Chemistry:C-peptide

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C-peptide[1]
C-Peptide.svg
Identifiers
3D model (JSmol)
ChemSpider
MeSH C-Peptide
UNII
Properties
C129H211N35O48
Molar mass 3020.29 g/mol
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
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Infobox references
Tracking categories (test):

The connecting peptide, or C-peptide, is a short 31-amino-acid polypeptide that connects insulin's A-chain to its B-chain in the proinsulin molecule. In the context of diabetes or hypoglycemia, a measurement of C-peptide blood serum levels can be used to distinguish between different conditions with similar clinical features.

In the insulin synthesis pathway, first preproinsulin is translocated into the endoplasmic reticulum of beta cells of the pancreas with an A-chain, a C-peptide, a B-chain, and a signal sequence. The signal sequence is cleaved from the N-terminus of the peptide by a signal peptidase, leaving proinsulin. After proinsulin is packaged into vesicles in the Golgi apparatus (beta-granules), the C-peptide is removed, leaving the A-chain and B-chain bound together by disulfide bonds, that constitute the insulin molecule.

History

Proinsulin C-peptide was first described in 1967 in connection with the discovery of the insulin biosynthesis pathway.[2] Isolation of bovin C-peptide, determination of sequence, preparation of human C-peptide were done in 1971.[3] C-peptide serves as a linker between the A- and the B- chains of insulin and facilitates the efficient assembly, folding, and processing of insulin in the endoplasmic reticulum. Equimolar amounts of C-peptide and insulin are then stored in secretory granules of the pancreatic beta cells and both are eventually released to the portal circulation. Initially, the sole interest in C-peptide was as a marker of insulin secretion and has, as such, been of great value in furthering the understanding of the pathophysiology of type 1 and type 2 diabetes. The first documented use of the C-peptide test was in 1972[citation needed]. During the past decade, however, C-peptide has been found to be a bioactive peptide in its own right, with effects on microvascular blood flow and tissue health.

Function

Cellular effects of C-peptide

C-peptide has been shown to bind to the surface of a number of cell types such as neuronal, endothelial, fibroblast and renal tubular, at nanomolar concentrations to a receptor that is likely G-protein-coupled. The signal activates Ca2+-dependent intracellular signaling pathways such as MAPK, PLCγ, and PKC, leading to upregulation of a range of transcription factors as well as eNOS and Na+K+ATPase activities.[4] The latter two enzymes are known to have reduced activities in patients with type I diabetes and have been implicated in the development of long-term complications of type I diabetes such as peripheral and autonomic neuropathy.

In vivo studies in animal models of type 1 diabetes have established that C-peptide administration results in significant improvements in nerve and kidney function. Thus, in animals with early signs of diabetes-induced neuropathy, C peptide treatment in replacement dosage results in improved peripheral nerve function, as evidenced by increased nerve conduction velocity, increased nerve Na+,K+ ATPase activity, and significant amelioration of nerve structural changes.[5] Likewise, C-peptide administration in animals that had C-peptide deficiency (type 1 model) with nephropathy improves renal function and structure; it decreases urinary albumin excretion and prevents or decreases diabetes-induced glomerular changes secondary to mesangial matrix expansion.[6][7][8][9] C-peptide also has been reported to have anti-inflammatory effects as well as aid repair of smooth muscle cells.[10][11] A recent epidemiologic study suggests a U-shaped relationship between C-peptide levels and risk of cardiovascular disease.[12]

Clinical uses of C-peptide testing

Patients with diabetes may have their C-peptide levels measured as a means of distinguishing type 1 diabetes from type 2 diabetes or maturity-onset diabetes of the young (MODY).[13] Measuring C-peptide can help to determine how much of their own natural insulin a person is producing as C-peptide is secreted in equimolar amounts to insulin. C-peptide levels are measured instead of insulin levels because C-peptide can assess a person's own insulin secretion even if they receive insulin injections, and because the liver metabolizes a large and variable amount of insulin secreted into the portal vein but does not metabolise C-peptide, meaning blood C-peptide may be a better measure of portal insulin secretion than insulin itself.[14][15] A very low C-peptide confirms Type 1 diabetes and insulin dependence and is associated with high glucose variability, hyperglycaemia and increased complications. The test may be less helpful close to diagnosis, particularly where a patient is overweight and insulin resistant, as levels close to diagnosis in Type 1 diabetes may be high and overlap with those seen in type 2 diabetes.[16]

C-peptide can be used for differential diagnosis of hypoglycemia. The test may be used to help determine the cause of hypoglycaemia (low glucose), values will be low if a person has taken an overdose of insulin but not suppressed if hypoglycaemia is due to an insulinoma or sulphonylureas.

