Tyrosine kinase

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Current revision

Human Fyn tyrosine kinase kinase domain with phosphotyrosine in stick model complex with inhibitor staurosporine (PDB code 2dq7).

Drag the structure with the mouse to rotate

1 Function
2 Relevance
3 Disease
4 Structural highlights
5 Traditional Chinese medicine as dual guardians against hypertension and cancer? ^[11]
6 3D structures of tyrosine kinase
7 References

Function

Tyrosine kinase (TK) transfers a phosphate group from ATP to tyrosine residues of proteins^[1]. TKs are classified as receptor-TK which are membrane-attached and cytoplasmic non-receptor TKs. Staurosporine inhibits TK and prevents ATP binding to it.
For Abelson tyrosine kinase see:

Bcr-Abl and Imatinib (STI571 or Gleevec)
Imatinib (Gleevec)
Dasatinib (Sprycel)
Nilotinib (Tasigna)

For Bruton's tyrosine kinase see:

Ibrutinib (Imbruvica)

For Src tyrosine kinase^[2] see:

For Kit tyrosine kinase (or SCF or stem cell factor) see:

SCF-KIT

For Tyk tyrosine kinase see:

Student Project 5 for UMass Chemistry 423 Spring 2015
Ephrin receptors belong to the receptor tyrosine kinases.

For Focal adhesion kinase see:

Focal adhesion kinase
Csk tyrosine kinase (or C-terminal Src kinase) has a role in regulating apoptosis, survival, proliferation^[3].
Fgr tyrosine kinase has a role in regulating diet-induced obesity, insulin resistance and liver steatosis^[4].
Syk tyrosine kinase (or spleen tyrosine kinase) has a role in adaptive immun receptor signalling^[5].
Mer tyrosine kinase has a role in macrophage physiology like regulating cytokine secretion and clearance of apoptotic cells^[6].
Hck tyrosine kinase activates kinase-dependent and caspase-mediated apoptosis^[7].

Relevance

Bcr-Abl inhibitors are used against chronic myelogenous leukemia (CLM)^[8].

Disease

Mutated TK can cause unregulated growth of the cell and their inhibitors can be effective cancer treatment^[9].

Structural highlights

TK contains, starting from the N-terminal, SH4 – a membrane attachment domain; SH3 and SH2 domains which are a sequence-specific phosphotyrosine binding domains with roles in protein-protein interactions and the SH1 catalytic kinase domain. The of Fyn TK which contains a , in the ^[10].

Traditional Chinese medicine as dual guardians against hypertension and cancer? ^[11]

functions as a signal protein and is implicated in various diseases. The carboxyl terminal of Src kinase is important in regulating conformation and activity of Src. Src protein is locked as an inward folding conformation through binding between the phosphorylated Tyr527 and the SH2 domain under normal inactive conditions. Src is activated when dephosphorylation of Tyr527 and phosphorylation of Tyr419 occurs. From N-terminal to C-terminal, Src is composed of a (residues 270–340; colored in violet) which binds adenosine triphosphate (ATP) and a (residues 345–523; colored in green) which binds with substrates. The ATP binding site is also partially located in the larger lobe. By regulating the alpha-helix structure, the large lobe can move toward or away from the small lobe, opening or closing the cleft between the two lobes. The Src catalytic site is located within the cleft. An open conformation allows the entrance of ATP into the cleft and exit of adenosine diphosphate (ADP) from the cleft. Drugs that can either interact with the residues (404–432) on the activation loop or inhibit the activation loop from moving away and opening the cleft as a result of Tyr419 phosphorylation can effectively inhibit Src activity. In this in vivo study, and have multiple stable interactions with the two Src cleft loops while simultaneously interacting with Asp407, hindering the activation loop from activation. Considering the aforementioned interactions with Src and high afﬁnity with EGFR, HER2, and HSP90, we suggest that Angeliferulate and HMID which both originate from the TCM Angelica sinensis may have potential as multi-targeting drug leads.

3D structures of tyrosine kinase

Tyrosine kinase 3D structures

References

↑ Hubbard SR, Till JH. Protein tyrosine kinase structure and function. Annu Rev Biochem. 2000;69:373-98. PMID:10966463 doi:http://dx.doi.org/10.1146/annurev.biochem.69.1.373
↑ Roskoski R Jr. Src protein-tyrosine kinase structure and regulation. Biochem Biophys Res Commun. 2004 Nov 26;324(4):1155-64. PMID:15504335 doi:http://dx.doi.org/10.1016/j.bbrc.2004.09.171
↑ Fortner A, Chera A, Tanca A, Bucur O. Apoptosis regulation by the tyrosine-protein kinase CSK. Front Cell Dev Biol. 2022 Dec 12;10:1078180. PMID:36578781 doi:10.3389/fcell.2022.1078180
↑ Acín-Pérez R, Iborra S, Martí-Mateos Y, Cook ECL, Conde-Garrosa R, Petcherski A, Muñoz MDM, Martínez de Mena R, Krishnan KC, Jiménez C, Bolaños JP, Laakso M, Lusis AJ, Shirihai OS, Sancho D, Enríquez JA. Fgr kinase is required for proinflammatory macrophage activation during diet-induced obesity. Nat Metab. 2020 Sep;2(9):974-988. PMID:32943786 doi:10.1038/s42255-020-00273-8
↑ Mócsai A, Ruland J, Tybulewicz VL. The SYK tyrosine kinase: a crucial player in diverse biological functions. Nat Rev Immunol. 2010 Jun;10(6):387-402. PMID:20467426 doi:10.1038/nri2765
↑ Anwar A, Keating AK, Joung D, Sather S, Kim GK, Sawczyn KK, Brandão L, Henson PM, Graham DK. Mer tyrosine kinase (MerTK) promotes macrophage survival following exposure to oxidative stress. J Leukoc Biol. 2009 Jul;86(1):73-9. PMID:19386698 doi:10.1189/jlb.0608334
↑ Shivakrupa R, Radha V, Sudhakar Ch, Swarup G. Physical and functional interaction between Hck tyrosine kinase and guanine nucleotide exchange factor C3G results in apoptosis, which is independent of C3G catalytic domain. J Biol Chem. 2003 Dec 26;278(52):52188-94. PMID:14551197 doi:10.1074/jbc.M310656200
↑ Tolomeo M, Dieli F, Gebbia N, Simoni D. Tyrosine kinase inhibitors for the treatment of chronic myeloid leukemia. Anticancer Agents Med Chem. 2009 Oct;9(8):853-63. PMID:19538165
↑ Lengyel E, Sawada K, Salgia R. Tyrosine kinase mutations in human cancer. Curr Mol Med. 2007 Feb;7(1):77-84. PMID:17311534
↑ Kinoshita T, Matsubara M, Ishiguro H, Okita K, Tada T. Structure of human Fyn kinase domain complexed with staurosporine. Biochem Biophys Res Commun. 2006 Aug 4;346(3):840-4. Epub 2006 Jun 13. PMID:16782058 doi:10.1016/j.bbrc.2006.05.212
↑ Tou WI, Chen CY. Traditional Chinese medicine as dual guardians against hypertension and cancer? J Biomol Struct Dyn. 2012 Jul;30(3):299-317. Epub 2012 Jun 12. PMID:22694277 doi:10.1080/07391102.2012.680030

