Lavender (EDTA), 4mL

Immediately following collection, mix sample thoroughly by gently inverting 8 - 10 times, to prevent clotting

Lavender (EDTA), 4mL

Refrigerated (preferred) - 8 days

Ambient - 1 day

Frozen - NO

• Frozen specimen
• Specimens other than EDTA whole blood
• Gross hemolysis

Whole blood washing and red blood cell harvesting/counting.

Liquid chromatography/tandem mass spectrometry (LC/MS-MS) after acidic hydrolysis

6-TGN
For treatment of inflammatory bowel disease (IBD)*
Suboptimal dosing:
            <235 pmol 6-TGN/8×108 red blood cells
Optimal dosing:
          235−450 pmol 6-TGN/8×108 red blood cells
Increasing risk for myelotoxicity and leucopenia :
        >450 pmol 6-TGN/8×108 red blood cells
 
6-MMPN
Hepatotoxicity risk:  >5700 pmol 6-MMPN/8×108 red blood cells

Once thiopurine therapy has been undertaken and an equilibrated drug level is achieved (usually 3 to 6 months), literature suggest that the measurement of thiopurine metabolites is warranted in the following situations:

1. Unresponsive patients to rule out:
1. patient non-compliance (low 6-MMP and low 6-TG in those not taking medications),
2. those with diversion of metabolites away from 6-TG production (low 6-TG and normal or increased 6-MMP),
3. those with refractory to treatment (adequate 6-TG but lack of clinical response), and
4. those with excessive 6-MMP (or increased 6-MMP:6-TG ratio with adequate 6-TG) leading to increased hepatotoxicity.
2. Clinically responsive patients to look for excessive levels of either 6-MMP or 6-TG to avoid toxicity.