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Lipoprotein Structures, Function and Metabolism (1)

Lipoprotein Structures, Function and Metabolism (1)

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Page 2: Lipoprotein Structures, Function and Metabolism (1)

Lecture Outline

• What are lipoproteins?

• What do they do?

• Basic structure of lipoproteins

• Lipoprotein metabolism

• Hyperlipoproteinemia

• Cholesterol and bile acid metabolism

• Role of lipoproteins in atherosclerosis

Page 3: Lipoprotein Structures, Function and Metabolism (1)

What are lipoproteins?

• Molecular complexes that consist of lipids and proteins. They function as transport vehicles for lipids in blood plasma.

• Lipoproteins deliver the lipid components (cholesterol and triglyceride etc.) to various tissues for utilization.

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Hydrophobic lipids

Amphiphilic lipids

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In phospholipids

X=

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Structure of lipoprotein Hydrophobic lipids (TG, CE) in the core Amphiphilic lipids (C, PL) and proteins on the surface

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Classification of plasma lipoproteins according to their density

• Chylomicron (CM)

• Very low density lipoprotein (VLDL)

• Intermediate density lipoprotein (IDL)

• Low density lipoprotein (LDL)

• High density lipoprotein (HDL)

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• Each contains different kinds and amounts of lipids and proteins

– The more protein, the higher the density

– The more lipid, the lower the density

• Each has different function

Lipoproteins

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CM VLDL LDL HDL

Density (g/mL) <0.96 0.96-1.006 1.006-1.063 1.063-1.21

Diameter (nm) 100-1000 30-90 20-25 10-20

Apolipoprotein A,C,E,B48 A,C,E,B100 B100 A,C,D,E

Composition (%)

Proteins 2 10 20 40

Lipids 98 90 80 60

Lipid composition (%)

TG 88 55 12 12

CE+C 4 24 59 40

PL 8 20 28 47

Free fatty acid - 1 1 1

Characteristics of human plasma lipoproteins

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Classification of plasma lipoproteins according to

their electrophoretic mobility

(CM)

-lipoprotein (HDL)

Pre--lipoprotein (VLDL)

-lipoprotein (LDL)

CM

1967, Fredrickson et al.

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Important enzymes and proteins involved in lipoprotein metabolism

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LPL (Lipoprotein Lipase)

• Locate in extracellular on the walls of

blood capillaries, anchored to the endothelium.

• Hydrolyze triglyceride (TG) in the core of

CM and VLDL to free fatty acids and glycerol.

• The free fatty acids are transported into the

tissue, mainly adipose, heart, and muscle (80%),

while about 20% goes indirectly to the liver.

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HL (Hepatic Lipase)

• Bound to the surface of liver cells,

• Hydrolyzes TG to free fatty acids and glycerol

• Unlike LPL, HL does not react readily with CM or VLDL but is concerned with TG hydrolysis in VLDL remnants and HDL metabolism

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LCAT (Lecithin:Cholesterol Acyltransferase)

Formation of cholesterol esters in lipoproteins

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CETP

(Cholesterol Ester Transfer Protein)

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Apolipoproteins

• Act as structural components of lipoproteins

• Recognize the lipoprotein receptors on cell membrane surface as ligand

• Activate/inhibit enzymes involved in lipoprotein metabolism

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• Apo AI: Activator LCAT

• Apo AII: Inhibitor of hepatic lipase (HL)

• Apo A-IV: Activator of LCAT

• Apo B-100 (liver, 4564 Aa): structure, ligand

• Apo B-48 (intestine, 2152Aa): structure

• Apo C-I : Activator of LCAT

• Apo C-II: Activator of LPL

• Apo C-III: Inhibitor of LPL

• Apo D: Function unknown

• Apo E: Ligand

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ApoB100 and ApoB48 come from same gene

In liver

In intestine

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What do lipoproteins do?

