Female, Ethnicity, White, Country of Treatment, New Zealand, Diagnosis and Treatment, Signs and Symptoms, Behavioural problems, Diabetes mellitus type 1, Investigation, Continuous glucose monitoring, Glucose (blood), Insulin, Potassium, Intervention, Diet, Medication, Glucose, Insulin, Insulin Aspart, Related Disciplines, Nursing, Paediatrics, Publication Details, Case Report Type, Novel treatment
DOI:
https://doi.org/10.1530/EDM-18-0044
Volume/Issue:
Volume 2018: Issue 1
Open access
Eleanor P Thong Department of Endocrinology, Monash Health, Clayton, Australia
Monash Centre for Health Research and Implementation, Clayton, Australia

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Sarah Catford Department of Endocrinology, Monash Health, Clayton, Australia
Hudson Institute of Medical Research, Clayton, Australia

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Julie Fletcher Department of Anatomical Pathology, Concord Repatriation General Hospital, Concord, Australia

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Phillip Wong Department of Endocrinology, Monash Health, Clayton, Australia
Hudson Institute of Medical Research, Clayton, Australia

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Peter J Fuller Department of Endocrinology, Monash Health, Clayton, Australia
Hudson Institute of Medical Research, Clayton, Australia

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Helena Teede Department of Endocrinology, Monash Health, Clayton, Australia
Monash Centre for Health Research and Implementation, Clayton, Australia

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Frances Milat Department of Endocrinology, Monash Health, Clayton, Australia
Hudson Institute of Medical Research, Clayton, Australia

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Summary

The association between type 1 diabetes mellitus (T1DM) and bone health has garnered interest over the years. Fracture risk is known to be increased in individuals with T1DM, although bone health assessment is not often performed in the clinical setting. We describe the case of a 21-year-old male with longstanding T1DM with multilevel vertebral fractures on imaging, after presenting with acute back pain without apparent trauma. Dual-energy X-ray absorptiometry (DXA) revealed significantly reduced bone mineral density at the lumbar spine and femoral neck. Extensive investigations for other secondary or genetic causes of osteoporosis were unremarkable, apart from moderate vitamin D deficiency. High-resolution peripheral quantitative computed tomography and bone biospy revealed significant alterations of trabecular bone microarchitecture. It later transpired that the patient had sustained vertebral fractures secondary to unrecognised nocturnal hypoglycaemic seizures. Intravenous zoledronic acid was administered for secondary fracture prevention. Despite anti-resorptive therapy, the patient sustained a new vertebral fracture after experiencing another hypoglycaemic seizure in his sleep. Bone health in T1DM is complex and not well understood. There are significant challenges in the assessment and management of osteoporosis in T1DM, particularly in young adults, where fracture prediction tools have not been validated. Clinicians should be aware of hypoglycaemia as a significant risk factor for fracture in patients with T1DM.

Learning points:

  • Type 1 diabetes mellitus (T1DM) is a secondary cause of osteoporosis, characterised by reduced bone mass and disturbed bone microarchitecture.

  • Hypoglycaemic seizures generate sufficient compression forces along the thoracic column and can cause fractures in individuals with compromised bone quality.

  • Unrecognised hypoglycaemic seizures should be considered in patients with T1DM presenting with fractures without a history of trauma.

  • Patients with T1DM have increased fracture risk and risk factors should be addressed. Evaluation of bone microarchitecture may provide further insights into mechanisms of fracture in T1DM.

  • Further research is needed to guide the optimal screening and management of bone health in patients with T1DM.

Taxonomy:
Clinical Overview, Gland/Organ, Bone, Topic, Bone, Hormone, Insulin, Condition/ Syndrome, Diabetes mellitus type 1, Hypoglycaemia, Osteoporosis, Patient Demographics, Age, Adolescent/young adult, Gender, Male, Ethnicity, White, Country of Treatment, Australia, Diagnosis and Treatment, Signs and Symptoms, Back pain, Bone fracture(s), Diabetes mellitus type 1, Hypoglycaemia, Osteoporosis, Seizures, Investigation, Bone biopsy, Bone mineral density, CT scan, DEXA scan, Haemoglobin A1c, MRI, Trabecular thickness, Vitamin D, X-ray, Intervention, Analgesics, Medication, Bisphosphonates, Insulin, Insulin Aspart, Teriparatide, Vitamin D, Zoledronic acid, Publication Details, Case Report Type, Insight into disease pathogenesis or mechanism of therapy
DOI:
https://doi.org/10.1530/EDM-18-0010
Volume/Issue:
Volume 2018: Issue 1
Open access
Clarissa Ern Hui Fang Bariatric Medicine Service, Centre for Diabetes, Endocrinology and Metabolism, Galway University Hospitals, Galway, Ireland

