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営業時間、予約なし診療およびご予約。Coproporphyrins I and III; uroporphyrins; heptacarboxylporphyrins; hexacarboxylporphyrins; pentacarboxylporphyrins
The test request form must state 24-hour collection volume.
3 - 7 days
Turnaround time is defined as the usual number of days from the date of pickup of a specimen for testing to when the result is released to the ordering provider. In some cases, additional time should be allowed for additional confirmatory or additional reflex tests. Testing schedules may vary.
Urine (24-hour), protected from light
2-mL aliquot
1.5-mL aliquot (Note: This volume does not allow for repeat testing.)
12-mL plastic transport tube without preservative.
Instruct patient to void at 8 AM (or 8 PM) and discard the specimen. Then collect all the urine, including the final specimen voided at the end of the 24-hour collection period (ie, 8 AM [or 8 PM] the following day). Mix well. Measure and record total urine volume on the test request form, along with the patient's name, date, and time collection started and finished. Transfer required aliquot into a LabCorp amber plastic transport tube with amber cap (LabCorp N° 23598). (If amber transport tubes are unavailable, cover transport tube completely, top and bottom, with aluminum foil. Identify specimen with patient's name directly on the amber transport tube and on the outside of the aluminum foil. Secure with tape.) Specimen must be kept refrigerated during transport.
Refrigerate and protect from light.
Temperature | Period |
---|---|
Room temperature | Unstable |
Refrigerated | 7 days |
Frozen | 14 days |
Freeze/thaw cycles | Stable x3 |
Stored specimen not refrigerated; specimen exposed to light; acid preservative; pH <3
Evaluate porphyrias, including those involving deficiencies of enzymes that are needed for heme synthesis and chemical porphyrias.
In congenital erythropoietic porphyria, elevations of urinary uroporphyrin and coproporphyrin occur, with the former exceeding the latter.
In acute intermittent porphyria, porphobilinogen and δ-aminolevulinic acid are elevated in acute attacks, and mild increases of urinary uroporphyrin and coproporphyrin may be found. Porphobilinogen is increased in many but not all patients with acute intermittent porphyria in latent periods. Quantitative porphobilinogen is a better test than δ-aminolevulinic acid overall for acute intermittent porphyria, but both are used (as well as the Watson-Schwartz test).1
Coproporphyrin and porphobilinogen excretion in urine are markedly increased during acute attacks of hereditary coproporphyria, increase of urinary uroporphyrin may be found, and increased fecal coproporphyrin III is described.
In variegate porphyria in acute attacks, results are similar to those of acute intermittent porphyria. Porphobilinogen and ALA are prone to become normal between attacks. Urine coproporphyrin exceeds uroporphyrin excretion during acute attacks.
Chemical porphyrias occur. Porphyrinogenic chemicals include certain halogenated hydrocarbons that cause the excretion of increased uroporphyrin.
In lead poisoning elevation of δ-aminolevulinic acid greater than that of porphobilinogen occurs and porphobilinogen may be normal. Urinary coproporphyrin characteristically is increased. Free erythrocyte protoporphyrin is increased. Toxins such as lead interfere with heme synthesis and cause porphyrinuria.
Increased urine excretion of uroporphyrinogen, uroporphyrin, and coproporphyrin occurs in porphyria cutanea tarda. It is found in (1) middle-aged men who like ethanol, (2) young women on oral contraceptives, and in (3) subjects on dialysis. These patients do not excrete increased porphobilinogen, but they may have slight elevations of δ-aminolevulinic acid.
Cutaneous Porphyria | Clinical Notes | Neurologic Porphyria | Clinical Notes |
---|---|---|---|
*Note: Low urine values are meaningless. Only greatly increased values (10-15 times the upper limit of the reference interval) have clinical significance for porphyrias. | |||
†Timing of urine collection for the investigation of cutaneous porphyria is not as critical as in neurologic porphyrias in which PBG screening test should be collected when the patient is symptomatic. | |||
Congenital erythropoietic porphyria (CEP) | Very rare; generally diagnosed in childhood | Acute intermittent porphyria (AIP) | 80% of neurologic porphyrias |
Protoporphyria (PP) | Seen in adolescents | Variegate porphyria (VP) | |
Porphyria cutanea tarda (PCT) | 90% (most common) of cutaneous porphyrias; seen in middle age | Coproporphyria (CP) |
The accompanying flow diagrams outline steps for the investigation of cutaneous and neurologic porphyrias.
