Learning Objectives

• Differentiate the four major types of Familial Dyslipidemias by inheritance and blood levels.
• Identify the pathognomonic clinical findings (e.g., palmar xanthomas, Achilles tendon xanthomas).
• Explain the biochemical defects involving LPL, Apo CII, Apo B-100, and Apo E.
• Recognize which types carry an accelerated risk for atherosclerosis.

1. Type I: Hyperchylomicronemia

An autosomal recessive disorder where the body cannot “cut” the triglycerides out of chylomicrons.

• Pathogenesis: Deficiency in Lipoprotein Lipase (LPL) or its cofactor, Apo CII.
• Blood Levels: Massive elevation in Chylomicrons and Triglycerides (TG).
• Clinical: Recurrent acute pancreatitis, hepatosplenomegaly, and eruptive/pruritic xanthomas.
• Key Note: Surprisingly, there is no increased risk for atherosclerosis. A “creamy” layer forms in the supernatant of standing plasma.

2. Type II: Hypercholesterolemia

An autosomal dominant disorder leading to dangerously high cholesterol levels.

• Pathogenesis: Absent or defective LDL receptors, or defective Apo B-100.
• Blood Levels:
  • IIa: Elevated LDL and Cholesterol.
  • IIb: Elevated LDL, Cholesterol, and VLDL.
• Clinical: Accelerated atherosclerosis (MI can occur before age 20 in homozygotes), tendon (Achilles) xanthomas, and corneal arcus.

3. Type III: Dysbetalipoproteinemia

An autosomal recessive disorder where the liver cannot “grab” remnants.

• Pathogenesis: Defective Apo E (Defective in Type thrEE).
• Blood Levels: Elevated Chylomicron remnants and VLDL (IDL).
• Clinical: Premature atherosclerosis and palmar xanthomas (yellow creases in the palms).

Activity:

4. Type IV: Hypertriglyceridemia

An autosomal dominant disorder is often linked to metabolic health.

• Pathogenesis: Hepatic overproduction of VLDL.
• Blood Levels: Elevated VLDL and TG.
• Clinical: Extremely high triglycerides (> 1000 mg/dL) can cause acute pancreatitis. This type is strongly related to insulin resistance.

Activity: Dyslipidemia Matching Challenge

Activity: