Introduction
When energy demands rise or glucose is scarce (e.g., fasting, exercise), fatty acids become the primary fuel. Hormone-sensitive lipase (HSL) in adipose tissue is activated by glucagon and epinephrine, liberating FFAs into the bloodstream. FFAs, bound to serum albumin, are transported to oxidative tissues like heart, skeletal muscle, and liver. metabolismo de lipideos
Dysregulation of these pathways underlies major diseases. results from chronic positive energy balance, with hypertrophied adipocytes becoming insulin-resistant and releasing excess FFAs (lipotoxicity). Atherosclerosis is driven by retention of apoB-containing lipoproteins (LDL) in artery walls, where they become oxidized, triggering inflammation and plaque formation. NAFLD arises from ectopic TAG accumulation in the liver due to increased lipogenesis and reduced VLDL export, often in the context of insulin resistance. The carnitine shuttle defects cause hypoketotic hypoglycemia and cardiomyopathy in infants. Understanding these pathways has led to effective therapies: statins (HMG-CoA reductase inhibitors), fibrates (PPAR-α activators that enhance fatty acid oxidation), and emerging inhibitors of ACC or SCD1 for NAFLD. Introduction When energy demands rise or glucose is
Once inside the mitochondrial matrix, β-oxidation proceeds as a four-step cycle (dehydrogenation, hydration, dehydrogenation, thiolysis) that shortens the fatty acid chain by two carbons (acetyl-CoA) per turn. For a saturated 16-carbon palmitate, this yields 8 acetyl-CoA, 7 FADH2, and 7 NADH. The acetyl-CoA enters the TCA cycle for complete oxidation to CO2 and water, generating substantial ATP via oxidative phosphorylation. In times of prolonged fasting or uncontrolled diabetes, however, the liver produces acetyl-CoA in excess of the TCA cycle’s capacity. This surplus is channeled into —the synthesis of ketone bodies (acetoacetate, β-hydroxybutyrate, and acetone). Ketone bodies serve as a water-soluble, alternative fuel for the brain, heart, and muscle, preserving glucose for obligate users like red blood cells. Pathological overproduction leads to ketoacidosis, a life-threatening condition. Dysregulation of these pathways underlies major diseases
In conclusion, the metabolismo de lípidos is not a simple tale of fat storage and fuel use. It is an elegantly integrated system of digestion, transport, mitochondrial oxidation, ketone body production, and cytosolic synthesis of fatty acids and cholesterol. These pathways are dynamically tuned by hormonal signals (insulin, glucagon) and energy sensors (AMPK) to maintain metabolic homeostasis. From providing sustained energy during a marathon to building the phospholipid bilayers that define cellular life, from synthesizing steroid hormones to the pathological consequences of their dysregulation—lipid metabolism lies at the very core of human physiology and disease. A deep, mechanistic understanding of these processes is indispensable for developing rational therapies against the modern epidemics of metabolic syndrome and cardiovascular disease. Future research continues to uncover the nuances of lipid signaling, organelle crosstalk, and tissue-specific regulation, promising new targets for therapeutic intervention.
Inside the cell, FFAs are activated to fatty acyl-CoA by acyl-CoA synthetase. The critical entry step into the mitochondria, where β-oxidation occurs, is mediated by the carnitine shuttle. The enzyme carnitine palmitoyltransferase I (CPT1) is the rate-limiting, regulated step; it converts fatty acyl-CoA to acylcarnitine, which is transported across the inner mitochondrial membrane by translocase and then reconverted to acyl-CoA by CPT2. Malonyl-CoA, the first intermediate in fatty acid synthesis, allosterically inhibits CPT1—a prime example of reciprocal regulation between catabolism and anabolism.
The journey of dietary lipids begins in the gastrointestinal tract. The hydrophobic nature of triglycerides (TAGs), phospholipids, and cholesterol esters necessitates emulsification by bile salts in the small intestine. Pancreatic lipase, along with its cofactor colipase, then cleaves TAGs into free fatty acids (FFAs) and 2-monoacylglycerols. Phospholipase A2 acts on phospholipids, while cholesterol esterase hydrolyzes cholesterol esters. These breakdown products are incorporated into mixed micelles, which diffuse to the enterocyte brush border for absorption.