Increased porphobilinogen may occur in patients on oral contraceptives. This test and δ-aminolevulinic acid will not detect protoporphyria. Coproporphyrinuria alone lacks specificity and sensitivity for lead testing. Erythrocyte uroporphyrinogen-1-synthase is decreased in latent acute intermittent porphyria, and is needed in patients with possible latent acute intermittent porphyria. Quantitative porphobilinogen is of value in active and in many cases of latent acute intermittent porphyria, but will miss some of the latter when compared to red cell uroporphyrinogen-1-synthase.
High-pressure liquid chromatography (HPLC) with fluorometric detection
• Coproporphyrin (CP) I: 0−24 μg/24 hours
• Coproporphyrin (CP) III: 0−74 μg/24 hours
• Heptacarboxylporphyrins (7-CP): 0−4 μg/24 hours
• Hexacarboxylporphyrins (6-CP): 0−1 μg/24 hours
• Pentacarboxylporphyrins (5-CP): 0−4 μg/24 hours
• Uroporphyrins (UP): 0−24 μg/24 hours
See table.
Disease | Uro | Hepta | Hexa | Penta | Copro I | Copro III |
---|---|---|---|---|---|---|
+ = increased; ++ = strongly increased; n = normal; v = varies. | ||||||
Values from: Doss M. Porphyrinstoffwechsel. In: Greiling H, Gressner AM (Hrsg). Lehrbuch der Klinischen Chemie und Pathobiochemie. Dritte Auflage. Stuttgart, Germany: Schattauer Verlag. | ||||||
Values marked with * and ** respectively, are derived from: | ||||||
*Hindmarsh JT, Oliveras L, Greenway DC. Biochemical differentiation of the porphyrias. Clin Biochem. 1999 Nov; 32(8):609-619. | ||||||
**Elder GH, Smith SG, Smyth SJ. Laboratory investigation of the porphyrias. Ann Clin Biochem. 1990 Sep; 27(Pt 5):395-412. | ||||||
Porphyria cutanea tarda (PCT) | ++ | ++ | + | + | +* | +* |
Acute intermittent porphyria (AIP) | ++ | + | + | ++ | +* | ++* |
Porphyria variegata (VP) | ++ | + | + | ++ | +* | ++* |
Hereditary coproporphyria (CP) | + | + | + | ++ | n* | ++* |
Protoporphyria | v | n | n | v | +* | v |
Morbus Gunther | ++ | + | + | + | ++** | |
Porphobilinogen synthase deficiency | + | + | + | ++ | ++ |
Increased urine porphyrin excretion may be secondary to other diseases (eg, hepatobiliary diseases), especially coproporphyrin excretion. These are secondary porphyrinurias. They lack increased urinary porphobilinogen or Δ-ALA, with the important exception of lead poisoning.2 The table provides an abbreviated overview of the porphyrias. Porphyrin fractionation of plasma can be done. Increases of urine porphyrins are found with congenital erythropoietic porphyria, acute intermittent porphyria, hereditary coproporphyria, variegate porphyria, and porphyria cutanea tarda.
