Matrix metalloproteinase: Difference between revisions

From Proteopedia
Jump to navigation Jump to search
← Older edit
Michal Harel (talk | contribs)
31,761 edits
No edit summary
Michal Harel (talk | contribs)
31,761 edits
No edit summary
 
Line 42: Line 42:


</StructureSection>
</StructureSection>
==3D structures of matrix metalloproteinase==
Updated on {{REVISIONDAY2}}-{{MONTHNAME|{{REVISIONMONTH}}}}-{{REVISIONYEAR}}
{{#tree:id=OrganizedByTopic|openlevels=0|
*MMP1 interstitial or fibroblast collagenase
**[[1su3]] – pro-hMMP – human<br />
**[[2clt]] – hMMP (mutant)<br />
**[[3shi]], [[1hfc]], [[1cge]], [[1cgf]] - hMMP catalytic domain<br />
**[[2tcl]], [[966c]], [[1cgl]] - hMMP catalytic domain + inhibitor<br />
**[[2ayk]], [[3ayk]], [[4ayk]], [[1ayk]] - hMMP catalytic domain - NMR<br />
**[[4auo]] - hMMP catalytic domain + collagen peptide<br />
**[[1fbl]] – MMP - pig
*MMP2 gelatinase-A
**[[1qib]], [[1ck7]] - hMMP catalytic domain (mutant) <BR />
**[[1rtg]] - hMMP hemopexin-like domain<BR />
**[[1ks0]] – hMMP first fibronectin type II domain – NMR<BR />
**[[1cxw]] - hMMP second fibronectin type II domain – NMR<BR />
**[[1j7m]] - hMMP third fibronectin type II domain (mutant) – NMR<BR />
**[[1gen]] – hMMP C terminal <br />
**[[1eak]] – pro-hMMP catalytic domain (mutant) + peptide inhibitor<br />
**[[3ayu]] - hMMP catalytic domain (mutant) + peptide inhibitor<br />
**[[1hov]], [[1eub]] - hMMP catalytic domain + inhibitor– NMR<BR />
**[[1gxd]] – pro-hMMP (mutant) + TIMP-2
*MMP3 stromelysin 1
**[[1qia]], [[1qic]], [[1cqr]], [[1slm]] - hMMP catalytic domain<BR />
**[[3ohl]], [[3oho]], [[1g49]], [[1ciz]], [[1b8y]], [[1caq]], [[1usn]], [[2usn]], [[1ums]], [[1umt]],  [[2d1n]], [[2d1o]], [[2ow9]], [[1bqo]], [[1g4k]], [[1b3d]], [[1biw]], [[1c3i]], [[1d5j]], [[1d7x]], [[1d8f]], [[1d8m]], [[1g05]], [[1hfs]], [[1hy7]], [[2srt]], [[4dpe]], [[4g9l]], [[4ja1]], [[5uwn]], [[5uwm]], [[5uwk]], [[5uwl]] - hMMP catalytic domain + inhibitor<br />
**[[1c8t]] - hMMP catalytic domain (mutant) + inhibitor<br />
**[[1uea]] - hMMP catalytic domain + TIMP-1<BR />
**[[1oo9]] - hMMP catalytic domain + TIMP-1 N terminal<BR />
**[[2jt5]], [[2jt6]], [[2jnp]], [[3usn]], [[1sln]], [[1bm6]] - hMMP catalytic domain + inhibitor – NMR<BR />
*MMP7 matrilysin
**[[2y6c]], [[2y6d]], [[2ddy]], [[1mmp]], [[1mmq]], [[1mmr]] – hMMP catalytic domain + inhibitor<br />
**[[2mze]] – hpro-MMP (mutant)  - NMR<br />
**[[2mzh]], [[2mzi]] – hpro-MMP (mutant) + membrane bilayer - NMR<br />
**[[5ue5]], [[5ue2]] – hMMP (mutant) + heparin - NMR<br />
*MMP8 neutrophil collagenase
**[[2oy4]], [[1mnc]], [[1bzs]] - hMMP catalytic domain<br />
**[[3dng]], [[3dpe]], [[3dpf]], [[1zp5]], [[1jh1]], [[1jj9]], [[1i76]], [[1a85]], [[1mmb]], [[1zs0]], [[1zvx]], [[1kbc]], [[3tt4]], [[4qkz]], [[5h8x]]  – hMMP catalytic domain + inhibitor<br />
**[[1i73]], [[2oy2]], [[1jan]], [[1jao]], [[1jap]], [[1jaq]] - hMMP catalytic domain + peptide inhibitor<br />
**[[1a86]] - hMMP catalytic domain + aspartate-based inhibitor
*MMP9 gelatinase-B
**[[1l6j]] - pro-hMMP<BR />
**[[1itv]] – hMMP haemopexin-like domain<br />
**[[1gkc]], [[4xct]], [[4wzv]], [[5cuh]], [[5i12]], [[5ue4]], [[5ue3]], [[5th6]] - hMMP catalytic domain + inhibitor<br />
**[[2ovx]], [[2ovz]], [[2ow0]], [[2ow1]], [[2ow2]], [[1gkd]], [[4h1q]], [[4h82]], [[4hma]], [[4h2e]], [[4h3x]], [[6esm]] - hMMP catalytic domain (mutant) + inhibitor<br />
**[[4jij]], [[4jqg]] - hMMP catalytic domain (mutant) + FRET substrate<br />
**[[5th9]] - hMMP catalytic domain + antibody<br />
*MMP10 stromelysin 2
