Advanced Laboratory Panel Interpretation

Advanced laboratory interpretation requires the NP to move beyond identifying individual abnormal values toward recognizing patterns, understanding physiological relationships between analytes, and integrating results with clinical context. A systematic approach follows: identify the primary abnormality, determine if it is acute or chronic, evaluate compensatory responses, and correlate with the clinical presentation.

The comprehensive metabolic panel (CMP) reveals interconnected physiological information. Sodium disorders require assessment of serum osmolality and volume status: hyponatremia with low osmolality and euvolemia suggests SIADH (check urine osmolality >100 and urine sodium >40); hyponatremia with hypervolemia suggests heart failure, cirrhosis, or nephrotic syndrome; hyponatremia with hypovolemia suggests renal or extrarenal salt losses. The BUN-to-creatinine ratio differentiates prerenal azotemia (ratio >20:1, due to dehydration/decreased renal perfusion) from intrinsic renal disease (ratio 10-20:1) and post-renal obstruction.

The complete blood count requires pattern recognition: pancytopenia (all three lineages decreased) suggests bone marrow failure (aplastic anemia, myelodysplastic syndrome, leukemia infiltration, severe B12/folate deficiency). Anemia classification by MCV directs the differential: microcytic (MCV <80) suggests iron deficiency or thalassemia (differentiate with iron studies and hemoglobin electrophoresis); normocytic (MCV 80-100) suggests acute blood loss, chronic disease, or hemolysis (check reticulocyte count); macrocytic (MCV >100) suggests B12/folate deficiency or medications (methotrexate, hydroxyurea).

Liver function panels must distinguish hepatocellular from cholestatic patterns: predominant AST/ALT elevation (transaminases >10x normal) suggests hepatocellular injury (viral hepatitis, toxin, ischemia); predominant alkaline phosphatase and GGT elevation suggests cholestasis (biliary obstruction, drug-induced); AST:ALT ratio >2:1 with GGT elevation strongly suggests alcoholic liver disease.