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Tyrosine kinase

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Contents

Function

Relevance

Disease

Structural highlights

Traditional Chinese medicine as dual guardians against hypertension and cancer? ^[11]

3D structures of tyrosine kinase

References

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@@ Line 3: / Line 3: @@
 ==Function==
-'''Tyrosine kinase''' (TK) transfers a phosphate group from ATP to tyrosine residues of proteins<ref>PMID:10966463</ref>.   TKs are classified as receptor-TK which are membrane-attached and cytoplasmic non-receptor TKs.  Staurosporine inhibits TK and prevents ATP binding to it.<br />
+'''Tyrosine kinase''' (TK) transfers a phosphate group from ATP to tyrosine residues of proteins<ref>PMID:10966463</ref>.  TKs are classified as [[Receptor tyrosine kinases|receptor-TK]] which are membrane-attached and cytoplasmic non-receptor TKs.  Staurosporine inhibits TK and prevents ATP binding to it.<br />
 For '''Abelson tyrosine kinase''' see:<br />
 *[[Bcr-Abl and Imatinib (STI571 or Gleevec)]]<br />
@@ Line 9: / Line 9: @@
 *[[Dasatinib]] (Sprycel)<br />
 *[[Nilotinib]] (Tasigna)<br />
+For '''Bruton's tyrosine kinase''' see:<br />
+*[[Ibrutinib]] (Imbruvica)<br />
 For '''Src tyrosine kinase'''<ref>PMID:15504335</ref> see:<br />
 *[[SRC]]<br />
@@ Line 15: / Line 17: @@
 For '''Tyk tyrosine kinase''' see:<br />
 *[[Student Project 5 for UMass Chemistry 423 Spring 2015]]<br />
-See also
+*[[Ephrin receptor|Ephrin receptors]] belong to the receptor tyrosine kinases.
+For '''Focal adhesion kinase''' see:<br />
+*[[Focal adhesion kinase]]
+*'''Csk tyrosine kinase''' (or C-terminal Src kinase) has a role in regulating apoptosis, survival, proliferation<ref>PMID:36578781</ref>.
+*'''Fgr tyrosine kinase'''  has a role in regulating diet-induced obesity, insulin resistance and liver steatosis<ref>PMID:32943786</ref>.
+*'''Syk tyrosine kinase''' (or spleen tyrosine kinase) has a role in adaptive immun receptor signalling<ref>PMID:20467426</ref>.
+*'''Mer tyrosine kinase'''  has a role in macrophage physiology like regulating cytokine secretion and clearance of apoptotic cells<ref>PMID:19386698</ref>.
+*'''Hck tyrosine kinase''' activates kinase-dependent and caspase-mediated apoptosis<ref>PMID:14551197</ref>.
+See also
 *[[Proto-oncogene tyrosine-protein kinase]]<br />
 *[[Tyrosine Kinase Inhibitor Pharmacokinetics]]<br />
-*[[Oncogenes & Tumor Suppressor Genes]].
+*[[Treatments:TYKI References]]<br />
+*[[Oncogenes & Tumor Suppressor Genes]]
+*[[Cancer]]
+*[[Ephrin Type-A Receptor]]
 For references see [[Treatments:TYKI References]].
@@ Line 30: / Line 44: @@
 == Structural highlights ==
-TK contains, starting from the N-terminal, SH4 – a membrane attachment domain; SH3 and SH2 domains which are a sequence-specific phosphotyrosine binding domains with roles in protein-protein interactions and the SH1 catalytic kinase domain.  The <scene name='48/483859/Cv/3'>staurosporine inhibitor binds the kinase domain</scene> of Fyn TK which contains a <scene name='48/483859/Cv/4'>phosphotyrosine</scene>, in the <scene name='48/483859/Cv/5'>groove between the N- and C-lobes</scene><ref>PMID:16782058</ref>.
+TK contains, starting from the N-terminal, SH4 – a membrane attachment domain; SH3 and SH2 domains which are a sequence-specific phosphotyrosine binding domains with roles in protein-protein interactions and the SH1 catalytic kinase domain.  The <scene name='48/483859/Cv/6'>staurosporine inhibitor binds the kinase domain</scene> of Fyn TK which contains a <scene name='48/483859/Cv/7'>phosphotyrosine</scene>, in the <scene name='48/483859/Cv/8'>groove between the N- and C-lobes</scene><ref>PMID:16782058</ref>.