**[[1q3a]] - hMMP catalytic domain (mutant)<br />
**[[3v96]], [[4ilw]] - hMMP catalytic domain + metalloproteinase inhibitor
*MMP11 stromelysin 3
**[[1hv5]] - hMMP catalytic domain + inhibitor<br />
*MMP12 macrophage metalloelastase
**[[3ba0]], [[2oxu]] - hMMP<BR />
**[[2krj]], [[2k9c]] - hMMP catalytic domain – NMR<BR />
**[[1jk3]], [[1jiz]], [[2oxu]] -  hMMP catalytic domain <BR />
**[[4ijo]] - hMMP catalytic domain (mutant)<br />
**[[2poj]] - hMMP catalytic domain (mutant) - NMR<BR />
**[[2jxy]] - hMMP hemopexin-like domain - NMR<BR />
**[[3n2u]], [[3n2v]], [[2wo8]], [[2wo9]], [[2woa]], [[1utt]], [[1utz]], [[1ros]], [[3rts]], [[3rtt]] – hMMP catalytic domain + inhibitor<br />
**[[3lk8]], [[3lik]], [[3lil]], [[3lir]], [[3ljg]], [[3nx7]], [[3lka]], [[3ehx]], [[3ehy]], [[3f15]], [[3f16]], [[3f17]], [[3f18]], [[3f19]], [[3f1a]], [[1y93]], [[1rmz]], [[1os2]], [[1os9]], [[2hu6]], [[3ts4]], [[3tsk]], [[3uvc]], [[4gql]], [[4gr0]], [[4gr3]], [[4gr8]], [[4h30]], [[4h49]], [[4h76]], [[4h84]], [[4io3]], [[1jk3]],[[4efs]], [[4gql]], [[4gr0]], [[4gr3]], [[4gr8]], [[4guy]], [[4h30]], [[4h49]], [[4h76]], [[4h84]], [[4i03]], [[5cxa]], [[5czm]], [[5d2b]], [[5d3c]], [[5i0l]], [[5i2z]], [[5i3m]], [[5i43]], [[5i4o]], [[5l79]], [[5l7f]], [[5lab]], [[6ekn]], [[6ela]], [[6enm]], [[6eox]], [[5n5k]], [[5n5j]] - hMMP catalytic domain (mutant) + inhibitor<br />
**[[2oxn]], [[2oxz]], [[2oxw]] - hMMP catalytic domain (mutant) + peptide<br />
**[[2n8r]] - hMMP catalytic domain (mutant) + collagen peptide – NMR<br />
**[[2k2g]], [[2z2d]] - hMMP catalytic domain + inhibitor - NMR<BR />
**[[2mlr]], [[2mls]] - hMMP catalytic domain + membrane billayer<br />
**[[2w0d]], [[1ycm]], [[1z3j]] - hMMP catalytic domain (mutant) + inhibitor - NMR<BR />
*MMP13 collagenase 3
**[[1pex]] – hMMP hemopexin-like domain<br />
**[[2yig]], [[3ljz]], [[3kec]], [[3kej]], [[3kek]], [[3kry]], [[3i7g]], [[3i7i]], [[3elm]], [[2pjt]], [[2ozr]], [[1xuc]], [[1xud]], [[1xur]], [[1you]], [[1ztq]], [[3o2x]], [[3zxh]], [[4a7b]], [[1fls]], [[1fm1]], [[456c]], [[830c]], [[3tvc]], [[4jp4]], [[4jpa]], [[3wv1]], [[3wv2]], [[3wv3]], [[4l19]], [[5b5o]], [[5b5p]], [[5bot]], [[5boy]], [[5bpa]] – hMMP catalytic domain + inhibitor<br />
**[[2e2d]] - hMMP catalytic domain + TIMP-2<br />
**[[4fu4]], [[4fvl]], [[4g0d]] - hMMP catalytic domain (mutant) + pro-domain peptide<br />
**[[6hv2]] - hMMP catalytic domain + peptide<br />
**[[1cxv]] - MMP catalytic domain - mouse<BR />
*MMP14 Membrane T1
**[[3ma2]] – hMMP residues 112-292 + TIMP-1 (mutant) <BR />
**[[1buv]], [[1bqq]] residues 112-292 hMMP + TIMP-2<BR />
**[[5h0u]] - hMMP residues 112-292 + polyHis<br />
**[[3c7x]] – hMMP hemopexin domain residues 316-511<br />
**[[6cm1]], [[6clz]] – hMMP hemopexin domain + apolipoprotein<br />
**[[2mqs]] - hMMP + collagen<br />
*MMP16 Membrane T3
**[[1rm8]] - hMMP catalytic domain + inhibitor<br />
*MMP20 enamelysin
**[[2jsd]] - hMMP catalytic domain + inhibitor - NMR<BR />
*MMP23 CA-MMP
**[[2k72]] – hMMP residues 254-290 - NMR<BR />
*MMP adamalysin
**[[1iag]] – MMP – diamondback rattlesnake<br />
**[[3k7l]] - MMP - cobra<br />
}}