Factitious (or factitial) hypoglycemia may occur secondary to the surreptitious use of insulin. Measuring C-peptide levels will help differentiate a healthy patient from a diabetic one.

C-peptide may be used for determining the possibility of gastrinomas associated with Multiple Endocrine Neoplasm syndromes (MEN 1). Since a significant number of gastrinomas are associated with MEN involving other hormone producing organs (pancreas, parathyroids, and pituitary), higher levels of C-peptide together with the presence of a gastrinoma suggest that organs besides the stomach may harbor neoplasms.

C-peptide levels may be checked in women with Polycystic Ovarian Syndrome (PCOS) to help determine degree of insulin resistance.

Ultrasensitive C-peptide assays have made it possible to detect very low levels of circulating C-peptide even in patients with longstanding type-1 diabetes.[17] Studies have demonstrated that the presence of residual C-peptide in longstanding type-1 diabetes is associated with a lower risk for developing microvascular complications and a significant reduction in incidence of severe hypoglycaemia.[18]

Therapeutics

Therapeutic use of C-peptide has been explored in small clinical trials in diabetic kidney disease.[19][20] Creative Peptides,[21] Eli Lilly,[22] and Cebix[23] all had drug development programs for a C-peptide product. Cebix had the only ongoing program until it completed a Phase IIb trial in December 2014 that showed no difference between C-peptide and placebo, and it terminated its program and went out of business.[24][25]