 ==Traditional Chinese medicine as dual guardians against hypertension and cancer? <ref>DOI 10.1080/07391102.2012.680030</ref> ==
@@ Line 37: / Line 51: @@
 	From N-terminal to C-terminal, Src is composed of a <scene name='Journal:JBSD:14/Cv/3'>smaller amino-terminal lobe</scene> (<span style="color:violet;background-color:black;font-weight:bold;">residues 270–340; colored in violet</span>) which binds adenosine triphosphate (ATP) and a <scene name='Journal:JBSD:14/Cv/5'>larger carboxyl-terminal lobe</scene> (<span style="color:lime;background-color:black;font-weight:bold;">residues 345–523; colored in green</span>) which binds with substrates. The ATP binding site is also partially located in the larger lobe. By regulating the alpha-helix structure, the large lobe can move toward or away from the small lobe, opening or closing the cleft between the two lobes. The Src catalytic site is located within the cleft. An open conformation allows the entrance of ATP into the cleft and exit of adenosine diphosphate (ADP) from the cleft. Drugs that can either interact with the residues (404–432) on the activation loop or inhibit the activation loop from moving away and opening the cleft as a result of Tyr419 phosphorylation can effectively inhibit Src activity.
 	In this ''in vivo'' study, <scene name='Journal:JBSD:14/Cv/7'>Angeliferulate</scene> and <scene name='Journal:JBSD:14/Cv/8'>HMID</scene> have multiple stable interactions with the two Src cleft loops while simultaneously interacting with Asp407, hindering the activation loop from activation. Considering the aforementioned interactions with Src and high af&#64257;nity with EGFR, HER2, and HSP90, we suggest that Angeliferulate and HMID which both originate from the TCM ''Angelica sinensis'' may have potential as multi-targeting drug leads.
-</StructureSection>
 ==3D structures of tyrosine kinase==
+[[Tyrosine kinase 3D structures]]
-Updated on {{REVISIONDAY2}}-{{MONTHNAME|{{REVISIONMONTH}}}}-{{REVISIONYEAR}}
+==References==
-{{#tree:id=OrganizedByTopic|openlevels=0|
-*'''NON-RECEPTOR TYROSINE KINASES - nRTK'''
-*'''Fyn tyrosine kinase''' (Domains: SH3 80-141; SH2 142-247; kinase 260-537)
-**[[1shf]], [[3ua6]] – hTK Fyn SH3 domain – human<br />
-**[[3h0f]], [[3h0h]], [[3h0i]], [[3cqt]] - hTK Fyn SH3 domain (mutant)<br />
-**[[2l2p]], [[2lp5]] - cTK Fyn SH3 domain (mutant)- chicken - NMR<br />
-**[[3uf4]] – mTK Fyn SH3-SH2 domain – mouse<br />
-**[[1zbj]] - hTK Fyn SH3 domain – NMR<br />
-**[[1g83]] - hTK Fyn SH2+SH3 domains (mutant)<br />
-*Fyn complex
-**[[1fyn]], [[4znx]] - hTK Fyn SH3 domain + peptide<br />
-**[[1nyf]], [[1nyg]] - hTK Fyn SH3 domain + peptide – NMR<br />
-**[[1efn]], [[1avz]] - hTK Fyn SH3 domain + HIV Nef protein<br />
-**[[1m27]] - hTK Fyn SH3 domain + SH2 domain protein 1A + SLAM peptide<br />
-**[[4d8d]] - hTK Fyn SH3 domain (mutant) + HIV Nef protein<br />
-**[[3ua7]] – hTK Fyn SH3 domain + hepatitis virus peptide<br />
-**[[4eik]] - hTK Fyn SH3 domain + VSL12 peptide<br />
-**[[1aot]], [[1aou]] - hTK Fyn SH2 domain + phosphopeptide - NMR<BR />
-**[[2dq7]] – hTK kinase domain + staurosporine<br />
-*'''Abelson tyrosine kinase'''
-*Abl1 SH2 domain residues 120-220
-**[[1ab2]] - hTK SH2 domain – NMR<BR />
-**[[3uyo]], [[3t04]], [[3k2m]], [[5dc4]], [[5dc9]] - hTK SH2 domain + monobody <br />
-*Abl1 SH3 domain residues 60-121
-**[[5oaz]] - hTK SH3 domain <br />
-**[[1ju5]] - hTK SH3 domain (mutant) + CRK SH2 domain + phosphopeptide - NMR<br />
-**[[1awo]] - hTK SH3 domain + phosphopeptide – NMR<BR />
-**[[1bbz]] - hTK SH3 domain + peptide<br />
-**[[2o88]] - hTK SH3 domain (mutant} + peptide<br />
-**[[1abo]] - mTK SH3 domain + peptide<br />
-**[[1abq]] - mTK SH3 domain <br />
