Parvin

spinqualitylabelsall models PDB ID 2vzc Show:Asymmetric Unit Biological Assembly Drag the structure with the mouse to rotate   Export Animated Image

Alpha-parvin^[1], also known as actopaxin^[2] or CH domain-containing integrin-linked kinase (ILK)-binding protein (CH-ILK-BP)^[3] is an adapter protein known to interact with a number of focal adhesion proteins leading to focal adhesion stabilisation. Knock-out analysis confirmed it to be essential for efficient directional cell migration during embryogenesis in mice^[4]. Spatially and temporarily regulated dynamic changes in the phosphorylation status of alpha-parvin at serines 4 and 8 and consequent changes in affinities towards its binding partners (icluding CdGAP, TESK1 and possibly others, e.g. ILK) may be responsible for 1) focal adhesion turnover (disassembly of old adhesions, assembly of new ones) and 2) actin cytoskeleton reorganization, two interrelated processes contributing to cell migration.^[5][6][7][8]

Contents 1 Biological significance 1.1 Focal adhesions and cell migration 1.2 Alpha-parvin's interactions in the adhesome 1.3 Alpha-parvin phosphorylation and cell migration 2 Structure and function 2.1 Domain composition 2.2 C-terminal CH domain 2.3 Paxillin binding 2.4 ILK binding 3 3D structures of Alpha-parvin 4 References

Biological significance

Focal adhesions and cell migration

The extracellular matrix (ECM) composed of matrix molecules such as collagens, laminins, proteoglycans and non-matrix proteins including growth factors, provides physical support and mediates bidirectional flow of signals in all tissues and organs^[9]. Cell-ECM attachments, critical for appropriate localization and functioning of cells, are mediated by integrins.^[10]The engagement of integrins to the ECM results in the recruitment of various proteins to the cell periphery and consequent assembly of dot-like focal complexes (FXs or nascent adhesions), which can mature to much larger focal adhesions (FAs or focal contacts). Focal adhesions are bound to the integrins on one hand and to the actin cytoskeleton on the other, thus accounting for the mechanical continuity and signal transduction between the ECM outside the cell and the cytoskeleton inside the cell.^[11] The complex FA network (the adhesome), is composed of, among others, actin regulators, Tyr and Ser/Thr kinases and phosphatases, phosphatidylinositols and their modifiers, Rho family GTPases and their effectors. Interactions between these components are mediated by various adapter proteins, including talin, vinculin, paxillin and alpha-parvin^[12]. FAs can grow and shrink and, even in stationary cells, disappear on average tens of minutes after maturation.^[13] The spatially and temporarily regulated FA turnover together with changes in cytoskeletal contractability enable cell migration in development and regeneration.^[14][15]

Alpha-parvin's interactions in the adhesome

Alpha-parvin is thus a component of the adhesome, but a more basic unit of which it is part is the IPP (ILK-PINCH-parvin) complex. The central component of this complex, ILK, binds both PINCH and alpha-parvin, which do not interact directly with each other, and it is by means of ILK's pseudokinase domain that the complex is recruited to the cytoplasmic tail of integrins. The IPP complex is important for the correct FA assembly and promotes anti-apoptotic signalling^[16]. Alpha-parvin is also known to interact with a number of other proteins, including F-actin^[17], paxillin^[18][19], paxillin's homologue HIC5^[20] (and possibly also another paralogue, leupaxin^[21]), TESK1^[22], CdGAP^[23] and alphaPIX^[24].

