Glucose and insulin changes following a renoportal shunt in streptozotocin diabetic rats with pancreatic islet isografts under the kidney capsule

H, Reece-Smith; McShane, Paul; Morris, Peter J.

doi:10.1007/bf00253742

Cited by 18 publications

(7 citation statements)

References 20 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…However, this does not apply to other rat strains (21) or other species (22). Metabolic advantages have been claimed for grafts with portal venous compared with systemic venous drainage (23,24). However, in a study comparing the efficacy of kidney subcapsular and intraportal islets in normalizing the glucose metabolism, there was no superiority for either site, which is in agreement with our results (25).…”

Section: Discussionsupporting

confidence: 91%

Progressive Deterioration of Endocrine Function After Intraportal but Not Kidney Subcapsular Rat Islet Transplantation

Hiller

Klempnauer²,

Lück³

et al. 1991

Diabetes

View full text Add to dashboard Cite

In inbred streptozocin-induced diabetic rats, the long-term function of different endocrine pancreatic isografts was compared. Isolated islets transplanted into the portal vein showed a progressive deterioration of function over time. In contrast, islets under the kidney capsule sustained a constant long-term function controlling all clinical signs of diabetes. Recipients of kidney subcapsular islets displayed normal growth rate, peripheral serum glucose and insulin levels, and metabolic parameters. However, their functional reserve was markedly reduced as revealed by diminished glucose tolerance and reduced insulin-secreting capacity after an intravenous glucose challenge. Vascularized whole-organ pancreatic grafts with portal venous drainage led to complete normalization of all parameters determined in this study. This study showed that the long-term function of islets transplanted under the kidney capsule is superior compared with islets transplanted into the portal vein.

show abstract

Section: Discussionsupporting

confidence: 91%

Progressive Deterioration of Endocrine Function After Intraportal but Not Kidney Subcapsular Rat Islet Transplantation

Hiller

Klempnauer²,

Lück³

et al. 1991

Diabetes

View full text Add to dashboard Cite

show abstract

“…Critical data in this study are the insulin extractions from the pancreases of all the animals and from the grafts. Previous studies addressing the question of portal insulin drainage (Kemp et al, 1973;Feldman et al, 1977;Brown et al, 1979;Reece-Smith et al, 1982) did not determine the final total insulin content in the animal. Without knowing how much islet tissue remains, it is impossible to assess accurately the efficacy of the graft in handling a metabolic challenge.…”

Section: Discussionmentioning

confidence: 98%

“…However, these grafts drained insulin into the systemic venous circulation and therefore the physiological first-pass of the hormone through the liver was absent (Madison et al, 1958;Blackard and Nelson, 1971;Felig, 1975). Some studies from other laboratories have suggested that portal venous drainage is more effective in controlling diabetes than insulin secreted into the systemic circulation (Kemp et al, 1973;Brown et aL, 1979;Reece-Smith, McShane and Morris, 1982). However, recently Kruszynska, Home and Alberti (1985a,b) reported the ability to achieve consistent euglycaemia with systemically draining Abbreviations used in this paper: GHb, glycosylated haemoglobin; IP, intraperitoneal; RBG, random blood glucose; and STZ, streptozotocin.…”

Section: Introductionmentioning

confidence: 99%

A Comparison of Portal Versus Systemic Venous Drainage in Murine Foetal Pancreatic Islet Transplantation

Mandel

1986

Aust J Exp Biol Med

View full text Add to dashboard Cite

Summary.We have compared the efficiency of foetal islet graft growth and function in renal subcapsular (systemic drainage) and splenic (portal drainage) sites. Age-matched female BALB/c streptozotocin (STZ)-diabetic mice were grafted either under the left renal capsule or on to the hilar surface of the spleen with one half of a syngeneic 17-day gestation foetal -pancreas which had been in organ culture for 2 weeks. Gain in body weight, return to jiormoglycaemia and to normal glycosylated haemoglobin levels were not significantly different between the two groups. However, when an intraperitoneal arginine challenge was performed the portally grafted mice showed more normal responses than the systemically grafted mice. Although still not normal after the arginine challenge, mean blood glucose values were lower and serum insulin values higher in the spleen grafted animals than in the renal subcapsular graft group. The total amount of insulin was assayed by extraction of both the graft and the pancreas of each animal. The amount of insulin in the grafts from the spleen was not significantly different from those in the renal subcapsular site. We conclude that the efficiency of a graft draining into the portal circulation is greater than an equivalent sized graft draining systemically when a maxima! challenge is applied.

show abstract

“…Basal glucose and insulin levels in animals with grafts to the spleen were similar to those in controls, but they were significantly higher in animals with grafts to the liver and to the kidney. The increased basal insulin levels seen after transplantation to the kidney can be attributed to the absence of the first-pass insulin extraction by the liver as a consequence of systemic instead of portal venous drainage [6,[19][20][21]. Hyperinsulinaemia, after transplantation to the liver, cannot be attributed to an absent first-pass extraction of insulin, but there is substantial evidence to suggest that this extraction is quantitatively reduced.…”

Section: Discussionmentioning

confidence: 99%

“…As islets differ considerably in size [3,4], seemingly similar graft sizes, when defined by the nmnber of transplanted islets, may well represent a considerable difference in the actual number of Beta cells of the islet grafts. In addition, the differing results between the transplant sites have been attributed to efficacy of engraftment after islet transplantation [5] and to the route of venous drainage of insulin by the endocrine graft, i. e. to the portal or to the systemic circulation [6][7][8]. However, the individual influence either of graft size or of properties related to the graft site on the reported graft function cannot easily be distinguished.…”

mentioning

confidence: 99%

Insulin secretion by rat islet isografts of a defined endocrine volume after transplantation to three different sites

et al. 1992

View full text Add to dashboard Cite

Glucose and insulin changes following a renoportal shunt in streptozotocin diabetic rats with pancreatic islet isografts under the kidney capsule

Cited by 18 publications

References 20 publications

Progressive Deterioration of Endocrine Function After Intraportal but Not Kidney Subcapsular Rat Islet Transplantation

Progressive Deterioration of Endocrine Function After Intraportal but Not Kidney Subcapsular Rat Islet Transplantation

A Comparison of Portal Versus Systemic Venous Drainage in Murine Foetal Pancreatic Islet Transplantation

Insulin secretion by rat islet isografts of a defined endocrine volume after transplantation to three different sites

Contact Info

Product

Resources

About