-**[[4jjb]], [[4jjc]], [[4jjd]] - hTK abl SH3 domain <br />
-**[[4j9b]], [[3egu]], [[3eg2]], [[3eg3]], [[3eg0]], [[3eg1]] - hTK abl SH3 domain (mutant)<br />
-**[[4j9c]], [[4j9e]], [[4j9i]] - hTK abl SH3 domain (mutant) + p17 peptide<br />
-**[[4j9d]], [[4j9f]] - hTK abl SH3 domain (mutant) + p0 peptide<br />
-**[[4j9g]], [[4j9h]] - hTK abl SH3 domain (mutant) + p7 peptide<br />
-*Abl1 SH3-SH2 domain residues 57-218
-**[[2abl]] - hTK SH3-SH2 domain<br />
-**[[2fo0]] - hTK SH3-SH2 domain (mutant)<br />
-*Abl1 regultory module residues 1-255
-**[[6amv]], [[6amw]] - hTK <br />
-*Abl1 kinase domain residues 229-512
-**[[6bl8]] - hTK kinase domain<br />
-**[[2g2h]] - hTK kinase domain (mutant)<br />
-**[[1opj]], [[1opk]] - mTK kinase domain <br />
-**[[2g1t]] - hTK kinase domain + peptide<br />
-**[[2g2i]], [[2g2f]] - hTK kinase domain (mutant) + peptide<br />
-**[[3ue4]], [[3cs9]], [[2hzi]], [[2hz4]], [[2hz0]], [[2hyy]], [[2gqg]], [[4wa9]] - hTK kinase domain + cancer drug<br />
-**[[2f4j]], [[4twp]] - hTK kinase domain (mutant) + cancer drug<br />
-**[[3qrk]], [[3qri]], [[3qrj]], [[2v7a]], [[2e2b]], [[2hiw]], [[4zog]], [[5hu9]], [[4yc8]] - hTK kinase domain + inhibitor<br />
-**[[1fpu]], [[1m52]], [[2qoh]], [[3kf4]], [[3kfa]] - mTK kinase domain + inhibitor<br />
-**[[2z60]], [[3dk3]], [[3dk6]], [[3dk7]] - mTK kinase domain (mutant) + inhibitor<br />
-**[[1iep]], [[2hzn]], [[3k5v]], [[3ms9]], [[3mss]], [[3oxz]], [[6hd6]] - mTK kinase domain + cancer drug<br />
-**[[3ik3]], [[3oy3]] - mTK kinase domain (mutant) + cancer drug<br />
-*Abl1 SH2-kinase domain residues 119-531
-**[[4xey]] - hTK SH2-kinase domain  <br />
-*Abl1 SH3-SH2-kinase domain residues 1-531
-**[[1opl]] - hTK SH3-SH2-kinase domain (mutant} <br />
-*Abl1 F-actin binding domain residues 1007-1130
-**[[1zzp]] - hTK abl F-actin binding domain – NMR <br />
-*Abl2 SH2 domain residues 165-273
-**[[4eih]] - hTK SH2 domain <BR />
-**[[2ecd]] - hTK SH2 domain – NMR<BR />
-*Abl2 kinase domain residues 279-546
-**[[3gvu]] - hTK kinase domain + Gleevec<br />
-**[[3hmi]] - hTK kinase domain + inhibitor<br />
-**[[2xyn]] - hTK kinase domain + cancer drug<br />
-*Abl2 C-terminal residues 1058-1182
-**[[2kk1]] – hTK C terminal – NMR<BR />
-*'''Anaplastic lymphoma kinase (Alk)'''
-**[[4tt7]] - hTK kinase domain<br />
-**[[3l9p]], [[3lcs]], [[3lct]], [[2yhv]], [[2yjr]], [[2yjs]], [[4fnw]], [[4fnx]], [[4anl]] - hTK kinase domain (mutant)<br />
-**[[2xb7]], [[2xba]], [[3aox]], [[5imx]], [[5kz0]] - hTK kinase domain + inhibitor<br />
-**[[4dce]], [[4fob]], [[4foc]], [[4fod]], [[4fny]], [[4fnz]], [[4joa]], [[4mkc]], [[4z55]], [[5iug]], [[5iuh]], [[5iui]] - hTK kinase domain (mutant) + inhibitor<br />
-**[[2xp2]], [[5j7h]], [[5fto]], [[5ftq]] - hTK kinase domain + cancer drug<br />
-**[[2yfx]], [[4anq]], [[4ans]], [[5aaa]], [[5aab]], [[5aac]], [[5a9u]], [[5aa8]], [[5aa9]] - hTK kinase domain (mutant) + cancer drug<br />
-*'''Csk tyrosine kinase'''
-**[[3eac]] - hTK SH2 domain<br />
-**[[3eaz]] - hTK SH2 domain (mutant)<br />
-**[[2rsy]] - hTK SH2 domain + CBP phosphopeptide - NMR<br />
-**[[1csk]] - hTK SH3 domain<br />
-**[[1jeg]] - hTK SH3 domain + tyrosine phosphatase peptide - NMR<br />
-**[[1byg]] - hTK kinase domain + staurosporine<br />
-**[[3d7t]], [[3d7u]] - hTK kinase domain (mutant) + C-Src<br />
-**[[1k9a]] - TK C terminal - rat<br />
-*'''Jak tyrosine kinase''' see [[Janus kinase]]
-*'''p55-blk tyrosine kinase'''
-**[[1blj]], [[1blk]] - mTK p55-blk SH2 domain – NMR<BR />
-* '''Src tyrosine kinase''' (Domains: SH3 85-140; SH2 140-251; kinase 253-535)
-*Src tyrosine kinase SH2 domain
-**[[3eac]] - hTK  <br />
-**[[4f59]], [[3eaz]] - hTK  (mutant) <br />
-**[[1f2f]] - cTK  (mutant) <br />
