Scale in the biological world
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1 Scale in the biological world
2 From living cells to atoms
3 A cell seen by TEM
4 Compartmentalisation in the cell: internal membranes and the cytosol
5 The cytosol: more than just H2O RNAs Proteins Ribosomes
6 Πιθανή εξελικτική πορεία για το Ε και την πυρηνική µεµβράνη
7 The Origin of mitochondria: The endosymbion hypothesis
8 Νέα οργανίδια φτιάχνονται από προυπάρχοντα οργανίδια ιαίρεση οργανιδίων κατά την κυτταρική διαίρεση Και Ανάπτυξη των µεµβρανών µε την προµήθεια λιπιδίων και πρωτεινών ΠΡΟΒΛΗΜΑ : ΙΑΛΟΓΗ ΠΡΩΤΕΙΝΩΝ PROTEIN SORTING
9 The Eukaryotic Cell
10 Different ways to target proteins in the cell
11 Mitochondria are essential for life
12 Energy Conversion: Mitochondria and Chloroplasts Membrane-bounded bounded Occupy a major fraction of cell volume Large amount of internal membrane Common pathway for energy conversion: Chemiosmotic coupling
13 Chemiosmotic coupling
14 The Mitochondrion 1. Substantial portion of cell volume About 20% of the volume of a eukaryotic cell Mitochondrial IM is 1/3 of total cell membrane 2. Mitochondrial function supplies 30 ATP molecules (only 2 ATP from anaerobic (cytosolic) glycolysis 3. Mobile, shape-changing,fusion/separation
15 EM view of a Mitochondrion 3D Reconstruction mobile, shape-changing
16 Large GTPases control mitochondrial fusion (Fzo1, OM) fission (Dnm1, OM) and Inner membrane remodelling (Mgm1, IMS)
17 Mitochondrial Structure Outer Membrane (semipermeable( semipermeable) 6% of total mit.protein lipid metabolism enzymes, porin IMS 6% of total mit.protein enzymes that use ATP to phosphorylate other nucleotides Inner Membrane (impermeable) 21% of total mit.protein ATP synthase,, respiratory chain enzymes, transport proteins Matrix 67% of total mit.protein Hundreds of enzymes, DNA, ribosomes, trnas
18 Mitochondrial Energy Metabolism
19 The Electrochemical Proton Gradient 140 mv 60 mv (-1 ph unit) TOTAL 200 mv
20 Active transport processes are driven by the electrochemical proton gradient
21 The Respiratory chain consists of 3 large membrane-embedded enzyme complexes
22 ATP Synthase is a reversible coupling device: It interconverts the energies of the electrochemical proton gradient and chemical bonds
23 Functional Complexity Structural Complexity Respiration and ATP Synthesis Synthesis of heme, lipids, amino acids and nucleotides Intracellular homeostasis of inorganic ions 5-15% of total cell protein 20% volume of eukaryotic cell IM is 1/3 of total cell membrane About 1000 different polypeptides (600 in yeast) Only a dozen encoded by mtdna
24 Protein import is the major mechanism of mitochondria biogenesis
25 Identification of components of the Mitochondrial Protein Import System Genetic analyses (fungal genetics) In vitro import assay system with isolated functional mitochondria Chemical Crosslinking Biochemical reconstitution
26
27 Import into the matrix - 1 Depends on a matrix-targeting signal: The presequence Cleavable, usually located at the N-terminus usually residues long amphiphilic, with positively charged residues on one side of an a-helix
28 Presequence binding to Tom20
29 Import into the matrix - 2 This is a multistep process Interactions with chaperones in the cytosol keep the precursor in an unfolded conformation ( import-competent ) Different import complexes in the OM (TOM complex) and the IM (TIM complex). Electrostatic interactions between the positive presequence and negative patches of receptors along the import pathway: The Acid chain hypothesis- Gradation of affinities leads the presequence along the import pathway The electrophoretic function of the potential across the IM draws the precursor across the IM The pulling force of the translocation motor mhsp70/tim44 actively draws the precursor to complete translocation
30 Import into the matrix - 3 Energy requirements: ATP Hydrolysis In the cytosol (function of ATPase chaperones) In the mitochondrial matrix (Hsp70 translocation motor) Electrochemical potential across the inner membrane
31 Import into the matrix - 4 Components TOM Complex: Receptors: Tom70, Tom20, Tom37, Tom22 Channel-forming: Tom40, Tom5 Channel modulating: Tom6, Tom7 TIM Complex: Receptor: Tim23 Channel-forming: Tim23, Tim17 Translocation motor: Tim44, Hsp70, GrpE (co-chaperone) chaperone)
32 Protein import into the matrix (70% of mitochondrial proteins) The essentials: presequence (amphipathic, positively charged) energetics: electrostatic and hydrophobic interactions of the presequence ATP hydrolysis (cytosolic chaperones and mthsp70) electrophoretic function of the electrochemical potential
33 Summary of Protein Import into the Mitochondrial Matrix II I IV III
34 Import into the IMS A. Variation of the matrix targeting pathway example: cytochrome b2 B. Distinct pathway involving a specific IMS targeting signal example: mitochondrial heme lyases
35 Cytb2 IMS targeting - 1 The Signal: Bipartite nature: matrix targeting signal followed by an IMS sorting signal IMS sorting signal contains mainly uncharged residues cleaved by specific IMS protease NOT very highly conserved
36