Disorder | Inheritance | Age of Clinical Onset | Primary Organ Involvement | Useful Tests | Primary Symptoms |
---|---|---|---|---|---|
Congenital erythropoietic porphyria | Autosomal recessive | Birth−5 y | Erythroid cells | Urinary porphyrins; Fecal porphyrins; Uroporphyrinogen III synthase, erythrocytes | Severe photosensitivity |
(Günther disease) | Rare | Fluorescence of a diaper under Wood light | Red urine; diaper stains; hemolytic anemia | ||
Acute intermittent porphyria | Autosomal dominant | Adults | Hepatic, probably erythroid cells | Urine porphobilinogen; Porphobilinogen deaminase, erythrocyte; Urine porphyrins; Urinary δ-aminolevulinic acid; Erythrocyte uroporphyrinogen-1-synthase; Fecal porphyrins | Mild/severe neurologic/visceral (autonomic) symptoms |
Precipitating causes include barbiturates, hydantoins, sulfonamides | Most common acute hepatic porphyria in US | Acute attacks | |||
Hereditary coproporphyria | Autosomal dominant | Adults | Hepatic, possibly erythroid cells | Urine PBG and ALA in acute attacks; Urine porphyrins including coproporphyrin; Fecal porphyrins; Plasma porphyrins | Similar to variegate porphyria; acute attacks |
Variegate porphyria | Autosomal dominant | Adults | Hepatic, possibly erythroid cells | Urine PBG and ALA in acute attacks; Urine porphyrins; Fecal porphyrins; Plasma porphyrins; Erythrocyte uroporphyrinogen-1-synthase | Mild/severe photosensitivity, neurologic/visceral symptoms; acute attacks |
Porphyria cutanea tarda | Autosomal dominant, type II (inherited type); sporadic type also known; most common porphyria in US | Adults | Hepatic, possibly erythroid cells; photosensitivity | Urine porphyrins; Plasma porphyrins; Uroporphyrinogen decarboxylase, type II (RBCs) | Similar to variegate porphyria; photosensitization; liver damage |
Protoporphyria | Autosomal dominant | Usually childhood | Erythroid cells, probably liver | Protoporphyrin, free erythrocyte | Photosensitization; liver damage |
Acquired (intoxication) porphyria | Acquired | Children and adults | Hepatic, erythroid cells | Erythrocyte porphyrins; Urinary δ-aminolevulinic acid; Urine porphobilinogen; Urine porphyrins; Fecal porphyrins | Mild photosensitivity |
Fecal porphyrin examination for hereditary coproporphyria, variegate porphyria, and protoporphyria can be used for adult patients. Stool examination for coproporphyrin and protoporphyrin is recommended for diagnosis of variegate porphyria.3
Neurologic dysfunction occurs in the hepatic porphyrias, the types of porphyria in which acute attacks develop: acute intermittent porphyria, variegate porphyria, hereditary coproporphyria, and ALA dehydrase deficiency. Abdominal pain, caused by autonomic neuropathy, occurs with acute attacks (eg, acute intermittent porphyria). It is the most common symptom of acute intermittent porphyria.2
Cutaneous aspects of the porphyrias are caused by photosensitization (eg, porphyria cutanea tarda, protoporphyria).
Hepatic complications are found with porphyria cutanea tarda and protoporphyria. Fluorescence is demonstrable in liver biopsies from patients with the former, as well as siderosis. Crystalline deposits may be found in protoporphyria.2 The amount of porphobilinogen excreted in acute intermittent porphyria is usually greater than the excretion of δ-aminolevulinic acid (Δ-ALA). When there is more Δ-ALA, another diagnosis should be considered, including lead poisoning, another type of porphyria, or hereditary tyrosinemia.2
Order Code | Order Code Name | Order Loinc | Result Code | Result Code Name | UofM | Result LOINC |
---|---|---|---|---|---|---|
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121042 | Uroporphyrins (UP) | ug/L | 11228-4 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121043 | Uroporph(UP),24hr | ug/24 hr | 3113-8 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121044 | Heptacarboxyl (7-CP) | ug/L | 2407-5 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121045 | Heptacarb(7-CP),24hr | ug/24 hr | 24462-4 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121046 | Hexacarboxyl (6-CP) | ug/L | 27400-1 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121047 | Hexacarb(6-CP),24hr | ug/24 hr | 9527-3 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121048 | Pentacarboxyl (5-CP) | ug/L | 11221-9 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121049 | Pentacarb(5-CP),24hr | ug/24 hr | 9730-3 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121050 | Coproporphyrin (CP) I | ug/L | 47253-0 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121051 | Coproporph(CP)I,24hr | ug/24 hr | 6877-5 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121052 | Coproporphyrin (CP) III | ug/L | 47254-8 |
003194 | Porphyrins, Qn, 24 Hr Ur. | 43116-3 | 121053 | Copropor(CP)III,24hr | ug/24 hr | 6878-3 |
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