Alpha-parvin phosphorylation and cell migration

Alpha-parvin possesses 6 putative proline-directed serine/threonine phosphorylation targets (residues 4, 8, 14, 16, 19, 61), of which serines 4 and 8 were shown to be the most important. Phosphorylation of alpha-parvin at serines 4 and 8 is correlated with the tightly regulated process of FA turnover during cell migration. Firstly, phosphorylation of these residues by cyclin B1/cdc2 is observed in the context of mitosis, whereby it contributes to FA disassembly required for cell-rounding prior to cell division, suggesting it may cause a similar effect during cell migration.^[25] Indeed, in migrating cells these residues are observed to be phosphorylated^[26], likely as a result of MAP kinase^[27] and/or PI3K^[28]. Secondly, phosphomimetic mutations of serines 4 and 8 to aspartates result in faster migration and spreading, while mutations preventing phosphorylation impair these processes.^[29] Finally, as has already been mentioned in the introduction, knock-out mice phenotype (embryonic lethality due to severe cardiovascular defects) suggests alpha-parvin deficiency results in impaired directional migration of endothelial cells during embryonic development, heart development in particular.^[30] The macroscopic effects of alpha-parvin phosphorylation likely result from the altered affinity for its binding partners. So far it has been demonstrated that phosphorylation at serines 4 and 8 affects binding of alpha-parvin to TESK1 and CdGAP. When TESK1 is bound to alpha-parvin it is prevented from severing actin fibres. TESK1 is thought to be released from inhibition upon alpha-parvin phosphorylation and this can contribute to the decomposition of actin fibres and FA disassembly.^[31] CdGAP, on the other hand, is involved in the regulation of small GTPase signalling, which accounts for changes in cytoskeletal contractability during cell migration.^[32] Evidence suggesting that also the interaction with ILK is affected by phosphorylation is not strong^[33][34], but it is likely that this or yet other binding partners bind in the phosphorylation-dependent manner.

Structure and function

Domain composition

Alpha-parvin's structure can be divided into four regions: 1) N-terminal flexible domain (residues 1-96), 2) N-terminal CH domain (97-200 according to SMART^[35]), 3) linker region (201-241) and 4) C-terminal CH domain (242-372 identified by limited subtilisin proteolysis^[36]). Most interactions of alpha-parvin are mapped to the C-terminal CH domain, but CdGAP and perhaps alphaPIX or other, yet unknown partners, interact with the N-terminal flexibile domain. This flexible domain seems to lack a well defined 3D structure and can therefore be classified as a putative intrinsically disordered region. The interactions of this regions with the binding partners are therefore likely to be characterized by relatively low affinity, but high affinity nonetheless.^[37] The abovementioned phosphorylation sites (serines 4 and 8) involved in focal adhesion regulation are located in this segment, which makes them so called disorder-enhanced phosphorylation sites.^[38][39]

spinqualitylabelsall models Structure of the C-terminal CH domain(2vzc) Show:Asymmetric Unit Biological Assembly Drag the structure with the mouse to rotate   Export Animated Image

C-terminal CH domain

The calponin-homology (CH) domains are helical structural units around 100 amino acids long. They comprise at least four helices, three of them forming a helical bundle. CH domains usually comprise elements of big multidomain proteins and are present either in singlet^[40] or duplex/tandem arrangement.^[41] The tandem arrangement of CH domains is often associated with F-actin binding^[42][43] (and is thus called actin-binding domain or ABD), but generally CH domains seem to be characterized by functional plasticity and ability to bind various structural motifs.^[44] In the case of alpha-parvin, the interactions of CH domains with both F-actin and other partners (paxillin, ILK) are observed. The interactions with paxillin and ILK are mediated by a single CH domain, the C-terminal one. This domain has attracted most attention. While no full-length structure of alpha-parvin has been solved to date, the structure of the C-terminal CH domain, on its own^[45] and in complexes (with paxillin^[46][47] and the pseudokinase domain of ILK^[48]) are available.

The scene on the left shows the structure of the at around 1.05 Å (2vzc). When a sequence alignment of alpha-parvin with all its sequence homologues is performed and the protein is coloured according to , one can see that the highest degree of conservation is exhibited by the residues located in , while the residues in linker helices and loops are less conserved. When the of the C-terminal CH domain of alpha-parvin and one of the CH domains of alpha-actinin 3 (1wku) is performed, a good overall overlap is observed, as represented by the RMSD of 1.19 Å for 103 equivalent C^α positions, despite low sequence homology (≤26% identity).^[49] Again the best overlap is seen for the core helices. This suggests that the structural framework of CH domain and its core in particular are quite robust under evolution.