37 Cytb2 IMS targeting - 2 Energetics: Electrochemical potential absolutely essential but ATP hydrolysis s NOT required Components: Known Subunits of the TOM complex TIM23 complex IMS sorting peptidase Mechanism: Stop-transfer mechanism: the hydrophobic sorting signal is stuck at the TIM23 complex and laterally diffuses out into the lipid bilayer of the IM
38 Import into the IMS A. Variation of the matrix targeting pathway example: cytochrome b2 B. Distinct pathway involving a specific IMS targeting signal example: mitochondrial heme lyases
39 The Signal: Internal Heme Lyase IMS targeting - 1 about 60 residues long highly conserved sequence highly hydrophilic (30% charged residues, similar number of + and - charged residues, distributed throughout the sequence) mainly a-helical, a but NOT amphiphilic Key reference: Diekert et al Proc. National Acad. Sci.. USA 1999, 96,
40 Energetics: Heme Lyase IMS targeting - 2 Energy is provided by high affinity interactions with import components in the OM (TOM complex) and the IMS (trans side of Tom40 and unknown components) Components: Known Subunits of the TOM complex others unidentified yet (IMS?) Mechanism: Still unknown but TOM subunits thought to play a major role
41 Import into the IM A. Some IM proteins contain a presequence-like region internally: They are targeted via the TIM23 complex following a variation of the matrix targeting pathway The presequence is decoded by the TIM23 complex in a looped conformation B. IM proteins without a presequence: Example: Mitochondrial carriers like the ADP/ATP carrier (AAC) They follow a distinct import pathway
42 In mammalian cells mitochondrial carriers are involved in a number of disorders: diseases, like several myopathies obesity programmed cell death (apoptosis)
43 The Mitochondrial Carrier Family Function as metabolite transporters 37 proteins in yeast (10-15% of the total mitochondrial protein) kda Common topology: 3 similar repeated motifs (3X2 helix model)
44 Active transport processes are driven by the electrochemical proton gradient
45 Summary of Protein Import into the Mitochondrial Matrix II I IV III
46
47
48 II I III IV V
49 Properties of the small Tim proteins - 1 Sequence characteristics: They are all homologous They are intrinsically soluble (No transmembrane domains) They have a putative zinc-binding motif, twin CX3C motif X 15/16 Found in all eukaryotic cells Human homologue of Tim8 H 2 N C X 3 C Zn 2+ C X 3 C COOH involved in Mohr-Tranebjaerg syndrome Organisation in assemblies: Tim9/10 and Tim8/13 are found in 70 kda complexes in the IMS Tim12 is associated with the membrane-embedded embedded TIM22 complex (IM)
50 Properties of the small Tim proteins - 2 Function: Tim9/10 (essential( essential) ) function as chaperones in the IMS and facilitate targeting to the IM Tim12 (essential( essential) ) facilitates insertion in the context of the TIM22 complex Tim8/13 are non-essential but also seem to function as chaperones in the IMS
51 Distinct features of the carrier pathway compared to matrix targeting : 1. Internal targeting signals spanning the whole protein 2. Requirement for a chaperone function in the IMS 2. No ATP hydrolysis in the matrix is necessary 3. No translocation motor in the matrix is required 4. The electrochemical membrane potential across the IM is enough to complete insertion at the IM
52 KEY POINTS 1. Multiplicity of pathways to cope with targeting and sorting to the different mitochondrial compartment 2. All mitochondrial import processes are mediated by specific translocation machineries in all subcompartments 3. Only one TOM complex in the outer membrane through which all precursors are imported. After the barrier of the outer membrane, import routes to subcompartments divert. At least two distinct TIM complexes in the inner membrane
53 TOM SAM TIM23 TIM22 OXA1
54 Energy Conversion: Mitochondria and Chloroplasts Membrane-bounded bounded Occupy a major fraction of cell volume Large amount of internal membrane Common pathway for energy conversion: Chemiosmotic coupling
55 FUNCTIONAL and STRUCTURAL similarities among Mitochondria and Chloroplasts
56 Chloroplast features Photosynthesis: light-driven ATP synthesis Member of the plastid family of organelles: unique to plant cells All contain their own DNA
57 Chloroplasts resemble mitochondria but have an extra compartment
58 Comparison of a Mitochondrion and a Chloroplast
59
60
61
62 Photosynthesis reactions in a chloroplast Light reactions: Light-driven production of ATP and NADPH Dark reactions: Conversion of CO2 to carbohydrate Carbon-Fixation is catalysed in the chloroplast stroma by ribulose biphosphate carboxylase (500 kda), 50% of total chloroplast protein and the most abundant protein on earth
63 Electron Flow during photosynthesis in the chloroplast thylakoid membrane
64 The Electrochemical Proton Gradient is similar in mitochondria and chloroplasts
65 Overview of protein import into chloroplasts
66 Toc GTP GTP P 159 ATP P P hsp70 cytosol 34/ OE Tic hsp intermembrane space IE hsp100 hsp70 stroma SPP hsp70
67 Targeting of thylakoid proteins At least 4 different pathways: A. Soluble thylakoid lumen proteins 1. Sec pathway (unfolded proteins) 2. Tat pathway (fully-folded folded proteins, ph- dependent) B. Hydrophobic membrane proteins 1. SRP pathway 2. Spontaneous insertion
68 Toc Tic envelope Spontaneous insertion Sec/ATP A TAT/ ph FtsY SRP stroma YE B C A/E Alb3 lumen
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