• Serve to transport lipids and lipid-soluble compounds between tissues and organs

– Substrates for energy metabolism (TG)

– Essential components for cells (PL, C)

– Precursors for hormones (C)

– Lipid soluble vitamins

– Precursors for bile acids (C)

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Metabolism of chylomicrons

Surface Monolayer Surface Monolayer Phospholipids Phospholipids Free Cholesterol Free Cholesterol Protein Protein

Hydrophobic CoreHydrophobic CoreTriglyceride Triglyceride Cholesteryl Esters Cholesteryl Esters

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Metabolism of chylomicrons

• Transport dietary TG and Cholesterol from the intestine to the peripheral tissues

• The dietary TG are first acted by intestine lipase and absorbed as monoacylglycerol, fatty acid and glycerol. Within the intestine cells, they are resynthesized into TG.

• CM are synthesized in the intestine using TG, PL, C, ApoB48, and ApoAs and secreted into the lymph and reach blood through thoracic duct.

• Nascent CM pick up apoE, apoCs and some apoAs from HDL.

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• In the capillaries of peripheral tissue, lipoprotein lipase (LPL) degrades triglycerol (TG) of chylomicrons to fatty acids (FA) and glycerol which enter tissues by diffusion

• Lipoprotein lipase (LPL) is activated by apo C-II

• After most of the TG is removed, chylomicrons become chylomicron remnants. During the process, CM give apoC and apoA to HDL

Metabolism of chylomicrons

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• CM remnants bind to specific receptors on the surface of liver cells through apo E and then the complex is endocytosed. remnant receptor or apoE receptor or LRP (LDL receptor-related protein)

• Chylomicron remnants deliver dietary cholesterol and some cellular cholesterol (via HDL) to the liver.

• Half life of CM is short, less than 1 hour.

Metabolism of chylomicrons

Page 25: Lipoprotein Structures, Function and Metabolism (1)

Metabolic fate of chylomicrons. (A, apolipoprotein A; B-48, apolipoprotein B-48; , apolipoprotein C; E, apolipoprotein E; HDL, high-density lipoprotein; TG, triacylglycerol; C, cholesterol and cholesteryl ester; P, phospholipid; HL, hepatic lipase; LRP, LDL receptor-related protein.) Only the predominant lipids are shown.

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Metabolism of VLDL and LDL

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VLDL• VLDL are made by liver. Liver synthesizes TG and cholesterol and

packages them into VLDL for export into blood.

• Most lipid in the core of VLDL is triglyceride

• Nascent VLDL contain apoB100. In blood nascent VLDL pick up apoE and apoCs from HDL and become matured VLDL.

Page 28: Lipoprotein Structures, Function and Metabolism (1)

VLDL

• In the capillaries of various tissues, LPL degrades TG to fatty acids and glycerol, which enter the tissues by diffusion. ApoC-II is needed in this step to activate LPL.

• When VLDL loses triglyceride, it transforms into VLDL remnant, also named as IDL (intermediate-density lipoprotein).

• During the process, some apolipoproteins (apo As and apoCs) are transferred back to HDL.

• VLDL function: Deliver TG from liver to peripheral tissue cells.

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Fates of VLDL remnants (IDL)

• Results from loss of TG in VLDL

• Contains relatively more cholesterol esters

• Taken up by liver or transform into LDL

1) A proportion of the VLDL remnant (IDL) is taken up by liver through the LDL receptor (apoE-mediated).

2) The other remnant is further acted upon by hepatic lipase (HL) and converted into LDL. LDL loses all apolipoproteins except apoB100.

VLDL remnant

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LDL

Most core lipid in LDL is cholesterol ester.

ApoB100 is only apolipoprotein in the surface.

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LDL receptor• Also named as apoB-100/apoE receptors

• LDL receptors exist in the liver and in most peripheral tissues

• The complexes of LDL and receptor are taken into the cells by endocytosis, where LDL is degraded but the receptors are recycled

• LDL cholesterol levels are positively related to risk of cardiovascular disease

• Therefore, cholesterol in LDL has been called “bad cholesterol”