BIOMAT Database Logo BIOMAT Database Logo

The C-peptide response to glucagon injections in IDDM and NIDDM patients. 1985

S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson

UI MeSH Term Description Entries
D002096 C-Peptide The middle segment of proinsulin that is between the N-terminal B-chain and the C-terminal A-chain. It is a pancreatic peptide of about 31 residues, depending on the species. Upon proteolytic cleavage of proinsulin, equimolar INSULIN and C-peptide are released. C-peptide immunoassay has been used to assess pancreatic beta cell function in diabetic patients with circulating insulin antibodies or exogenous insulin. Half-life of C-peptide is 30 min, almost 8 times that of insulin. Proinsulin C-Peptide,C-Peptide, Proinsulin,Connecting Peptide,C Peptide,C Peptide, Proinsulin,Proinsulin C Peptide
D003922 Diabetes Mellitus, Type 1 A subtype of DIABETES MELLITUS that is characterized by INSULIN deficiency. It is manifested by the sudden onset of severe HYPERGLYCEMIA, rapid progression to DIABETIC KETOACIDOSIS, and DEATH unless treated with insulin. The disease may occur at any age, but is most common in childhood or adolescence. Diabetes Mellitus, Brittle,Diabetes Mellitus, Insulin-Dependent,Diabetes Mellitus, Juvenile-Onset,Diabetes Mellitus, Ketosis-Prone,Diabetes Mellitus, Sudden-Onset,Diabetes, Autoimmune,IDDM,Autoimmune Diabetes,Diabetes Mellitus, Insulin-Dependent, 1,Diabetes Mellitus, Type I,Insulin-Dependent Diabetes Mellitus 1,Juvenile-Onset Diabetes,Type 1 Diabetes,Type 1 Diabetes Mellitus,Brittle Diabetes Mellitus,Diabetes Mellitus, Insulin Dependent,Diabetes Mellitus, Juvenile Onset,Diabetes Mellitus, Ketosis Prone,Diabetes Mellitus, Sudden Onset,Diabetes, Juvenile-Onset,Diabetes, Type 1,Insulin Dependent Diabetes Mellitus 1,Insulin-Dependent Diabetes Mellitus,Juvenile Onset Diabetes,Juvenile-Onset Diabetes Mellitus,Ketosis-Prone Diabetes Mellitus,Sudden-Onset Diabetes Mellitus
D003924 Diabetes Mellitus, Type 2 A subclass of DIABETES MELLITUS that is not INSULIN-responsive or dependent (NIDDM). It is characterized initially by INSULIN RESISTANCE and HYPERINSULINEMIA; and eventually by GLUCOSE INTOLERANCE; HYPERGLYCEMIA; and overt diabetes. Type II diabetes mellitus is no longer considered a disease exclusively found in adults. Patients seldom develop KETOSIS but often exhibit OBESITY. Diabetes Mellitus, Adult-Onset,Diabetes Mellitus, Ketosis-Resistant,Diabetes Mellitus, Maturity-Onset,Diabetes Mellitus, Non-Insulin-Dependent,Diabetes Mellitus, Slow-Onset,Diabetes Mellitus, Stable,MODY,Maturity-Onset Diabetes Mellitus,NIDDM,Diabetes Mellitus, Non Insulin Dependent,Diabetes Mellitus, Noninsulin Dependent,Diabetes Mellitus, Noninsulin-Dependent,Diabetes Mellitus, Type II,Maturity-Onset Diabetes,Noninsulin-Dependent Diabetes Mellitus,Type 2 Diabetes,Type 2 Diabetes Mellitus,Adult-Onset Diabetes Mellitus,Diabetes Mellitus, Adult Onset,Diabetes Mellitus, Ketosis Resistant,Diabetes Mellitus, Maturity Onset,Diabetes Mellitus, Slow Onset,Diabetes, Maturity-Onset,Diabetes, Type 2,Ketosis-Resistant Diabetes Mellitus,Maturity Onset Diabetes,Maturity Onset Diabetes Mellitus,Non-Insulin-Dependent Diabetes Mellitus,Noninsulin Dependent Diabetes Mellitus,Slow-Onset Diabetes Mellitus,Stable Diabetes Mellitus
D005215 Fasting Abstaining from FOOD. Hunger Strike,Hunger Strikes,Strike, Hunger,Strikes, Hunger
D005934 Glucagon A 29-amino acid pancreatic peptide derived from proglucagon which is also the precursor of intestinal GLUCAGON-LIKE PEPTIDES. Glucagon is secreted by PANCREATIC ALPHA CELLS and plays an important role in regulation of BLOOD GLUCOSE concentration, ketone metabolism, and several other biochemical and physiological processes. (From Gilman et al., Goodman and Gilman's The Pharmacological Basis of Therapeutics, 9th ed, p1511) Glucagon (1-29),Glukagon,HG-Factor,Hyperglycemic-Glycogenolytic Factor,Proglucagon (33-61),HG Factor,Hyperglycemic Glycogenolytic Factor
D006801 Humans Members of the species Homo sapiens. Homo sapiens,Man (Taxonomy),Human,Man, Modern,Modern Man

Related Publications

S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
C-peptide response to glucagon in young diabetics.
June 1989, Taiwan yi xue hui za zhi. Journal of the Formosan Medical Association,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
Comparative renal pathophysiology relevant to IDDM and NIDDM patients.
August 1988, Diabetes/metabolism reviews,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
C-peptide response to glucagon in patients with non-insulin-dependent diabetes mellitus.
May 1992, Journal of the Formosan Medical Association = Taiwan yi zhi,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
Lipoprotein(a) and retinopathy in IDDM and NIDDM patients.
January 1997, Diabetes care,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
Ultrasonographic abnormalities of the pancreas in IDDM and NIDDM patients.
September 1993, Diabetes care,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
C-peptide response to glucagon in diabetics with and without complications.
April 1979, The New Zealand medical journal,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
[Human glucagon-like peptide-1 receptor gene in NIDDM].
October 1994, Nihon rinsho. Japanese journal of clinical medicine,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
C-peptide improves autonomic nerve function in IDDM patients.
June 1996, Diabetologia,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
Is antihypertensive treatment the same for NIDDM and IDDM patients?
April 1998, Diabetes research and clinical practice,
S Poulsen, and P Billesbølle, and K Kølendorf, and B Thorsteinsson
The clinical relevance of fetal hemoglobin in IDDM and NIDDM patients.
June 1995, Diabetes care,
Copied contents to your clipboard!