==References==
==References==

Latest revision as of 12:08, 29 October 2019


Function

Matrix metalloproteinases (MMP) are Zinc-dependent endopeptidases. MMP degrades extracellular matrix proteins. They are inhibited by proteases called tissue inhibitors of metalloproteinase (TIMP). The pro-MMP contains a pro-peptide which must be removed to render the MMP active[1]. See details in

MMPs are produced by 28 different genes and are classified according to their protein substrates.

  • MMP1 cleaves collagens I, II, III, VII and X.
  • MMP2 cleaves collagen IV and denatured collagen.
  • MMP3 cleaves the core protein of aggrecan and plasminogen activator.
  • MMP7 cleaves proteoglycans, fibronectin, elastin and casein.
  • MMP8 cleaves aggrecan.
  • MMP9 cleaves gelatin. See details in Molecular Playground/MMP9
  • MMP10 cleaves collagens III, IV, V, fibronectin,gelatin and aggrecan.
  • MMP11 cleaves peptides in human tumors.
  • MMP12 cleaves collagens I and III. See details in Matrix Metalloproteinase 12
  • MMP13 cleaves collagen II and laminin-5 γ2.
  • MMP14 is a membrane-type MMP which cleaves aggrecan. See details in Molecular Playground/MMP14
  • MMP16 cleaves collagen III, proteoglycans, fibronectin, gelatin, vitronectin, laminin and α2-macroglobulin.
  • MMP20 cleaves E-cadherin.
  • MMP23 function is unknown.
  • MMP adamalysin is a snake toxin. See details in Atragin

Relevance

MMPs have a role in cancer progression[2]. MMP-2 and MMP-9 secretion is elevated in ovarian cancer and are associated with poor prognosis[3]. MMP-8, MMP-9, MMP-13 and MMP-14 have a role in periodontal diseases[4].

MT1-MMP-TIMP-1 complex

The human matrix metalloproteinases (MMPs) family comprises a large group of structurally homologous zinc-dependent endopeptidases (e.g. (darkmagenta) and (magenta), ) that perform a wide variety of biological roles. In general, the MMPs are inhibited unselectively by all four known tissue inhibitors of metalloproteinases (TIMPs 1-4) which have 40-50% sequence identity. For example, can form complex with (1uea, colored orange). (cyan) is mainly composed of the N-terminal segment that approaches the active site, the AB loop (Thr33-Tyr35), the CD loop (Ala65-Cys70), and the EF loop (Thr97-Ser100). The pivotal residue, threonine 98 (Thr98), is shown as red sticks. In general, (Cys1-Ser68, Val69-Met66, Gly71-Met66, Cys70-Glu67, and Cys70-Thr98) are intimately involved in the conformational stability of TIMP binding interface when bound to MMP.