The most diverged fragments in the C-terminal CH domain of alpha-parvin correspond to 1) an (so called N-terminal linker helix; it is labelled αN or helix N) located at the N-terminal end of the domain and not observed in any other CH domain and 2) a between two helices (αC and αE). One could ask whether the N-terminal linker helix is an integral part of the C-terminal CH domain or just a part of a linker region between the two CH domains. The fact that it interacts strongly with the core helices by means of both electrostatic () and hydrophobic () interactions suggests that it is indeed integral to the domain. The long loop mentioned above contains a (313-315) relative to other known CH domains and differs in conformation between different structures of alpha-parvin, suggesting it is relatively flexible.^[50] Interestingly, these two regions, the N-terminal linker helix and the long loop, are involved in binding of alpha-parvin to its binding partners, paxillin and ILK respectively.

spinqualitylabelsall models The alignment of three C-terminal CH domains of alpha-parvin bound to different paxillin LD motifs (2vzd, 2vzg, 2vzi) Show:Asymmetric Unit Biological Assembly Drag the structure with the mouse to rotate   Export Animated Image

Paxillin binding

The shows the superimposition of the three conformations that alpha-parvin adopts when bound to paxillin LD motifs, LD1 (2vzd), LD2 (2vzg) and LD4 (2vzi) respectively. These three LD motifs differ in sequence, but they are all helical. Surprisingly, the orientation of LD1 binding is reversed compared to that of LD2 and LD4. One of the LD motifs (LD1) is shown in the scene, represented by a blue helix. LD2 and LD4 are not shown, but they bind in the same location. As you can see, all three peptides, despite different sequences and different binding orientations, induce a very similar conformation of alpha-parvin, as represented by a very good alignment of the three alpha-parvin structures coloured differently. In particular, residues 248 to 264, which experience conformational change upon binding, are similar in all complexes with RMSD values of 0.28 Å (LD1 versus LD2), 0.23 Å (LD1 versus LD4), and 0.15 Å (LD2 versus LD4) in 16 equivalent C^α positions.^[51]

When you the structure of one of the alpha-parvin-LD complexes, say the one with LD1 peptide bound, and the structure of alpha-parvin on its own (apo), you also get a good overall overlap (disregarding the long loop between helices αC and αE which, as was said before, is relatively flexible), but you can see that the has slightly altered conformation. In particular, the angle between the

spinqualitylabelsall models Kinase domain of ILK/C-terminal CH domain of alpha-parvin core complex (3kmw) Show:Asymmetric Unit Biological Assembly Drag the structure with the mouse to rotate   Export Animated Image

N-linker helix and αA widens by around 15° and the N-linker helix rotates.^[52] In this paragraph the binding of paxillin to the isolated C-terminal CH domain was described. However, the NMR measurements in solution confirmed that the rest of alpha-parvin molecule makes little energetic contribution to the binding. The pictue is not complete, though, since it is possible that the conformational alterations induced by LD binding in the N-terminal part of the C-terminal CH domain are somehow propagated to the nearby linker region and thus the rest of the molecule, possible affecting the behaviour of alpha-parvin towards other binding partners.

ILK binding

The shows the complex (3kmw) of the kinase domain of integrin-linked kinase (ILK, red) bound to the C-terminal CH domain of alpha-parvin (blue). One can also see the molecule of ATP (green) and the space-fill representation of the magnesium atom (white). When we so that the N-terminal helix (now orange) of the CH domain of alpha-parvin is pointing up, we can see that unlike paxillin LD motifs, ILK kinase domain does not bind to the N-terminal region of the CH domain, but rather near the between helices αC and αE. Other parts of the CH domain are also involved in binding, leading to a high interface area (around 1900 Ų) characteristic of high-affinity complexes.^[53] Interestingly, ILK, which was recently proved to lack kinase activity^[54][55], binds alpha-parvin analogously to the way in which kinases bind their substrates, i.e. with its pseudoactive site. The binding is not dependent on the presence of ATP. On the ILK's side the binding is mediated primarily by (αG) and a . The complex formation is particularly dependent on in αG of ILK - if these two residues are mutated to alanines, the complex formation is completely abolished. These residues are involved in many interactions with alpha-parvin (one of them, a hydrogen bond to asparagine 280, is shown) or water molecules (one of them shown as a pink dot).