-**[[1spr]] - RsvTK  + phosphate – Rous sarcoma virus<br />
-**[[2jyq]] – RsvTK – NMR<br />
-**[[1kc2]], [[1sps]], [[1is0]], [[1nzl]], [[1nzv]] - RsvTK  + peptide<br />
-**[[1sha]], [[1shb]] - RsvTK  + phosphopeptide<br  />
-**[[1shd]] - cTK  + TRKA receptor<br />
-**[[4f5b]] - hTK  (mutant) + phosphotyrosine<br />
-**[[4f5a]] - hTK  (mutant) + phosphate<br />
-**[[1o4c]] - hTK  + phosphate<br />
-**[[1o41]], [[1o42]], [[1o43]], [[1o44]], [[1o45]], [[1o46]], [[1o47]], [[1o48]], [[1o49]], [[1o4a]], [[1o4b]], [[1o4d]], [[1o4e]], [[1o4f]], [[1o4g]], [[1o4h]], [[1o4i]], [[1o4j]], [[1o4k]], [[1o4l]], [[1o4m]], [[1o4n]], [[1o4o]], [[1o4p]], [[1o4q]], [[1o4r]] - hTK + inhibitor<br />
-**[[1hcs]], [[1hct]] - hTK  + peptide - NMR<br />
-**[[1a07]], [[1a08]], [[1a09]], [[1a1a]], [[1a1b]], [[1a1c]], [[1a1e]] - hTK  + peptide <br />
-**[[1f1w]] - cTK  (mutant) + peptide<br />
-**[[1p13]] - cTK  + peptide<br />
-**[[1qwe]], [[1qwf]] - RsvTK  + peptide<br />
-*Src tyrosine kinase SH3 domain
-**[[1srl]], [[1srm]] - cTK – NMR<br />
-**[[3fj5]], [[4jz3]], [[4jz4]] - cTK<br />
-**[[4le9]], [[4oml]], [[4omm]], [[4omn]], [[4omo]], [[4omp]], [[4omq]], [[5i11]], [[4rtu]], [[4rtx]] - cTK (mutant) <br />
-**[[4y92]] - TK (mutant) Avian sarcoma virus<br />
-**[[4hxj]], [[1prl]], [[4qt7]], [[4rty]], [[4rtz]] - cTK + peptide<br />
-**[[1prm]], [[1rlp]], [[1rlq]], [[1nlo]], [[1nlp]] - cTK + peptide - NMR<br />
-**[[4hvu]], [[4hvv]], [[4hvw]], [[4rtv]], [[4rtw]], [[5ob2]], [[5ob1]], [[5ob0]], [[5oav]] - cTK (mutant) + peptide<br />
-**[[1jeg]] – TK + protein-tyrosine phosphatase peptide – mouse<br />
-*Src tyrosine kinase kinase domain residues 253-535
-**[[3of0]], [[2qi8]] - cTK (mutant) <br />
-**[[1yo6]] - hTK <br />
-**[[1yoj]] - hTK (mutant) <br />
-**[[3tz7]], [[3tz8]], [[3tz9]], [[4dgg]] – cTK (mutant) + pyrazolin derivative<br />
-**[[4fic]], [[3uqg]], [[3uqf]], [[3u51]], [[3u4w]], [[4agw]], [[3qlg]], [[3qlf]], [[3g6g]], [[3el8]], [[3f6x]], [[2hwo]], [[2hwp]], [[2oiq]], [[3en4]], [[3en5]], [[3en6]], [[3en7]], [[3el7]], [[5bmm]], [[5j5s]], [[4ybj]], [[4ybk]], [[5xp7]] – cTK + inhibitor<br />
-**[[4lgg]], [[4lgh]], [[3svv]], [[3oez]], [[3lok]], [[3g5d]], [[3f3w]], [[3f3v]], [[3geq]], [[3g6h]], [[3f3t]], [[3f3u]], [[2qlq]], [[2qq7]], [[4lgg]], [[4lgh]], [[4mcv]], [[4o2p]], [[5teh]], [[5t0p]], [[5sys]], [[5swh]] – cTK (mutant) + inhibitor<br />
-**[[4u5j]] – cTK (mutant) + cancer drug<br />
-**[[1yol]], [[1yom]] – hTK (mutant) + inhibitor<br />
-**[[2bdf]], [[2bdj]] – hTK + inhibitor<br />
-**[[1byg]] – hTK + staurosporine<br />
-**[[4mxo]] – hTK + cancer drug<br />
-**[[4mxx]], [[4mxy]], [[4mxz]] – hTK (mutant) + cancer drug<br />
-**[[3d7t]], [[3d7u]] – cTK + Csk<br />
-**[[3dqw]], [[3dqx]] - cTK (mutant) + ATP<br />
-*Src tyrosine kinase C terminal domain
-**[[1k9a]] – rTK – rat<br />
-*Src tyrosine kinase SH2+SH3+kinase domains residues 85-535
-**[[1ksw]] – hTK (mutant)+ ADP derivative<br />
-**[[1y57]] – hTK + inhibitor<br />
-**[[4k11]] – hTK (mutant) + inhibitor<br />
-**[[6f3f]] – mTK + ADP <br />
-*Src tyrosine kinase SH2+SH3+kinase+C terminal domains
-**[[1fmk]] – hTK  <br />
-**[[2ptk]] – cTK <br />
-**[[2src]] – hTK + AMPPNP<br />
-*Src tyrosine kinase N terminal+SH2+SH3+kinase domains
-**[[2h8h]] – hTK + inhibitor<br />
-*'''Lymphocyte-specific tyrosine kinase Lck''' (Domains: SH3 58-118; SH2 122-225; kinase 230-500)
-**[[1kik]], [[1h92]] - hTK Lck SH3 domain – NMR<BR />
-**[[2iim]] - hTK Lck SH3 domain<br />
-**[[4d8k]], [[1x27]] - hTK Lck SH3-SH2 domain<br />
-**[[3lck]] - hTK Lck kinase domain<br />
-*Lck complex
-**[[1lcj]], [[1lkk]], [[1lkl]] - hTK Lck SH2 domain (mutant) + phosphopeptide<br />
-**[[1cwd]], [[1cwe]], [[1ijr]] - hTK Lck SH2 domain + phosphopeptide<br />
-**[[1bhf]] - hTK Lck SH2 domain + peptide inhibitor<br />