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Mohammed Faraz Rafey Bariatric Medicine Service, Centre for Diabetes, Endocrinology and Metabolism, Galway University Hospitals, Galway, Ireland
HRB Clinical Research Facility, National University of Ireland Galway, Galway, Ireland

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Aine Cunningham Bariatric Medicine Service, Centre for Diabetes, Endocrinology and Metabolism, Galway University Hospitals, Galway, Ireland

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Sean F Dinneen Bariatric Medicine Service, Centre for Diabetes, Endocrinology and Metabolism, Galway University Hospitals, Galway, Ireland
HRB Clinical Research Facility, National University of Ireland Galway, Galway, Ireland

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Francis M Finucane Bariatric Medicine Service, Centre for Diabetes, Endocrinology and Metabolism, Galway University Hospitals, Galway, Ireland
HRB Clinical Research Facility, National University of Ireland Galway, Galway, Ireland

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Summary

A 28-year-old male presented with 2 days of vomiting and abdominal pain, preceded by 2 weeks of thirst, polyuria and polydipsia. He had recently started risperidone for obsessive-compulsive disorder. He reported a high dietary sugar intake and had a strong family history of type 2 diabetes mellitus (T2DM). On admission, he was tachycardic, tachypnoeic and drowsy with a Glasgow Coma Scale (GCS) of 10/15. We noted axillary acanthosis nigricans and obesity (BMI 33.2 kg/m2). Dipstick urinalysis showed ketonuria and glycosuria. Blood results were consistent with diabetic ketoacidosis (DKA), with hyperosmolar state. We initiated our DKA protocol, with intravenous insulin, fluids and potassium, and we discontinued risperidone. His obesity, family history of T2DM, acanthosis nigricans and hyperosmolar state prompted consideration of T2DM presenting with ‘ketosis-prone diabetes’ (KPD) rather than T1DM. Antibody markers of beta-cell autoimmunity were subsequently negative. Four weeks later, he had modified his diet and lost weight, and his metabolic parameters had normalised. We reduced his total daily insulin dose from 35 to 18 units and introduced metformin. We stopped insulin completely by week 7. At 6 months, his glucometer readings and glycated haemoglobin (HbA1c) level had normalised.

Learning points:

  • Risperidone-induced diabetic ketoacidosis (DKA) is not synonymous with type 1 diabetes, even in young white patients and may be a manifestation of ‘ketosis-prone’ type 2 diabetes (KPD).

  • KPD is often only confirmed after the initial presentation, when islet autoimmunity and cautious phasing out of insulin therapy have been assessed, and emergency DKA management remains the same.

  • As in other cases of KPD, a family history of T2DM and presence of cutaneous markers of insulin resistance were important clinical features suggestive of an alternative aetiology for DKA.

Taxonomy:
Clinical Overview, Gland/Organ, Pancreas, Topic, Diabetes, Hormone, Insulin, Condition/ Syndrome, Diabetes mellitus type 2, Diabetic ketoacidosis, Patient Demographics, Age, Adult, Gender, Male, Ethnicity, White, Country of Treatment, Ireland, Diagnosis and Treatment, Signs and Symptoms, Abdominal pain, Acanthosis nigricans, Altered level of consciousness, Diabetes mellitus type 2, Diabetic ketoacidosis, Glucosuria, Ketonuria, Obesity, Polydipsia, Polyuria, Somnolence, Tachycardia, Tachypnoea, Vomiting, Investigation, Alanine aminotransferase, Beta-hydroxybutyrate, Bicarbonate, BMI, Creatinine, Estimated glomerular filtration rate, Glucose (blood), Haemoglobin A1c, Plasma osmolality, Sodium, Urea and electrolytes, Urinalysis, Weight, Intervention, Diet, Fluid repletion, Medication, Antibiotics, Antivirals, Insulin, Insulin Aspart, Insulin glargine, Metformin, Potassium chloride, Promethazine, Risperidone, Related Disciplines, Dermatology, Publication Details, Case Report Type, Unique/unexpected symptoms or presentations of a disease
DOI:
https://doi.org/10.1530/EDM-18-0031
Volume/Issue:
Volume 2018: Issue 1
Open access
Akihiko Ando Division of Endocrinology and Metabolism, Department of Internal Medicine, Jichi Medical University, Tochigi, Japan

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Shoichiro Nagasaka Division of Endocrinology and Metabolism, Department of Internal Medicine, Jichi Medical University, Tochigi, Japan
Division of Diabetes, Metabolism and Endocrinology, Department of Internal Medicine, Showa University Fujigaoka Hospital, Kanagawa Japan

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Shun Ishibashi Division of Endocrinology and Metabolism, Department of Internal Medicine, Jichi Medical University, Tochigi, Japan

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Summary

We report a case of a woman with diabetes mellitus caused by a genetic defect in ABCC8-coding sulfonylurea receptor 1 (SUR1), a subunit of the ATP-sensitive potassium (KATP) channel protein. She was diagnosed with diabetes at 7 days after birth. After intravenous insulin drip for 1 month, her hyperglycaemia remitted. At the age of 13 years, her diabetes relapsed, and after that she had been treated by intensive insulin therapy for 25 years with relatively poor glycaemic control. She was switched to oral sulfonylurea therapy and attained euglycaemia. In addition, her insulin secretory capacity was ameliorated gradually.