3D structures of Alpha-parvin

Updated on 24-April-2013

3kmu - hAPAR + integrin-linked kinase pseudokinase domain – human

3rep, 3kmw – hAPAR + integrin-linked kinase pseudokinase domain + ATP
2vzc – hAPAR calponin homology domain
2vzd, 2vzg, 2vzi - hAPAR calponin homology domain + paxillin motif
2k2r - hAPAR calponin homology domain + paxillin LD1 motif - NMR

References

1. ↑ Olski TM, Noegel AA, Korenbaum E. Parvin, a 42 kDa focal adhesion protein, related to the alpha-actinin superfamily. J Cell Sci. 2001 Feb;114(Pt 3):525-38. PMID:11171322
2. ↑ Nikolopoulos SN, Turner CE. Actopaxin, a new focal adhesion protein that binds paxillin LD motifs and actin and regulates cell adhesion. J Cell Biol. 2000 Dec 25;151(7):1435-48. PMID:11134073
3. ↑ Tu Y, Huang Y, Zhang Y, Hua Y, Wu C. A new focal adhesion protein that interacts with integrin-linked kinase and regulates cell adhesion and spreading. J Cell Biol. 2001 Apr 30;153(3):585-98. PMID:11331308
4. ↑ Montanez E, Wickstrom SA, Altstatter J, Chu H, Fassler R. Alpha-parvin controls vascular mural cell recruitment to vessel wall by regulating RhoA/ROCK signalling. EMBO J. 2009 Oct 21;28(20):3132-44. Epub 2009 Oct 1. PMID:19798050 doi:10.1038/emboj.2009.295
5. ↑ Clarke DM, Brown MC, LaLonde DP, Turner CE. Phosphorylation of actopaxin regulates cell spreading and migration. J Cell Biol. 2004 Sep 13;166(6):901-12. Epub 2004 Sep 7. PMID:15353548 doi:10.1083/jcb.200404024
6. ↑ LaLonde DP, Brown MC, Bouverat BP, Turner CE. Actopaxin interacts with TESK1 to regulate cell spreading on fibronectin. J Biol Chem. 2005 Jun 3;280(22):21680-8. Epub 2005 Apr 6. PMID:15817463 doi:10.1074/jbc.M500752200
7. ↑ LaLonde DP, Grubinger M, Lamarche-Vane N, Turner CE. CdGAP associates with actopaxin to regulate integrin-dependent changes in cell morphology and motility. Curr Biol. 2006 Jul 25;16(14):1375-85. PMID:16860736 doi:S0960-9822(06)01676-9
8. ↑ Yang Y, Guo L, Blattner SM, Mundel P, Kretzler M, Wu C. Formation and phosphorylation of the PINCH-1-integrin linked kinase-alpha-parvin complex are important for regulation of renal glomerular podocyte adhesion, architecture, and survival. J Am Soc Nephrol. 2005 Jul;16(7):1966-76. Epub 2005 May 4. PMID:15872073 doi:10.1681/ASN.2004121112
9. ↑ Hynes RO. The extracellular matrix: not just pretty fibrils. Science. 2009 Nov 27;326(5957):1216-9. PMID:19965464 doi:10.1126/science.1176009
10. ↑ Barczyk M, Carracedo S, Gullberg D. Integrins. Cell Tissue Res. 2010 Jan;339(1):269-80. Epub 2009 Aug 20. PMID:19693543 doi:10.1007/s00441-009-0834-6
11. ↑ Wolfenson H, Henis YI, Geiger B, Bershadsky AD. The heel and toe of the cell's foot: a multifaceted approach for understanding the structure and dynamics of focal adhesions. Cell Motil Cytoskeleton. 2009 Nov;66(11):1017-29. PMID:19598236 doi:10.1002/cm.20410
12. ↑ Zaidel-Bar R, Itzkovitz S, Ma'ayan A, Iyengar R, Geiger B. Functional atlas of the integrin adhesome. Nat Cell Biol. 2007 Aug;9(8):858-67. PMID:17671451 doi:10.1038/ncb0807-858