-**[[1fbz]] - hTK Lck SH2 domain + inhibitor<br />
-**[[1bhh]] - hTK Lck SH2 domain + T-lymphocyte-specific TK<br />
-**[[5mtm]], [[5mtn]] - hTK Lck SH2 domain + monobody<br />
-**[[1lck]] - hTK Lck SH3-SH2 domain (mutant) + phosphopeptide<br />
-**[[1x27]] - hTK Lck SH3-SH2 domain + peptide<br />
-**[[1qpj]] - hTK Lck kinase domain + staurosporin<br />
-**[[2of2]], [[2of4]], [[2ofu]], [[2ofv]], [[2og8]], [[3b2w]], [[3bym]], [[3bys]], [[3byu]], [[2zm1]], [[2zm4]], [[3byo]], [[2zyb]], [[3ac1]], [[3ac2]], [[3ac3]], [[3ac4]], [[3ac5]], [[3ac8]], [[3acj]], [[3ack]], [[3kmm]], [[3ad4]], [[3ad5]], [[3ad6]], [[1qpc]], [[1qpd]], [[1qpe]] - hTK Lck kinase domain + inhibitor<br />
-**[[3mpm]] - hTK Lck kinase domain (mutant) + inhibitor<br />
-**[[4c3f]] - hTK Lck kinase domain (mutant) + chemotype<br />
-**[[2pl0]] - hTK Lck kinase domain + imatinib<br />
-**[[3kxz]] - hTK Lck kinase domain + probe molecule<br />
-**[[1q68]] - hTK Lck residues 6-34 (mutant) + CD4 peptide – NMR<br />
-**[[1q69]] - hTK Lck residues 6-34 (mutant) + CD8 – NMR<br />
-*'''Syk - spleen tyrosine kinase'''
-**[[1xba]], [[4xg2]] – Syk kinase domain
-*Syk complex
-**[[1xbb]] - Syk kinase domain + Gleevec<br />
-**[[1xbc]] - Syk kinase domain + staurosporine<br />
-**[[3emg]], [[3fqe]], [[3fqh]], [[3fqs]], [[3srv]], [[4dfl]], [[4dfn]], [[3vf8]], [[3vf9]], [[3tub]], [[3tuc]], [[3tud]], [[4f4p]], [[4fyn]], [[4fyo]], [[4fz6]], [[4fz7]], [[4gfg]], [[4i0r]], [[4i0s]], [[4i0t]], [[4puz]], [[4pv0]], [[4rx7]], [[4rx8]], [[4rx9]], [[5lma]], [[5lmb]], [[5ghv]], [[4wnm]], [[4xg3]], [[4xg4]], [[4xg6]], [[4xg7]], [[4xg8]], [[4xg9]], [[4rss]], [[4yjv]], [[5c26]], [[5c27]], [[4yjo]], [[4yjp]], [[4yjq]], [[4yjr]], [[4yjs]], [[4yjt]], [[4yju]], [[5tr6]], [[5tt7]], [[5tiu]], [[5t68]], [[5y5t]], [[5y5u]] - Syk kinase domain + inhibitor<br />
-**[[4px6]] - Syk kinase domain (mutant) + inhibitor<br />
-**[[1csy]], [[1csz]] - Syk SH2 domain + phosphopeptide – NMR<BR />
-**[[4fl1]], [[4fl2]] - Syk kinase domain + ANP<br />
-**[[4fl3]] - Syk kinase domain (mutant) + ANP<br />
-**[[1a81]] – Syk tandem SH2 domain + T-cell surface peptide <br />
-*'''Itk/Tsk tyrosine kinase'''
-**[[1lui]], [[1luk]], [[1lum]], [[1lun]] – mTK Itk SH2 domain – NMR<BR />
-**[[3s9k]] – mTK Itk SH2 domain <BR />
-**[[2etz]], [[2eu0]] – hTK Itk SH2 domain + phosphopeptide – NMR<BR />
-**[[1awj]], [[2rn8]], [[2rna]] – mTK Itk SH3 domain – NMR<BR />
-**[[2yuq]], [[2lmj]] – hTK Itk SH3 domain – NMR<BR />
-**[[2k79]], [[2k7a]] – mTK Itk SH2+SH3 domains – NMR<BR />
-**[[1sm2]], [[1snu]], [[1snx]] – hTK Itk kinase domain <BR />
-**[[3miy]] – hTK Itk kinase domain + cancer drug<BR />
-**[[3v5j]], [[3v5l]], [[3v8t]], [[3v8w]] – hTK Itk kinase domain + inhibitor<BR />
-**[[3mj1]], [[3mj2]], [[3qgw]], [[3qgy]], [[4hct]], [[4hcu]], [[4hcv]], [[4kio]] – hTK Itk kinase domain (mutant) + inhibitor<BR />
-**[[3t9t]] – hTK Itk kinase domain (mutant) + arthritis drug<BR />
-**[[2e6i]] – hTK Itk BTK motif – NMR<BR />
-**[[4l7s]], [[4m0y]], [[4m0z]], [[4m12]], [[4m13]], [[4m14]], [[4m15]], [[4mf0]], [[4mf1]]   - hTK Itk kinase domain + inhibitor<br />
-**[[4pp9]], [[4ppa]], [[4ppb]], [[4ppc]], [[4pqn]], [[4qd6]], [[4rfm]] - hTK Itk kinase domain (mutant) + inhibitor<br />
-*'''Zap tyrosine kinase'''
-**[[4k2r]] – hTK Zap<br />
-**[[2ozo]] - hTK Zap (mutant) <br />
-**[[1m61]] - hTK Zap SH2 domain
-*Zap complex
-**[[2oq1]], [[4xz1]] - hTK Zap SH2 domain + peptide<br />
-**[[4xz0]] - hTK Zap SH2 domain + inhibitor<br />
-**[[1u59]] - hTK Zap kinase domain + staurosporine
-*'''Pyk2 tyrosine kinase or or protein-tyrosine kinase 2-β (Domains: kinase 414-692; FAT 861-1009)'''
-**[[3cc6]], [[3fzo]] - hTK Pyk2 kinase domain <br />
-**[[3gm2]] - hTK Pyk2 FAT domain<br />
