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Molecular Motors I

Molecular Motors I. Andy Howard Introductory Biochemistry 25 November 2008. Chemistry and movement. Most purposeful biological motion is effected through actions of molecular motors. It’s worthwhile to understand the biochemistry of these systems. Definition Microtubules and their partners

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Molecular Motors I

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  1. Molecular Motors I Andy HowardIntroductory Biochemistry 25 November 2008 Biochemistry: Motors

  2. Chemistry and movement • Most purposeful biological motion is effected through actions of molecular motors. It’s worthwhile to understand the biochemistry of these systems Biochemistry: Motors

  3. Definition Microtubules and their partners Tubulin Structure Cilia & flagella Microtubules (concluded) Movement of organelles Dyneins & kinesins DNA helicases Muscle contraction: for next time! Bacterial flagella What we’ll discuss Biochemistry: Motors

  4. What is a molecular motor? • A protein-based system that interconverts chemical energy and mechanical work Biochemistry: Motors

  5. Microtubules • 30-nm structures composed of repeating units of a heterodimeric protein, tubulin • -tubulin: 55 kDa • -tubulin: 55 kDa also • Structure of microtubule itself: polymer in which the heterodimers wrap around in a staggered way to produce a tube Biochemistry: Motors

  6. Tubulin structure •  and  are similar but not identical • Structure determined by electron diffraction, not X-ray diffraction • Some NMR structures available too • Two GTP binding sites per monomer • Heterodimer is stable if Ca2+ present Biochemistry: Motors

  7. iClicker quiz question 1 • Why might you expect crystallization of tubulin to be difficult? • (a) It is too big to crystallize • (b) It is too small to crystallize • (c) Proteins that naturally form complex but non-crystalline 3-D structures are resistant to crystallization • (d) It is membrane-bound • (e) none of the above Biochemistry: Motors

  8. Tubulin dimer • G&G Fig. 16.2 Biochemistry: Motors

  9. Microtubule structure • Polar structure composed of / dimers • Dimers wrap around tube as they move • Asymmetric: growth at plus end Biochemistry: Motors

  10. Treadmilling • Dimers added at plus end while others removed at minus end (GTP-dependent): that effectively moves the microtubule • Fig. 16.3 Biochemistry: Motors

  11. Role in cytoskeleton • Microtubules have a role apart from their role in molecular motor operations: • They are responsible for much of the rigidity of the cytoskeleton • Cytoskeleton contains: • Microtubules (made from tubulin) • Intermediate fibers (7-12nm; made from keratins and other proteins) • Microfilaments (8nm diameter: made from actin) Biochemistry: Motors

  12. Cytoskeletal components • Fig. 16.4 Biochemistry: Motors

  13. Cilia and flagella • Both are microtubule-based structures used in movement • Cilia: • short, hairlike projections, found on many animal and lower-plant cells • beating motion moves cells or helps moved extracellular fluid over surface • Flagella • Longer, found singly or a few at a time • Propel cells through fluids Biochemistry: Motors

  14. Axonemes • Bundle of microtubule fibers: • Two central microtubules • Nine pairs of joined microtubules • Often described as a 9+2 arrangement • Surrounded by plasma membrane that connects to the cell’s PM • If we remove the PM and add a lot of salt, the axoneme will release a protein called dynein Biochemistry: Motors

  15. Axoneme structure • Inner pair connected by bridge • Outer nine pairs connected to each other and to inner pair • Fig. 16.5 Biochemistry: Motors

  16. How cilia move • Each outer pair contains asmaller, static A tubule anda larger, dynamic B tubule • Dynein walks along B tubulewhile remaining attached toA tubule of a different pair • Crosslinks mean the axoneme bends • Dynein is a complex protein assembly: • ATPase activity in 2-3 dynein heavy chains • Smaller proteins attach at A-tubule end Biochemistry: Motors

  17. Dynein movement • Fig. 16.6 Biochemistry: Motors

  18. Inhibitors of microtubule polymerization • Vinblastine & vincristine are inhibitors: show antitumor activity by shutting down cell division • Colchicine inhibits microtubule polymerization: relieves gout, probably by slowing movement of white cells Biochemistry: Motors

  19. Paclitaxel: a stimulator • Formerly called taxol • Stimulates microtubule polymerization • Antitumor activity • Stimulates search for other microtubule polymerization stimulants Biochemistry: Motors

  20. iClicker question 2 2. How do you imagine paclitaxel might work? • (a) by producing frantic cell division • (b) by interfering with microtubule disassembly, preventing cell division • (c ) by causing changes in tertiary structures of  and  tubulin • (d) none of the above Biochemistry: Motors

