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Abstract

Objective

Isoprene is the constitutive unit of isoprenoid lipids and sterols. However, it is also a potential toxic and carcinogenic agent. Recent findings of a marked and prolonged isoprene overproduction induced by hemodialysis sessions raises the question of isoprene behavior in patients on peritoneal dialysis.

Design

A study with repeated measures per patient and healthy control.

Setting

Nephrology and Dialysis Unit and Perugia University Medical School.

Patients

Sixteen consecutive patients on regular continuous ambulatory peritoneal dialysis (CAPD) were evaluated. Endogenous isoprene was analyzed using gas chromatographic assay of breath isoprene, collected at set times before and after dialysis fluid exchange.

Results

No significant variations were found in breath isoprene concentrations in the different samples from each patient, and levels were almost stable within the normal range of healthy controls.

Conclusion

These results show that CAPD, unlike hemodialysis, has little or no effect on isoprene and isoprenoid-related lipid turnover. This lack of increased endogenous isoprene synthesis, in addition to being a distinctive metabolic feature of CAPD, could have important pathophysiological and clinical implications.

Keywords

Human breath isoprene

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References

Zoccali

Cardiovascular risk in uraemic patients—is it fully explained by classical risk factors?

Nephrol Dial Transplant 2000; 15: 454–7.

Baigent

, Burbury

, Wheeler

Premature cardiovascular disease in chronic renal failure.

Lancet 2000; 356: 147–52.

Herzog

C.A.

Acute myocardial infarction in patients with end-stage renal disease.

Kidney Int Suppl 1999; 71: S130–3.

Marple

J.T.

, MacDougall

Development of malignancy in the end-stage renal disease patient.

Semin Nephrol 1993; 13: 306–14.

Ishikawa

Renal cell carcinomas in patients on long-term hemodialysis.

Contrib Nephrol 1999; 128: 28–44.

Vamvakas

, Bahner

, Heidland

Increased cancer incidence in terminal kidney failure: Potential pathogenetic mechanisms.

Schweiz Med Wochenschr 1997; 127: 597–604.

Murphy

S.W.

, Foley

R.N.

, Barrett

B.J.

, Kent

G.M.

, Morgan

, Barre

Comparative mortality of hemodialysis and peritoneal dialysis in Canada.

Kidney Int 2000; 57: 1720–6.

Berkoben

M.D.

Patient mortality in chronic dialysis: Comparisons between hemodialysis and peritoneal dialysis.

Curr Opin Nephrol Hypertens 1999; 8: 681–3.

Miyata

, Ueda

, Saito

, Kurokawa

‘Carbonyl stress’ and dialysis-related amyloidosis.

Nephrol Dial Transplant 2000; 15(Suppl 1): 25–8.

10.

Drueke

T.B.

Beta2-microglobulin and amyloidosis.

Nephrol Dial Transplant 2000; 15(Suppl 1): 17–24.

11.

Zima

, Mestek

, Nemecek

, Bartova

, Fialova

, Tesar

Trace elements in hemodialysis and continuous ambulatory peritoneal dialysis patients.

Blood Purif 1998; 1: 253–60.

12.

Capodicasa

, Trovarelli

, De Medio

G.E.

, Pelli

M.A.

, Lippi

, Verdura

Volatile alkanes and increased concentrations of isoprene in exhaled air during hemodialysis.

Nephron 1999; 82: 331–7.

13.

Trovarelli

, Brunori

, De Medio

G.E.

, Timio

, Lippi

, Pelli

M.A.

Onset, time course, and persistence of increased haemodialysis-induced breath isoprene emission.

Nephron 2001; 88: 44–7.

14.

Vishnuvardhan

, Beinfeld

M.C.

Lovastatin is a potent inhibitor of cholecystokinin secretion in endocrine tumor cells in culture.

Peptides 2000; 21: 553–7.

15.

Csanady

G.A.

, Filser

J.G.

Toxicokinetics of inhaled and endogenous isoprene in mice, rats, and humans.

Chem Biol Interact 2001; 135–136: 679–85.

16.

Bolt

H.M.

Butadiene and isoprene: Future studies and implications.

Toxicology 1996; 113: 356–60.

17.

Melnick

R.L.

, Kohn

M.C.

Dose-response analyses of experimental cancer data.

Drug Metab Rev 2000; 2: 193–209.

18.

Melnick

R.L.

, Sills

R.C.

, Roycroft

J.H.

, Chou

B.J.

, Ragan

H.A.

, Miller

R.A.

Isoprene, an endogenous hydrocarbon and industrial chemical, induces multiple organ neoplasia in rodents after 26 weeks of inhalation exposure.

Cancer Res 1994; 54: 5333–9.

19.

Brown

M.S.

, Goldstein

J.L.

Multivalent feedback regulation of HMG CoA reductase, a control mechanism coordinating isoprenoid synthesis and cell growth.

J Lipid Res 1980; 21: 505–17.

20.

Correll

C.C.

, Edwards

P.A.

Mevalonic acid-dependent degradation of 3-hydroxy-3-methylglutaryl-coenzyme A reductase in vivo and in vitro.

J Biol Chem 1994; 269: 633–8.

21.

Houten

S.M.

, Romeijn

G.J.

, Koster

, Gray

R.G.

, Darbyshire

, Smit

G.P.

Identification and characterization of three novel missense mutations in mevalonate kinase cDNA causing mevalonic aciduria, a disorder of isoprene biosynthesis.

Hum Mol Genet 1999; 8: 1523–8.

22.

Hinson

D.D.

, Chambliss

K.L.

, Toth

M.J.

, Tanaka

R.D.

, Gibson

K.M.

Post-translational regulation of mevalonate kinase by intermediates of the cholesterol and nonsterol isoprene biosynthetic pathways.

J Lipid Res 1997; 38: 2216–23.

23.

Scoppola

, De Paolis

, Menzinger

, Lala

, Di Giulio

Plasma mevalonate concentrations in uremic patients.

Kidney Int 1997; 51: 908–12.

24.

Mendis

, Sobotka

P.A.

, Euler

D.E.

Expired hydrocarbons in patients with acute myocardial infarction.

Free Radic Res 1995; 23: 117–22.

Lack of Isoprene Overproduction during Peritoneal Dialysis