13. ↑ Wolfenson H, Henis YI, Geiger B, Bershadsky AD. The heel and toe of the cell's foot: a multifaceted approach for understanding the structure and dynamics of focal adhesions. Cell Motil Cytoskeleton. 2009 Nov;66(11):1017-29. PMID:19598236 doi:10.1002/cm.20410
14. ↑ Zaidel-Bar R, Geiger B. The switchable integrin adhesome. J Cell Sci. 2010 May 1;123(Pt 9):1385-8. PMID:20410370 doi:10.1242/jcs.066183
15. ↑ Gardel ML, Schneider IC, Aratyn-Schaus Y, Waterman CM. Mechanical integration of actin and adhesion dynamics in cell migration. Annu Rev Cell Dev Biol. 2010 Nov 10;26:315-33. PMID:19575647 doi:10.1146/annurev.cellbio.011209.122036
16. ↑ Attwell S, Mills J, Troussard A, Wu C, Dedhar S. Integration of cell attachment, cytoskeletal localization, and signaling by integrin-linked kinase (ILK), CH-ILKBP, and the tumor suppressor PTEN. Mol Biol Cell. 2003 Dec;14(12):4813-25. Epub 2003 Sep 5. PMID:12960424 doi:http://dx.doi.org/10.1091/mbc.E03-05-0308
17. ↑ Olski TM, Noegel AA, Korenbaum E. Parvin, a 42 kDa focal adhesion protein, related to the alpha-actinin superfamily. J Cell Sci. 2001 Feb;114(Pt 3):525-38. PMID:11171322
18. ↑ Wang X, Fukuda K, Byeon IJ, Velyvis A, Wu C, Gronenborn A, Qin J. The structure of alpha-parvin CH2-paxillin LD1 complex reveals a novel modular recognition for focal adhesion assembly. J Biol Chem. 2008 Jul 25;283(30):21113-9. Epub 2008 May 28. PMID:18508764 doi:10.1074/jbc.M801270200
19. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
20. ↑ Nikolopoulos SN, Turner CE. Actopaxin, a new focal adhesion protein that binds paxillin LD motifs and actin and regulates cell adhesion. J Cell Biol. 2000 Dec 25;151(7):1435-48. PMID:11134073
21. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
22. ↑ LaLonde DP, Brown MC, Bouverat BP, Turner CE. Actopaxin interacts with TESK1 to regulate cell spreading on fibronectin. J Biol Chem. 2005 Jun 3;280(22):21680-8. Epub 2005 Apr 6. PMID:15817463 doi:10.1074/jbc.M500752200
23. ↑ LaLonde DP, Grubinger M, Lamarche-Vane N, Turner CE. CdGAP associates with actopaxin to regulate integrin-dependent changes in cell morphology and motility. Curr Biol. 2006 Jul 25;16(14):1375-85. PMID:16860736 doi:S0960-9822(06)01676-9
24. ↑ LaLonde DP, Grubinger M, Lamarche-Vane N, Turner CE. CdGAP associates with actopaxin to regulate integrin-dependent changes in cell morphology and motility. Curr Biol. 2006 Jul 25;16(14):1375-85. PMID:16860736 doi:S0960-9822(06)01676-9
25. ↑ Curtis M, Nikolopoulos SN, Turner CE. Actopaxin is phosphorylated during mitosis and is a substrate for cyclin B1/cdc2 kinase. Biochem J. 2002 Apr 15;363(Pt 2):233-42. PMID:11931650
26. ↑ Clarke DM, Brown MC, LaLonde DP, Turner CE. Phosphorylation of actopaxin regulates cell spreading and migration. J Cell Biol. 2004 Sep 13;166(6):901-12. Epub 2004 Sep 7. PMID:15353548 doi:10.1083/jcb.200404024
