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Query: UNIPROT:P01275 (
glucagon
)
26,492
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Glucagonoma is a rare and slow-growing pancreatic tumor that usually manifests as glucagonoma syndrome. It is mainly characterized by a typical Dermatosis named necrolytic migratory
erythema
(NME), Diabetes and
glucagon
oversecretion. Deep vein thrombosis and Depression complete this set. We report the case of an advanced glucagonoma with liver spread, where all these 4D symptoms occurred but a chronic secretory Diarrhea was the most relevant feature. A 65-year-old man was referred to our center to investigate multiple hepatic nodules evidenced by abdominal tomography. He had a recent diagnosis of diabetes and complained of significant weight loss (25 kg), crusted skin lesions and episodes of a large amount of liquid diarrhea during the past 6 months. On admission, there were erythematous plaques and crusted erosions on his face, back and limbs, plus angular cheilitis and atrophic glossitis. The typical skin manifestation promptly led dermatologists to suspect glucagonoma as the source of our patient's symptoms. A contrast-enhanced abdominal computed tomography showed a hypervascularized pancreatic lesion and multiple hepatic nodules also hypervascularized in the arterial phase. Despite initial improvement of diarrhea after subcutaneous octreotide, the patient's impaired nutritional status limited other therapeutic approaches and he died of respiratory failure due to sepsis. His high levels of serum
glucagon
were not yet available so we performed an autopsy, confirming the diagnosis of metastatic glucagonoma with NME on histology. Chronic diarrhea is not a common feature in glucagonoma syndrome; however, its severity can lead to serious nutritional impairment and set a poor outcome.
...
PMID:Diarrhea: a missed D in the 4D glucagonoma syndrome. 3180 36
Glucagonoma is a hormonally active rare pancreatic neuroendocrine tumour causing an excess of
glucagon
. This is a narrative review based on a multidisciplinary approach of the tumour. Typically associated dermatosis is necrolytic migratory
erythema
(NME) which is most frequently seen at disease onset. Insulin-dependent diabetes mellitus, depression, diarrhoea, deep vein thrombosis are also identified, as parts of so-called 'D' syndrome. Early diagnosis is life saving due to potential aggressive profile and high risk of liver metastasis. NME as paraneoplastic syndrome may be present for months and even years until adequate recognition and therapy; it is remitted after successful pancreatic surgery. Thus the level of practitioners' awareness is essential. If surgery is not curative, debulking techniques may improve the clinical aspects and even the outcome in association with other procedures such as embolization of hepatic metastasis; ablation of radiofrequency type; medical therapy including chemotherapy, targeted therapy with mTOR inhibitors such as everolimus, PRRT (peptide receptor radiotherapy), and somatostatin analogues (including combinations of medical treatments). Increased awareness of the condition involves multidisciplinary practitioners.
...
PMID:Glucagonoma: From skin lesions to the neuroendocrine component (Review). 3290 95
Background:
Congenital hyperinsulinism (CHI), a rare disease of excessive and dysregulated insulin secretion, can lead to prolonged and severe hypoglycemia. Dextrose infusions are a mainstay of therapy to restore normal glycemia, but can be associated with volume overload, especially in infants. By releasing intrahepatic glucose stores,
glucagon
infusions can reduce dependency on dextrose infusions. Recent studies have reported positive outcomes with
glucagon
infusions in patients with CHI; however, to date, there are no reports describing the clinical utility of titrated doses of infused
glucagon
to achieve glycemic stability.
Objective:
To assess the potential clinical utility of dose-titrated
glucagon
infusions in stabilizing glycemic status in pediatric patients with CHI, who were managed by medical and/or surgical approaches.
Methods:
Patients with CHI (
N
= 33), with or without mutations in the ATP-sensitive K
+
channel genes,
ABCC8
, and
KCNJ11
requiring
glucagon
by dose titration in addition to intravenous dextrose and medical therapy with diazoxide/octreotide to achieve glycemic stability were recruited. Following
glucagon
titration and a 24-h glucose stable period, glucose infusion rate (GIR) was reduced over a 24-h period. Achievement of glycemic stability and decrease in GIR were considered end points of the study.
Results:
All patients achieved glycemic stability with
glucagon
infusion, demonstrating clinical benefit. GIR reduced from 15.6 (4.5) to 13.4 (4.6) mg/kg/min mean (SD) (
p
= 0.00019 for difference;
n
= 32; paired
t
-test) over 24 h. By univariate analysis, no individual baseline characteristic was associated with changes in the GIR. However, by baseline-adjusted modeling, mutational status of the patient (
p
= 0.011) was inversely associated with a reduction in GIR. Adverse events were infrequent with diarrhea possibly attributed to
glucagon
treatment in 1 patient. With long-term treatment following GIR reduction, necrolytic migratory
erythema
was observed in another patient.
Conclusion:
These data suggest that dose-titrated
glucagon
infusion therapy aids hypoglycemia prevention and reduction in GIR in the clinical management of patients with CHI.
...
PMID:Efficacy of Dose-Titrated Glucagon Infusions in the Management of Congenital Hyperinsulinism: A Case Series. 3301 78
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