Primary systemic carnitine dehciency. II. Renal handling of carnitine

Engel, Andrew G.; Rebouche, Charles J.; Wilson, David M.; Glasgow, Allen M.; Romshe, Carolyn A.; Cruse, Robert P.

doi:10.1212/wnl.31.7.819

Cited by 145 publications

(54 citation statements)

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“…Because the normal mean fractional excretion of free carnitine is only 1-2%, the method tends to overestimate the threshold. This may partly account for fact that the value of 56 pmol/L found in the control child was considerably higher than the value of 35-40 pmol/L found in normal subjects by Engel et al (12) using carnitine loading. Moreover, as noted above, the effects of prior carnitine treatment had not disappeared completely in this child by the end of the study period.…”

Section: Resultscontrasting

confidence: 57%

“…The MCAD, IVA, and PA patients had estimated renal thresholds for free carnitine between 10 and 25 pmol/L, well below either that of the control child or the range found by the carnitine infusion method. In both of the LCAD patients, the estimated renal thresholds for free carnitine were lower than that of the control child but not below those reported by Engel et al (12). There was no evidence of other renal tubular dysfunction such as glucosuria or phosphate or bicarbonate wasting in any of the patients, and in vitro studies have shown that the carnitine transport system is normal in MCAD and LCAD (9).…”

Section: Resultscontrasting

confidence: 46%

“…Clearance rates were plotted against plasma concentrations and the intercept with a clearance rate of 5% estimated by linear interpolation. The normal renal threshold for free carnitine, based on a more precise method using short-term carnitine infusions, is similar to normal plasma concentrations of free carnitine (12). Table 1 shows the concentrations of plasma carnitine and rates of urinary carnitine excretion in 12 patients with five genetic defects in acyl-CoA oxidation obtained while they were not receiving carnitine treatment and compares them with values found in control children.…”

Section: Methodsmentioning

confidence: 69%

“…A second possible mechanism is that renal conservation of free carnitine is impaired, leading to carnitine deficiency in a manner similar to that seen in patients with a genetic defect in carnitine transport (9,10) or the renal Fanconi syndrome (I I). This mechanism is supported by observations that acylcarnitines inhibit the transport of free carnitine in cultured cells (10) and that the renal threshold for free carnitine is decreased in patients with MCAD (2,12,13). Previous studies of the initial stages in the development of carnitine deficiency in patients given pivalate and in patients with a genetic defect in carnitine transport have provided the clearest method of distinguishing between these two different mechanisms (6,9).…”

mentioning

confidence: 74%

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Renal Handling of Carnitine in Secondary Carnitine Deficiency Disorders

et al. 1993

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. Connecfic~rt 061 15 [W.R.T.] ABSTRACI'. Reduced plasma and tissue concentrations of carnitine, a cofactor required for fatty acid osidation, are present in patients with inherited disorders of mitochondrial acyl-CoA oxidation that are associated with accumulations of acylcarnitines. To determine whether the secondary carnitine deficiency in these patients is due to excessive urinary loss of acylcarnitines, the development of carnitine deficiency was examined in patients with four different acyl-CoA oxidation disorders, including medium-chain and long-chain fatty acyl-CoA dehydrogenase deficiencies, isovaleric acidemia, and propionic acidemia. After a 3-mo period of treatment with oral carnitine to raise plasma total carnitine concentrations to or above normal, patients were started on a carnitine-free diet and the changes in plasma total and free carnitine levels and urinary total and free carnitine escretion were followed for 5 d. Patients with all four disorders showed a return of plasma carnitine levels and urinary carnitine escretion to baseline within 2 to 4 d. The rapidity of these changes could not be explained solely by escessive acylcarnitine wasting. Continued escretion of free carnitine in all patients indicated the additional presence of an impairment in renal transport of free carnitine. Consistent with this interpretation, estimates of renal thresholds for free carnitine gave values that were less than that for a control child in all four disorders and ranged as low as one half those reported in normal individuals. These results suggest that secondary carnitine deficiency in the acyl-CoA oxidation disorders is due to indirect as well as direct effects of accumulated acylcarnitines. Lowered renal free carnitine thresholds in these patients may reflect inhibition of free carnitine transport in the kidney by acylcarnitines. (Pediatr Res 34: 89-97, 1993) Abbreviations IVA, isovaleric acidemia LCAD, long-chain acyl-CoA dehydrogenase deficiency MCAD, medium-chain acyl-CoA dehydrogenase deficiency MMA, methylmalonic aciduria ' PA, propionic acidemia

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Section: Resultscontrasting

confidence: 57%

Section: Resultscontrasting

confidence: 46%

Section: Methodsmentioning

confidence: 69%

mentioning

confidence: 74%

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Renal Handling of Carnitine in Secondary Carnitine Deficiency Disorders

et al. 1993

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“…However, during the first month of hemodialysis therapy, plasma L-carnitine concentrations declined by approximately 30%, and after 12 months they had decreased by approximately 40%, with a pattern suggesting an ongoing decline (12 L-carnitine is not bound to plasma proteins and therefore is freely filtered at the Glomerulus (13). However, at plasma concentrations greater than approximately 60 mmol/L, fractional reabsorption begins to decrease because of partial saturation of the tubular transporter (14).…”

Section: Discussionmentioning

confidence: 99%