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1 Phospholipid structure mphipathic molecule (phosphatidyl choline) hydrophobic part: fatty acids hydrophilic part: phosphate & choline

A&P - Ch.3 (Marieb, 8th Ed.)

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Marieb's 8th edition A&P book.Chapter 3 powerpoint

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Page 1: A&P - Ch.3 (Marieb, 8th Ed.)

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Phospholipid structure

Amphipathic molecule (phosphatidyl choline)hydrophobic part: fatty acidshydrophilic part: phosphate & choline

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Membrane structure

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Membrane components

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Transmembrane proteins

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Intercellular structures

Desmosomes

“spot welds”, dense proteins (cytoplasm & intercellular) fibers (intermediate filaments) extend across cells

epithelial cells (especially skin), cardiac intercalated disks

Tight junctions

cell “collar”, block large molecules, no lateral protein movement

epithelial cells

Gap junctions

cell-cell communication, small molecules (<1000 MWt)cardiac intercalated disks, smooth muscle

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Desmosomes

fig 3-10a

“spot welds”, dense proteins (cytoplasm & intercellular)

fibers (intermediate filaments) extend across cells

epithelial cells (especially skin), cardiac intercalated disks

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Tight junctions

fig 3-10b

cell “collar”, block large molecules, no lateral protein movement

epithelial tissue (esp. kidney, gut)

paracellular pathwaybetween cells

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Gap junctions

fig 3-10d

cell-cell communication, small molecules (<1000 MWt)

cardiac intercalated disks, smooth muscle

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Epithelial cell

fig 3-10c

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Protein ligand interaction

Proteins could be: Ligands would be:

enzymes substrates, allosteric regulators

receptors chemical messengers

transporters transported substances

transcription factors transcription regulators

any of above drugs

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Protein-ligand binding properties

Specificity:binding depends on ligand size, shape, charge

Affinity:strength of binding: i.e. [ligand] at 50% binding

Saturation:there is a finite number of binding sites

Competition:structurally similar molecules can compete for binding

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Specificity

binding depends on ligand size, shape, charge

fig 3-26 fig 3-27

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Specificity

protein Y specificity

greater than

protein X specificity

fig 3-28

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Affinity

strength of binding: i.e. [ligand] at 50% binding

fig 3-29

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Affinity & saturation

strength of binding: i.e. [ligand] at 50% binding

fig 3-30

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Affinity (different proteins)

strength of binding: i.e. [ligand] at 50% binding

fig 3-31

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Affinity (different ligands)

strength of binding: i.e. [ligand] at 50% binding

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Protein-ligand binding properties

Specificity:binding depends on ligand size, shape, charge

Affinity:strength of binding: i.e. [ligand] at 50% binding

Saturation:there is a finite number of binding sites

Competition:structurally similar molecules can compete for binding

and remember:the protein can be an enzyme, receptor, transporter, etc.

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Regulating binding site properties

a. Allosteric modulationreversible binding at another (“allo-”)

sitecan be activation or inhibition

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Regulating binding site properties

a. Covalent modulationchemical alteration of the proteincan be activation or inhibition

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Metabolism (pathways)

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Metabolism (key)

Key:A: glycogenesis, B: glycogenolysis, C: glycolysis, C+D: anaerobic

glycolysis (lactic acid fermentation), E: gluconeogenesis, F: irreversible step (pyruvate dehydrogenase), G: protein synthesis, H: proteolysis, I: lipogenesis, J: lipolysis, K: Krebs cycle, L: urea synthesis, M: ketogenesis

Anabolic pathways: A, G, I

Catabolic pathways: B, C, E, F, H, J, K

Liver only: E, L, M

Mitochondrial: K

Ribosomal: G

Smooth endoplasmic reticulum: I

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Energy content