Cyclosporine, Whole Blood, Immunoassay

CPT: 80158
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Synonyms

  • Cyclosporine A, Whole Blood
  • Gengraf®
  • Neoral®
  • Restasis®
  • Sandimmune®

Expected Turnaround Time

1 - 5 days


Specimen Requirements


Specimen

Whole blood


Volume

2 mL


Minimum Volume

0.6 mL


Container

Lavender-top (EDTA) tube


Storage Instructions

Refrigerate.


Stability Requirements

Temperature

Period

Refrigerated

7 days

Frozen

1 month


Test Details


Use

Cyclosporine is an immunosuppressive agent derived from Tolypocladium inflatum gams, a fungus originally isolated from a Norwegian soil sample. The agent is used extensively to control rejection of organ transplants, especially of liver, heart, or kidney. The effectiveness of cyclosporine results from specific and reversible inhibition of immunocomponent lymphocytes in the G0 and G1 phase of the cell cycle. T-lymphocytes are preferentially inhibited. The T-helper cell is the main target, although the T-suppressor cell may also be suppressed. Cyclosporine also inhibits lymphokine production and release including interleukin-2. Monitoring of blood levels is imperative because the pharmacokinetics of cyclosporine are not only complex, but vary over time in the same patient; thus, blood levels cannot be well predicted from dosing schedules. Furthermore, this drug has a narrow therapeutic window, and significant toxicity at levels above that range. Renal toxicity with eventual renal failure is the most severe complication. Other assays used to assess renal function (ie, BUN, creatinine clearance) should be ordered along with cyclosporine level, since toxicity may begin even with "acceptable" blood levels. Other toxicity includes hypertension, convulsions, tremors, pulmonary edema, and an increased risk of lymphoma. Drugs that enhance the potential toxicity of cyclosporine, include aminoglycoside antibiotics, amphotericin B, acyclovir, ketoconazole, lovastatin, NSAIDS, and ranitidine.


Methodology

Microgenics CEDIA immunoassay


Additional Information

Agents that are CYP3A3 and 3A4 inhibitors raise cyclosporine levels by decreasing biotransformation and include methylprednisolone, amphotericin B, cimetidine, amiodarone, fluoxetine, protease inhibitors, erythromycin, and grapefruit juice. Agents that increase hepatic metabolism (and thus lower cyclosporine levels) include phenobarbital, phenytoin, carbamazepine, rifampin, trimethoprim, and St John's Wort. Because results will vary depending on the method and cyclosporine antibody employed (monospecific or polyspecific), it is best for a given patient's specimens to be analyzed at a single laboratory to eliminate as many assay-dependent variables as possible.


References

American Medical Association, Division of Drugs and Toxicology. Drug Evaluations Subscription. Chicago, Ill: AMA; Winter, 1993.
Drug Information Handbook. 24th ed. Hudson, OH: Wolters Kluwer Clinical Drug Information, Inc; 2015; 522-529.
Hamwi A, Salomon A, Steinbrugger R, et al. Cyclosporine metabolism in patients after kidney, bone marrow, heart-lung, and liver transplantation in the early and late post-transplant periods. Am J Clin Pathol. 2000 Oct; 114(4):536-543. 11026099
Oellerich M, Armstrong VW, Kahan B, et al. Lake Louise Consensus Conference on cyclosporine monitoring in organ transplantation: Report of the consensus panel. Ther Drug Monit. 1995; 17(6):642-654. 8588235
Physicians' Desk Reference. 66th ed. Montvale, NJ: Thompson PDR; 2012.

LOINC® Map

Order Code Order Code Name Order Loinc Result Code Result Code Name UofM Result LOINC
706557 Cyclosporine, Blood 14978-1 706562 Cyclosporine by Immunoassay ng/mL 14978-1

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