  21. Movement of organelles and vacuoles • Can be fast:2-5 µm s-1 • Hard to study • 1985: Kinesin isolated • 1987: Cytosolic dynein found Biochemistry: Motors

  22. Cytosolic dynein • Mostly moves organelles & vesicles from (+) to (-), so it moves things toward the center of the cell • Heavy chain ~ 400kDa, plus smaller peptides (53-74 kDa) • Microtubule-activated ATPase activity Biochemistry: Motors

  23. Kinesin • Mostly moves organelles from (-) to (+) • That has the effect of moving things outward • 360 kDa: 110 kDa heavy chains, also 65-70 kDa subunits (2 + 2?) • Head domain of heavy chain (38 kDa) binds ATP and microtubule: cooperative interactions between pairs of head domains in kinesin, causing conformational changes in a single tubulin subunit • 8 nm movements along long axis of microtubule Biochemistry: Motors

  24. Kinesin motion depicted • Rolling movement involving two head domains at a time • Fig. 16.8(b) Biochemistry: Motors

  25. Hand-over-hand kinesin model • Two head groups begin in contact • After ATP hydrolysis hindmost head passes forward head • ATP binds to new leading head • Pi dissociates from trailing head Biochemistry: Motors

  26. DNA helicases • To replicate DNA we need to separate the strands • Efficient only if the helicase can travel along the duplex quickly • This kind of movement is called processive • E.coli BCD helicase can unwind 33kbp before it falls off • If we want to replicate DNA rapidly, we need processivity Biochemistry: Motors

  27. Achieving processivity • Some helicases form rings that encircle 1 or both strands of the duplex • Others, like rep helicase, are homodimeric; move hand-over-hand along the DNA, like kinesin Biochemistry: Motors

  28. Negative cooperativity • Rep is monomeric without DNA • Each monomer can bind either ss or dsDNA • BUT after one monomer binds DNA, the second subunit’s affinity drops 104-fold! Biochemistry: Motors

  29. Muscle contraction • This is an obvious case of an energy-dependent biological motion system • Involves an interaction called the sliding filament model, in which myosin molecules slide past actin molecules • Many other proteins and structural components involved • We’ll discuss this in detail next Tuesday Biochemistry: Motors

  30. Bacterial flagella • E.coli flagellum is 10 µm in length, 15 nm in diameter • ~6 filaments on surface of cell rotate counter-clockwise: that makes them bundle together and propel the cell through medium • Enabled by rotation of motor protein complexes in plasma membrane Biochemistry: Motors

  31. Motor structure • >= 2 rings, ~25nm diameter (M & S) • Rod attaches those to the helical filament • Rings surrounded by array of membrane proteins • This one is driven by a proton gradient, not by ATP hydrolysis: [H+]out > [H+]in, so protons want to move in • If we let protons in, we can use the thermodynamic energy to drive movement • Requires 800-1200 protons per full rotation! Biochemistry: Motors

  32. The shuttle • MotA & MotB form shuttling device • Proton movement drives rotation of flagellar motor • Fig. 16.26 Biochemistry: Motors

  33. iClicker question 3 3. Compare the pH inside the cell to the pH outside. • (a) pHin < pHout • (b) pHin> pHout • (c ) pHin = pHout • (d) We don’t have enough information to answer this question. Biochemistry: Motors

  34. Berg’s model • motB has protonexchanging sites • motA has half-channels—one half facing toward the inside of the cell, one facing out • When a motB site is protonated, the outside edges of motA can’t move past it • Center of motA can’t move past site when it’s empty • Those constraints cause coupling between proton translocation and rotation Biochemistry: Motors

  35. Coupling described • Proton enters outside of motA and binds to an exchange site on motB • motA is linked to cell wall, so when it rotates, it puts the inside channel over the proton • Proton moves through inside channel into cell; then another proton travels up the outside channel to bind to the next exchange site • That pulls the complex to the left, leading to counterclockwise rotation of disc, rod, & helical filament Biochemistry: Motors

  36. Coupling depicted • Fig. 16.27 Biochemistry: Motors

  37. What if it got reversed? • If outside became alkaline, the flagellar filaments would rotate clockwise • That doesn’t work as well because it loosens the microtubule Biochemistry: Motors

  38. Quantitation • M ring has about 100 motB exchange sites • 800-1200 protons for a full rotation of the filament • That enables ~ 100 rotations/sec Biochemistry: Motors

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