-**[[3gm3]] - hTK Pyk2 FAT domain (mutant)<br />
-**[[4eku]] – hTK Pyk2 FERM domain<br />
-**[[2lk4]] - hTK Pyk2 FAT domain – NMR<br />
-*Pyk2 complex
-**[[3fzp]] - hTK Pyk2 kinase domain + ATPγS<br />
-**[[3fzr]], [[3fzs]], [[3fzt]], [[3h3c]], [[3et7]], [[5to8]], [[5tob]] - hTK Pyk2 kinase domain + inhibitor<br />
-**[[3gm1]], [[4r32]] - hTK Pyk2 FAT domain + paxillin peptide<br />
-**[[4xek]], [[4xev]], [[4xef]] - hTK Pyk2 FAT domain + leupaxin peptide<br />
-**[[4h1j]] - hFAK2 kinase domain + pyrazole inhibitor<br />
-**[[3h3c]] - hFAK2 kinase domain + pyrimidine inhibitor<br />
-**[[4h1m]] - hFAK2 kinase domain + indole inhibitor<br />
-**[[3u3f]] – hFAK2 FAT domain (mutant) + paxillin LD2 motif<br />
-*'''CapAB tyrosine kinase'''
-**[[3bfv]] - SaTK CapA1/CapB2 – ''Staphylococcus aureus'' <br />
-**[[2ved]] - SaTK CapA1/CapB2 + Mg + ADP
-*'''Fer tyrosine kinase'''
-**[[2kk6]] - hTK Fer SH2 domain – NMR<BR />
-*'''Ptk6 tyrosine kinase or breast tumor kinase Brk'''
-**[[1rja]] - hTK Ptk6 SH2 domain – NMR<br />
-**[[2kgt]] - hTK Ptk6 SH3 domain – NMR<br />
-**[[5d7v]], [[6cz2]] - hTK Ptk6 kinase domain <br />
-**[[5da3]], [[6cz3]], [[6cz4]] - hTK Ptk6 kinase domain + inhibitor<br />
-**[[5h2u]] - hTK Ptk6 kinase domain + drug<br />
-*'''Lyn tyrosine kinase''' (Domains: SH3 39-101; SH2 115-229; kinase 239-512)
-**[[4tzi]] - hTK Lyn SH2 domain <br />
-**[[1w1f]] - hTK Lyn SH3 domain – NMR<br />
-**[[1wa7]] - hTK Lyn SH3 domain + peptide – NMR<br />
-**[[3a4o]] - hTK Lyn residues 233-512 + staurosporine<br />
-**[[5xy1]] - hTK Lyn kinase domain + inhibitor<br />
-**[[2zv7]] - mTK Lyn kinase domain<br />
-**[[2zv8]] - mTK Lyn kinase domain + AMPPNP<br />
-**[[2zv9]] - mTK Lyn kinase domain + PP2<br />
-**[[2zva]] - mTK Lyn kinase domain + cancer drug<br />
-*'''Txk tyrosine kinase'''
-**[[2dm0]] - hTK Txk SH2 domain – NMR<br />
-*'''Yes tyrosine kinase'''
-**[[2hda]] - hTK Yes SH3 domain <br />
-**[[5mtj]] - hTK Yes SH2 domain + monobody<br />
-*'''Tec tyrosine kinase'''
-**[[2lul]] - hTK Tec PH domain - NMR<br />
-**[[1gl5]] - hTK Tec SH3 domain - NMR<br />
-*'''Fes/Fps tyrosine kinase'''
-**[[1wqu]], [[2dcr]] - hTK Fes SH2 domain - NMR<br />
-**[[3bkb]] - hTK Fes SH2+kinase domain - NMR<br />
-**[[4dyl]] - hTK Fes F-Bar domain <br />
-**[[3cbl]] - hTK Fes SH2+kinase domain + peptide<br />
-**[[3cd3]] - hTK Fes SH2+kinase domain + peptide + staurosporine<br />
-**[[4e93]] - hTK TFes + inhibitor<br />
-*'''Etk tyrosine kinase'''
-**[[3cio]] - EcTK Etk kinase domain – ''Escherichia coli''<br />
-*'''Wzc tyrosine kinase'''
-**[[3la6]] - EcTK Wzc kinase domain <br />
-*'''Ros tyrosine kinase'''
-**[[3zbf]] - hTK Ros kinase domain + cancer drug<br />
-**[[4uxl]] - hTK Ros kinase domain + inhibitor<br />
-*'''Tyk2 tyrosine kinase''' (Domains: SH2+FERM 23-540; pseudokinase 541-880; kinase 880-1170)
-**[[5f20]], [[5f1z]] - hTK Tyk2 kinase domain + inhibitor<br />
-**[[3lxn]], [[3lxp]], [[3nyx]], [[3nz0]], [[4e1z]], [[4e20]], [[4gfo]], [[4gih]], [[4gii]], [[4gj2]], [[4gj3]], [[4py1]], [[5wal]], [[5wev]], [[6dbk]], [[6dbm]] - hTK Tyk2 kinase domain (mutant) + inhibitor<br />
-**[[6aam]] - hTK Tyk2 kinase domain (mutant) + drug<br />
-**[[4gvj]] - hTK Tyk2 kinase domain (mutant) + ADP<br />
-**[[4oli]] - hTK Tyk2 pseudokinase + kinase domains <br />
-**[[3zon]], [[5c01]], [[5c03]] - hTK Tyk2 pseudokinase domain <br />
-**[[4wov]], [[5tkd]] - hTK Tyk2 pseudokinase domain + inhibitor<br />
-**[[4po6]] - hTK Tyk2 SH2+FERM domains + IFNAR1 peptide<br />
-*'''Kit tyrosine kinase'''
-**[[2ec8]] - hNTPK Kit extracellular domain<br />
-**[[3g0e]], [[3g0f]] - hNTPK Kit kinase domain (mutant) + cancer drug<br />
-**[[2e9w]], [[2o26]] - hNTPK Kit extracellular domain + stem cell factor<br />