27. ↑ Ishibe S, Joly D, Zhu X, Cantley LG. Phosphorylation-dependent paxillin-ERK association mediates hepatocyte growth factor-stimulated epithelial morphogenesis. Mol Cell. 2003 Nov;12(5):1275-85. PMID:14636584
28. ↑ Attwell S, Mills J, Troussard A, Wu C, Dedhar S. Integration of cell attachment, cytoskeletal localization, and signaling by integrin-linked kinase (ILK), CH-ILKBP, and the tumor suppressor PTEN. Mol Biol Cell. 2003 Dec;14(12):4813-25. Epub 2003 Sep 5. PMID:12960424 doi:http://dx.doi.org/10.1091/mbc.E03-05-0308
29. ↑ Clarke DM, Brown MC, LaLonde DP, Turner CE. Phosphorylation of actopaxin regulates cell spreading and migration. J Cell Biol. 2004 Sep 13;166(6):901-12. Epub 2004 Sep 7. PMID:15353548 doi:10.1083/jcb.200404024
30. ↑ Montanez E, Wickstrom SA, Altstatter J, Chu H, Fassler R. Alpha-parvin controls vascular mural cell recruitment to vessel wall by regulating RhoA/ROCK signalling. EMBO J. 2009 Oct 21;28(20):3132-44. Epub 2009 Oct 1. PMID:19798050 doi:10.1038/emboj.2009.295
31. ↑ LaLonde DP, Brown MC, Bouverat BP, Turner CE. Actopaxin interacts with TESK1 to regulate cell spreading on fibronectin. J Biol Chem. 2005 Jun 3;280(22):21680-8. Epub 2005 Apr 6. PMID:15817463 doi:10.1074/jbc.M500752200
32. ↑ LaLonde DP, Grubinger M, Lamarche-Vane N, Turner CE. CdGAP associates with actopaxin to regulate integrin-dependent changes in cell morphology and motility. Curr Biol. 2006 Jul 25;16(14):1375-85. PMID:16860736 doi:S0960-9822(06)01676-9
33. ↑ Yang Y, Guo L, Blattner SM, Mundel P, Kretzler M, Wu C. Formation and phosphorylation of the PINCH-1-integrin linked kinase-alpha-parvin complex are important for regulation of renal glomerular podocyte adhesion, architecture, and survival. J Am Soc Nephrol. 2005 Jul;16(7):1966-76. Epub 2005 May 4. PMID:15872073 doi:10.1681/ASN.2004121112
34. ↑ Attwell S, Mills J, Troussard A, Wu C, Dedhar S. Integration of cell attachment, cytoskeletal localization, and signaling by integrin-linked kinase (ILK), CH-ILKBP, and the tumor suppressor PTEN. Mol Biol Cell. 2003 Dec;14(12):4813-25. Epub 2003 Sep 5. PMID:12960424 doi:http://dx.doi.org/10.1091/mbc.E03-05-0308
35. ↑ Schultz J, Milpetz F, Bork P, Ponting CP. SMART, a simple modular architecture research tool: identification of signaling domains. Proc Natl Acad Sci U S A. 1998 May 26;95(11):5857-64. PMID:9600884
36. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
37. ↑ Espinoza-Fonseca LM. Reconciling binding mechanisms of intrinsically disordered proteins. Biochem Biophys Res Commun. 2009 May 8;382(3):479-82. Epub 2009 Mar 3. PMID:19265676 doi:10.1016/j.bbrc.2009.02.151
38. ↑ Iakoucheva LM, Radivojac P, Brown CJ, O'Connor TR, Sikes JG, Obradovic Z, Dunker AK. The importance of intrinsic disorder for protein phosphorylation. Nucleic Acids Res. 2004 Feb 11;32(3):1037-49. Print 2004. PMID:14960716 doi:10.1093/nar/gkh253