(darkmagenta) also forms complex with (2j0t, colored orange), producing as well as . This network of hydrogen bonds stabilizes the CD and EF loops that compose the binding interface. Importantly, the . However, this MT1-MMP-WT-TIMP-1 complex is not tight-binding. MT1-MMP is unique since even though it exhibits high structural homology to all MMPs, it is not inhibited by TIMP-1, (1bqq). (mutant TIMP-1 is colored in yellow with T98L shown in red) transformed TIMP-1 into a high affinity inhibitor of MT1-MMP (3ma2). WT-TIMP-1, WT-TIMP-2, and TIMP-1 T98L mutant have kinetic dissociation binding constant (KD) 1.53 x 10-6, 5.61 x 10-8, and 8.70 x 10-8, respectively. So, KD of WT-TIMP-2 is 2 orders of magnitude smaller than that of WT-TIMP-1, indicating the weak affinity between MT1-MMP and WT-TIMP-1. The TIMP-1 T98L mutant regained high-affinity binding to MT1-MMP, resulting in a 2 order of magnitude decrease in KD, similar to the case for WT-TIMP-2, the in vivo inhibitor of MT1-MMP. The overall structures of the complexes of MT1-MMP-WT-TIMP-1 and MT1-MMP-mutant-T98L-TIMP-1 are . Even the structure of MT3-MMP-WT-TIMP-1 is (with wild-type and TIMP-1 T98L mutant). , which is situated near the MT1-MMP . So, this T98L replacement may stabilize the entire area by establishing a strong hydrophobic core upon binding to the enzyme. However, it seems unlikely that these additional bonds could account for the entire binding effect between MT1-MMP and TIMP-1. Statistical analysis of the stabilities in the TIMP-1 T98L mutant reveals that the hydrogen bonds network in mutant form is significantly more stable than that in WT-TIMP-1. Mutations that enhance hydrogen bond stability contribute to the stability of the bound-like, less flexible, conformation of TIMP-1, which eventually results in increasing binding affinity for MT1-MMP. Thus, mutation affected the instrinsic dynamics of the inhibitor rather than its structure, thereby facilitating the interaction [5].

3D structures of matrix metalloproteinase

Matrix metalloproteinase 3D structures


Complex of MMP14 (magenta) and TIMP-1 (orange) with Ca+2 (green) and Zn+2 (grey) ions (PDB code 3ma2)

Drag the structure with the mouse to rotate

ReferencesReferences

  1. Nagase H, Woessner JF Jr. Matrix metalloproteinases. J Biol Chem. 1999 Jul 30;274(31):21491-4. PMID:10419448
  2. Gialeli C, Theocharis AD, Karamanos NK. Roles of matrix metalloproteinases in cancer progression and their pharmacological targeting. FEBS J. 2011 Jan;278(1):16-27. doi: 10.1111/j.1742-4658.2010.07919.x. Epub 2010, Nov 19. PMID:21087457 doi:http://dx.doi.org/10.1111/j.1742-4658.2010.07919.x
  3. Roomi MW, Monterrey JC, Kalinovsky T, Rath M, Niedzwiecki A. Patterns of MMP-2 and MMP-9 expression in human cancer cell lines. Oncol Rep. 2009 May;21(5):1323-33. PMID:19360311
  4. Birkedal-Hansen H. Role of matrix metalloproteinases in human periodontal diseases. J Periodontol. 1993 May;64(5 Suppl):474-84. PMID:8315570 doi:http://dx.doi.org/10.1902/jop.1993.64.5s.474
  5. Grossman M, Tworowski D, Dym O, Lee MH, Levy Y, Murphy G, Sagi I. Intrinsic protein flexibility of endogenous protease inhibitor TIMP-1 controls its binding interface and effects its function. Biochemistry. 2010 Jun 14. PMID:20545310 doi:10.1021/bi902141x

Proteopedia Page Contributors and Editors (what is this?)Proteopedia Page Contributors and Editors (what is this?)

Michal Harel, Alexander Berchansky
Retrieved from "https://proteopedia.openfox.io/wiki/index.php?title=Matrix_metalloproteinase&oldid=3102098"