Learning points:

  • Genetic testing should be considered in any individuals or family with diabetes that occurred within the first year or so of life.

  • Sulfonylurea can achieve good glycaemic control in patients with KATP channel mutations by restoring endogenous insulin secretion, even if they were treated with insulin for decades.

  • Early screening and genetic testing are important to improve the prognosis of patients with neonatal diabetes mellitus arising from ABCC8 or KCNJ11 mutation.

Taxonomy:
Clinical Overview, Hormone, Insulin, Condition/ Syndrome, Hyperglycaemia, Neonatal diabetes, Patient Demographics, Age, Adult, Gender, Female, Ethnicity, White, Country of Treatment, Japan, Diagnosis and Treatment, Signs and Symptoms, Fatigue, Hyperglycaemia, Polydipsia, Investigation, C-peptide (24-hour urine), C-peptide (blood), GADA, Glucagon, Glucose (blood, fasting), Glucose tolerance (oral), Haemoglobin A1c, Insulin, Molecular genetic analysis, Urinalysis, Medication, Gliclazide, Insulin, Insulin Aspart, Insulin lispro, Sulphonylureas, Related Disciplines, Genetics, Publication Details, Case Report Type, Unusual effects of medical treatment
DOI:
https://doi.org/10.1530/EDM-18-0005
Volume/Issue:
Volume 2018: Issue 1
Open access
Ali A Zaied Divisions of Pulmonary and Critical Care Medicine, Mayo Clinic, Jacksonville, Florida, USA

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Halis K Akturk Divisions of Endocrinology, Mayo Clinic, Jacksonville, Florida, USA

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Richard W Joseph Divisions of Hematology and Oncology, Mayo Clinic, Jacksonville, Florida, USA

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Augustine S Lee Divisions of Pulmonary and Critical Care Medicine, Mayo Clinic, Jacksonville, Florida, USA

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Summary

Nivolumab, a monoclonal antibody against programmed cell death-1 receptor, is increasingly used in advanced cancers. While nivolumab use enhances cancer therapy, it is associated with increased immune-related adverse events. We describe an elderly man who presented in ketoacidosis after receiving nivolumab for metastatic renal cell carcinoma. On presentation, he was hyperpneic and laboratory analyses showed hyperglycemia and anion-gapped metabolic acidosis consistent with diabetic ketoacidosis. No other precipitating factors, besides nivolumab, were identified. Pre-nivolumab blood glucose levels were normal. The patient responded to treatment with intravenous fluids, insulin and electrolyte replacement. He was diagnosed with insulin-dependent autoimmune diabetes mellitus secondary to nivolumab. Although nivolumab was stopped, he continued to require multiple insulin injection therapy till his last follow-up 7 months after presentation. Clinicians need to be alerted to the development of diabetes mellitus and diabetic ketoacidosis in patients receiving nivolumab.

Learning points:

  • Diabetic ketoacidosis should be considered in the differential of patients presenting with metabolic acidosis following treatment with antibodies to programmed cell death-1 receptor (anti-PD-1).

  • Autoimmune islet cell damage is the presumed mechanism for how insulin requiring diabetes mellitus can develop de novo following administration of anti-PD-1.

  • Because anti-PD-1 works by the activation of T-cells and reduction of ‘self-tolerance’, other autoimmune disorders are likely to be increasingly recognized with increased use of these agents.