39. ↑ Collins MO, Yu L, Campuzano I, Grant SG, Choudhary JS. Phosphoproteomic analysis of the mouse brain cytosol reveals a predominance of protein phosphorylation in regions of intrinsic sequence disorder. Mol Cell Proteomics. 2008 Jul;7(7):1331-48. Epub 2008 Apr 3. PMID:18388127 doi:10.1074/mcp.M700564-MCP200
40. ↑ Friedberg F. Singlet CH domain containing human multidomain proteins: an inventory. Mol Biol Rep. 2010 Mar;37(3):1531-9. Epub 2009 May 21. PMID:19459066 doi:10.1007/s11033-009-9554-y
41. ↑ Friedberg F. Duplex (or quadruplet) CH domain containing human multidomain proteins: an inventory. Mol Biol Rep. 2010 Apr;37(4):1707-16. Epub 2009 Jun 30. PMID:19565353 doi:10.1007/s11033-009-9589-0
42. ↑ Stradal T, Kranewitter W, Winder SJ, Gimona M. CH domains revisited. FEBS Lett. 1998 Jul 17;431(2):134-7. PMID:9708889
43. ↑ Sjoblom B, Ylanne J, Djinovic-Carugo K. Novel structural insights into F-actin-binding and novel functions of calponin homology domains. Curr Opin Struct Biol. 2008 Dec;18(6):702-8. Epub 2008 Nov 13. PMID:18952167 doi:10.1016/j.sbi.2008.10.003
44. ↑ Gimona M, Djinovic-Carugo K, Kranewitter WJ, Winder SJ. Functional plasticity of CH domains. FEBS Lett. 2002 Feb 20;513(1):98-106. PMID:11911887
45. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
46. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
47. ↑ Wang X, Fukuda K, Byeon IJ, Velyvis A, Wu C, Gronenborn A, Qin J. The structure of alpha-parvin CH2-paxillin LD1 complex reveals a novel modular recognition for focal adhesion assembly. J Biol Chem. 2008 Jul 25;283(30):21113-9. Epub 2008 May 28. PMID:18508764 doi:10.1074/jbc.M801270200
48. ↑ Fukuda K, Gupta S, Chen K, Wu C, Qin J. The pseudoactive site of ILK is essential for its binding to alpha-Parvin and localization to focal adhesions. Mol Cell. 2009 Dec 11;36(5):819-30. PMID:20005845 doi:10.1016/j.molcel.2009.11.028
49. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
50. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
51. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
52. ↑ Lorenz S, Vakonakis I, Lowe ED, Campbell ID, Noble ME, Hoellerer MK. Structural analysis of the interactions between paxillin LD motifs and alpha-parvin. Structure. 2008 Oct 8;16(10):1521-31. PMID:18940607 doi:10.1016/j.str.2008.08.007
53. ↑ Fukuda K, Gupta S, Chen K, Wu C, Qin J. The pseudoactive site of ILK is essential for its binding to alpha-Parvin and localization to focal adhesions. Mol Cell. 2009 Dec 11;36(5):819-30. PMID:20005845 doi:10.1016/j.molcel.2009.11.028
54. ↑ Fukuda K, Gupta S, Chen K, Wu C, Qin J. The pseudoactive site of ILK is essential for its binding to alpha-Parvin and localization to focal adhesions. Mol Cell. 2009 Dec 11;36(5):819-30. PMID:20005845 doi:10.1016/j.molcel.2009.11.028
55. ↑ Wickstrom SA, Lange A, Montanez E, Fassler R. The ILK/PINCH/parvin complex: the kinase is dead, long live the pseudokinase! EMBO J. 2010 Jan 20;29(2):281-91. Epub 2009 Dec 24. PMID:20033063 doi:10.1038/emboj.2009.376