References

  1. C-Peptide - Compound Summary, PubChem.
  2. "Insulin biosynthesis: evidence for a precursor". Science 157 (3789): 697–700. August 1967. doi:10.1126/science.157.3789.697. PMID 4291105. Bibcode1967Sci...157..697S. 
  3. Brandenburg, Dietrich (2008). "History and Diagnostic Significance of C-Peptide". Experimental Diabetes Research 2008: 576862. doi:10.1155/2008/576862. ISSN 1687-5214. PMID 18509495. 
  4. "Intracellular signalling by C-peptide". Experimental Diabetes Research 2008: 635158. 2008. doi:10.1155/2008/635158. PMID 18382618. 
  5. "C-peptide prevents and improves chronic Type I diabetic polyneuropathy in the BB/Wor rat". Diabetologia 44 (7): 889–97. July 2001. doi:10.1007/s001250100570. PMID 11508275. 
  6. "Effects of C-peptide on glomerular and renal size and renal function in diabetic rats". Kidney International 60 (4): 1258–65. October 2001. doi:10.1046/j.1523-1755.2001.00964.x. PMID 11576340. 
  7. "C-peptide prevents glomerular hypertrophy and mesangial matrix expansion in diabetic rats". Nephrology, Dialysis, Transplantation 20 (3): 532–8. March 2005. doi:10.1093/ndt/gfh683. PMID 15665028. 
  8. "Proinsulin C-peptide reduces diabetes-induced glomerular hyperfiltration via efferent arteriole dilation and inhibition of tubular sodium reabsorption". American Journal of Physiology. Renal Physiology 297 (5): F1265-72. November 2009. doi:10.1152/ajprenal.00228.2009. PMID 19741019. 
  9. "C-Peptide: the missing link in diabetic nephropathy?". The Review of Diabetic Studies 6 (3): 203–10. 2009. doi:10.1900/RDS.2009.6.203. PMID 20039009. 
  10. "Human C-peptide antagonises high glucose-induced endothelial dysfunction through the nuclear factor-kappaB pathway". Diabetologia 51 (8): 1534–43. August 2008. doi:10.1007/s00125-008-1032-x. PMID 18493738. 
  11. "Cellular mechanisms by which proinsulin C-peptide prevents insulin-induced neointima formation in human saphenous vein". Diabetologia 53 (8): 1761–71. August 2010. doi:10.1007/s00125-010-1736-6. PMID 20461358. 
  12. "Association of low fasting C-peptide levels with cardiovascular risk, visit-to-visit glucose variation and severe hypoglycemia in the Veterans Affairs Diabetes Trial (VADT)". Cardiovascular Diabetology 20 (1): 232. 2021. doi:10.1186/s12933-021-01418-z. PMID 34879878. 
  13. "The clinical utility of C-peptide measurement in the care of patients with diabetes". Diabetic Medicine 30 (7): 803–17. July 2013. doi:10.1111/dme.12159. PMID 23413806. 
  14. "Assays for insulin, proinsulin(s) and C-peptide". Annals of Clinical Biochemistry 36 ( Pt 5) (5): 541–64. September 1999. doi:10.1177/000456329903600501. PMID 10505204. 
  15. "Peripheral insulin parallels changes in insulin secretion more closely than C-peptide after bolus intravenous glucose administration". The Journal of Clinical Endocrinology and Metabolism 67 (5): 1094–9. November 1988. doi:10.1210/jcem-67-5-1094. PMID 3053748. 
  16. R, Chandini; Udayabhaskaran V; Binoy J Paul; K.P Ramamoorthy (July 2013). "A study of non-obese diabetes mellitus in adults in a tertiary care hospital in Kerala, India". International Journal of Diabetes in Developing Countries 33 (2): 83–85. doi:10.1007/s13410-013-0113-7. 
  17. Keenan, Hillary A.; Sun, Jennifer K.; Levine, Jared; Doria, Alessandro; Aiello, Lloyd P.; Eisenbarth, George; Bonner-Weir, Susan; King, George L. (2010-08-10). "Residual Insulin Production and Pancreatic β-Cell Turnover After 50 Years of Diabetes: Joslin Medalist Study". Diabetes 59 (11): 2846–2853. doi:10.2337/db10-0676. ISSN 0012-1797. PMID 20699420. PMC 2963543. http://dx.doi.org/10.2337/db10-0676. 
  18. Jeyam, Anita; Colhoun, Helen; McGurnaghan, Stuart; Blackbourn, Luke; McDonald, Timothy J.; Palmer, Colin N.A.; McKnight, John A.; Strachan, Mark W.J. et al. (2021-02-05). "Erratum. Clinical Impact of Residual C-Peptide Secretion in Type 1 Diabetes on Glycemia and Microvascular Complications. Diabetes Care 2021;44:390–398". Diabetes Care: dc21er04b. doi:10.2337/dc21er04b. ISSN 0149-5992. PMID 33547206. http://dx.doi.org/10.2337/dc21er04b. 
  19. "C-peptide and diabetic kidney disease". Journal of Internal Medicine 281 (1): 41–51. January 2017. doi:10.1111/joim.12548. PMID 27640884. 
  20. "C-peptide as a Therapy for Kidney Disease: A Systematic Review and Meta-Analysis". PLOS ONE 10 (5): e0127439. 2015. doi:10.1371/journal.pone.0127439. PMID 25993479. Bibcode2015PLoSO..1027439S. 
  21. "C-peptide - Creative Peptides -". AdisInsight. http://adisinsight.springer.com/drugs/800010430. 
  22. "C-peptide - Eli Lilly". AdisInsight. http://adisinsight.springer.com/drugs/800005551. 
  23. "C-peptide long-acting - Cebix". AdisInsight. http://adisinsight.springer.com/drugs/800034107. 
  24. Bigelow, Bruce V. (23 February 2015). "Cebix Shuts Down Following Mid-Stage Trial of C-Peptide Drug". Xconomy. http://www.xconomy.com/san-diego/2015/02/23/cebix-shuts-down-following-mid-stage-trial-of-c-peptide-drug/#. 
  25. Garde, Damian (February 24, 2015). "Cebix hangs it up after raising $50M for diabetes drug". FierceBiotech. http://www.fiercebiotech.com/r-d/cebix-hangs-it-up-after-raising-50m-for-diabetes-drug. 

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