Taxonomy:
Clinical Overview, Gland/Organ, Pancreas, Topic, Diabetes, Hormone, Insulin, Condition/ Syndrome, Autoimmune disorders, Diabetes mellitus type 1, Diabetic ketoacidosis, Hyperglycaemia, Hyperkalaemia, Hyponatraemia, Metabolic acidosis, Metastatic carcinoma, Patient Demographics, Age, Geriatric, Gender, Male, Ethnicity, White, Country of Treatment, United States, Diagnosis and Treatment, Signs and Symptoms, Abdominal pain, Diabetes mellitus type 1, Diabetic ketoacidosis, Dyspnoea, Fatigue, Hyperglycaemia, Hyperkalaemia, Hyperpnoea, Hyponatraemia, Metabolic acidosis, Polyuria, Investigation, Albumin, Bicarbonate, Brain natriuretic peptide, Calcium (serum), Chloride, C-peptide (blood), CT scan, Glucose (blood), Glucose (blood, fasting), Glucose (urine), Haemoglobin A1c, Ketones (urine), Magnesium, Platelet count, Potassium, Red blood cell count, Sodium, Urea and electrolytes, Urinalysis, White blood cell count, White blood cell differential count, X-ray, Intervention, Fluid repletion, Medication, Aspirin, Insulin, Insulin Aspart, Insulin glargine, Lisinopril, Nivolumab, Tyrosine-kinase inhibitors, Related Disciplines, Oncology, Publication Details, Case Report Type, Unusual effects of medical treatment
DOI:
https://doi.org/10.1530/EDM-17-0174
Volume/Issue:
Volume 2018: Issue 1
Open access
Ploutarchos Tzoulis Department of Diabetes, The Whittington Hospital, Whittington Health NHS Trust, London, UK

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Richard W Corbett Department of Medicine, Imperial College London, London, UK

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Swarupini Ponnampalam Department of Diabetes, The Whittington Hospital, Whittington Health NHS Trust, London, UK

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Elly Baker Department of Diabetes, The Whittington Hospital, Whittington Health NHS Trust, London, UK

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Daniel Heaton Department of Diabetes, The Whittington Hospital, Whittington Health NHS Trust, London, UK

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Triada Doulgeraki Medical School, University of Athens, Athens, Greece

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Justin Stebbing Department of Surgery and Cancer, Imperial College London, London, UK

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Summary

Five days following the 3rd cycle of nivolumab, a monoclonal antibody, which acts as immune checkpoint inhibitor against the programmed cell death protein-1, for metastatic lung adenocarcinoma, a 56-year-old woman presented at the hospital critically ill. On admission, she had severe diabetic ketoacidosis (DKA), as evidenced by venous glucose of 47 mmol/L, blood ketones of 7.5 mmol/L, pH of 6.95 and bicarbonate of 6.6 mmol/L. She has had no personal or family history of diabetes mellitus (DM), while random venous glucose, measured 1 week prior to hospitalisation, was 6.1 mmol/L. On admission, her HbA1c was 8.2% and anti-GAD antibodies were 12 kIU/L (0–5 kU/L), while islet cell antibodies and serum C-peptide were undetectable. Nivolumab was recommenced without the development of other immune-mediated phenomena until 6 months later, when she developed hypothyroidism with TSH 18 U/L and low free T4. She remains insulin dependent and has required levothyroxine replacement, while she has maintained good radiological and clinical response to immunotherapy. This case is notable for the rapidity of onset and profound nature of DKA at presentation, which occurred two months following commencement of immunotherapy. Despite the association of nivolumab with immune-mediated endocrinopathies, only a very small number of patients developing type 1 DM has been reported to date. Patients should be closely monitored for hyperglycaemia and thyroid dysfunction prior to and periodically during immunotherapy.

Learning points:

  • Nivolumab can induce fulminant type 1 diabetes, resulting in DKA.

  • Nivolumab is frequently associated with thyroid dysfunction, mostly hypothyroidism.

  • Nivolumab-treated patients should be monitored regularly for hyperglycaemia and thyroid dysfunction.

  • Clinicians should be aware and warn patients of potential signs and symptoms of severe hyperglycaemia.

Taxonomy:
Clinical Overview, Gland/Organ, Pancreas, Thyroid, Topic, Diabetes, Hormone, Insulin, Thyroxine (T4), TSH, Condition/ Syndrome, Adenocarcinoma, Diabetes mellitus type 1, Diabetic ketoacidosis, Hyperglycaemia, Hypothyroidism, Metabolic acidosis, Metastatic carcinoma, Thyroiditis, Patient Demographics, Age, Adult, Gender, Female, Ethnicity, White, Country of Treatment, United Kingdom, Diagnosis and Treatment, Signs and Symptoms, Aggression, Agitation, Cold intolerance, Confusion, Diabetes mellitus type 1, Diabetic ketoacidosis, Fatigue, Hyperglycaemia, Hypothyroidism, Metabolic acidosis, Polydipsia, Polyuria, Weight gain, Investigation, Bicarbonate, C-peptide (blood), C-reactive protein, Creatinine (serum), FT4, GADA, Glucose (blood), Haemoglobin A1c, Ketones (plasma), TSH, Urea and electrolytes, White blood cell count, Medication, Insulin, Insulin Aspart, Insulin glargine, Levothyroxine, Nivolumab, Saline, Related Disciplines, Oncology, Publication Details, Case Report Type, Unusual effects of medical treatment
DOI:
https://doi.org/10.1530/EDM-18-0111
Volume/Issue:
Volume 2018: Issue 1
Open access