-*'''Hck tyrosine kinase'''
-**[[3hck]] - hTK SH2 domain - NMR<BR />
-**[[1bu1]] - hTK SH3 domain <BR />
-**[[4hck]], [[5hck]] - hTK SH3 domain - NMR<BR />
-**[[2oj2]], [[2oi3]] - hTK SH3 domain + peptide - NMR<BR />
-**[[3rbb]], [[3rea]], [[3reb]] - hTK SH3 domain (mutant) + HIV NEF<BR />
-**[[3nhn]] - hTK SH3-SH2-linker domain <BR />
-**[[4u5w]] - hTK Hck SH3-SH2 domains + NEF <br />
-**[[2c0i]], [[2c0o]], [[2c0t]] - hTK SH3-SH2-SH1 domain + inhibitor<BR />
-**[[2hk5]] - hTK kinase domain + inhibitor<BR />
-**[[1qcf]], [[3vry]], [[3vrz]], [[3vs0]], [[3vs1]], [[3vs2]], [[3vs3]], [[3vs4]], [[3vs5]], [[3vs6]], [[3vs7]] - hTK SH3-SH2-kinase-tail domain + inhibitor<BR />
-**[[1ad5]] - hTK SH3-SH2-kinase-tail domain + AMPPNP<BR />
-**[[2hck]] - hTK SH3-SH2-kinase-tail domain + quercetin<BR />
-**[[4lud]], [[4lue]] - hTK Hck SH2+SH3+kinase domain (mutant) + fluorescent compound<br />
-**[[4orz]] - hTK Hck SH3 domain (mutant) + NEF + single domain antibody<br />
-'''
-*'''RECEPTOR TYROSINE KINASES - RTK
-*'''Bruton’s tyrosine kinase''' (Domains: PH 1-170; SH3 216-273; SH2 273-378; kinase 378-659)
-**[[2z0p]] - hTK Btk PH domain<br />
-**[[1btk]] – hTK Btk PH domain (mutant) <br />
-**[[3p08]], [[1k2p]] - hTK Btk kinase domain<br />
-**[[1aww]], [[1awx]], [[1qly]] - hTK Btk SH3 domain – NMR<BR />
-**[[2ge9]] - hTK Btk SH2 domain – NMR<BR />
-**[[4xi2]] - hTK Btk SH3-SH2-kinase domain<br />
-*Btk complex
-**[[1b55]] - hTK Btk PH domain + inositol-tetrakisphosphate<br />
-**[[1bwn]] - hTK Btk PH domain (mutant) + inositol-tetrakisphosphate<br />
-**[[3gen]], [[3ocs]], [[3pix]], [[3piy]], [[3piz]], [[3pj1]], [[3pj2]], [[3pj3]], [[4nwm]], [[4yhf]], [[5jrs]], [[5fbo]], [[5fbn]], [[4rx5]], [[5bpy]], [[5bqo]], [[5vgo]], [[5u9d]], [[5t18]], [[5p9m]], [[5p9l]], [[5p9m]], [[5p9l]], [[5p9f]], [[5p9g]], [[5p9h]], [[5p9i]], [[5p9j]], [[5p9k]] - hTK Btk kinase domain + inhibitor<br />
-**[[3k54]], [[3t9t]], [[4ot5]], [[4ot6]], [[4otq]], [[4otr]], [[4otf]], [[4rfy]], [[4rfz]], [[4rg0]] - hTK Btk kinase domain (mutant) + inhibitor<br />
-**[[3oct]] - hTK Btk kinase domain (mutant) + cancer drug<br />
-**[[5kup]] - hTK Btk residues 427-691 + inhibitor<br />
-*'''Fms tyrosine kinase'''
-**[[2i0v]] - hTK Fms kinase domain
-*Fms complex
-**[[2i0y]], [[2i1m]] - hTK Fms kinase domain + inhibitor<br />
-**[[3dpk]] - hTK Fms kinase domain (mutant) + inhibitor<br />
-**[[1flt]] – hTK Fms Igg-like domain + VEGF<br />
-**[[1qty]] - hTK Fms domain 2 + VEGF
-*'''Mer tyrosine kinase (Domains: FN3 373-483; kinase 570-864)'''
-**[[2dbj]] - hTK Mer FN3 domain – NMR<BR />
-**[[2p0c]] - hTK Mer kinase domain
-*Mer complex
-**[[3brb]] - hTK Mer kinase domain + ADP<br />
-**[[3bpr]], [[3tcp]], [[4m3q]], [[4mh7]], [[4mha]], [[5u6c]], [[5tc0]] - hTK Mer kinase domain + inhibitor<br />
-*'''Bone marrow tyrosine kinase'''
-**[[2ekx]] - hTK Bmx SH2 domain – NMR<BR />
-**[[2ys2]] - hTK Bmx Btk motif – NMR<BR />
-*Bone marrow tyrosine kinase complex
-**[[3sxr]] - hTK Bmx kinase domain (mutant) + dasatinib<br />
-**[[3sxs]] - hTK Bmx kinase domain (mutant) + inhibitor<br />
-*'''ErbB tyrosine kinase''' see [[Epidermal Growth Factor Receptor]]
-*'''Musk tyrosine kinase'''
-**[[3hkl]] - rTK Musk Fz-Crd domain <br />
-**[[1luf]], [[2iep]] - rTK Musk cytoplasmic domain <br />
-*'''Sgk223 tyrosine kinase or sugen kinase'''
-**[[5ve6]] - hTK <br />
-}}
 <references/>
+</StructureSection>
 [[Category:Topic Page]]

Tyrosine kinase

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Traditional Chinese medicine as dual guardians against hypertension and cancer? [11]

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Traditional Chinese medicine as dual guardians against hypertension and cancer? ^[11]