Molecule Information
General Information of the Molecule (ID: Mol00933)
| Name |
DNA topoisomerase 4 subunit A (PARC)
,Escherichia coli
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| Synonyms |
Topoisomerase IV subunit A; b3019; JW2987
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| Molecule Type |
Protein
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| Gene Name |
parC
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| Gene ID | |||||
| Sequence |
MSDMAERLALHEFTENAYLNYSMYVIMDRALPFIGDGLKPVQRRIVYAMSELGLNASAKF
KKSARTVGDVLGKYHPHGDSACYEAMVLMAQPFSYRYPLVDGQGNWGAPDDPKSFAAMRY TESRLSKYSELLLSELGQGTADWVPNFDGTLQEPKMLPARLPNILLNGTTGIAVGMATDI PPHNLREVAQAAIALIDQPKTTLDQLLDIVQGPDYPTEAEIITSRAEIRKIYENGRGSVR MRAVWKKEDGAVVISALPHQVSGARVLEQIAAQMRNKKLPMVDDLRDESDHENPTRLVIV PRSNRVDMDQVMNHLFATTDLEKSYRINLNMIGLDGRPAVKNLLEILSEWLVFRRDTVRR RLNYRLEKVLKRLHILEGLLVAFLNIDEVIEIIRNEDEPKPALMSRFGLTETQAEAILEL KLRHLAKLEEMKIRGEQSELEKERDQLQGILASERKMNNLLKKELQADAQAYGDDRRSPL QEREEAKAMSEHDMLPSEPVTIVLSQMGWVRSAKGHDIDAPGLNYKAGDSFKAAVKGKSN QPVVFVDSTGRSYAIDPITLPSARGQGEPLTGKLTLPPGATVDHMLMESDDQKLLMASDA GYGFVCTFNDLVARNRAGKALITLPENAHVMPPVVIEDASDMLLAITQAGRMLMFPVSDL PQLSKGKGNKIINIPSAEAARGEDGLAQLYVLPPQSTLTIHVGKRKIKLRPEELQKVTGE RGRRGTLMRGLQRIDRVEIDSPRRASSGDSEE Click to Show/Hide
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| 3D-structure |
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| Function |
Topoisomerase IV is essential for chromosome segregation; it is the principal protein responsible for decatenating newly replicated chromosomes. It relaxes supercoiled DNA (12269820, PuMed:16023671300644). MukB stimulates the relaxation activity of topoisomerase IV and also has a modest effect on decatenation.
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| Uniprot ID | |||||
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Type(s) of Resistant Mechanism of This Molecule
ADTT: Aberration of the Drug's Therapeutic Target
EADR: Epigenetic Alteration of DNA, RNA or Protein
Drug Resistance Data Categorized by Drug
Approved Drug(s)
3 drug(s) in total
Ciprofloxacin XR
| Drug Resistance Data Categorized by Their Corresponding Mechanisms | ||||
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Epigenetic Alteration of DNA, RNA or Protein (EADR)
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| Disease Class: Escherichia coli infection [ICD-11: 1A03.0] | [1] | |||
| Resistant Disease | Escherichia coli infection [ICD-11: 1A03.0] | |||
| Resistant Drug | Ciprofloxacin XR | |||
| Molecule Alteration | Missense mutation | p.S80l |
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| Experimental Note | Discovered Using In-vivo Testing Model | |||
| In Vitro Model | Escherichia coli ECIS803 | 562 | ||
| Escherichia coli ATCC 43869 | 562 | |||
| Experiment for Molecule Alteration |
PCR; DNA sequence assay | |||
| Experiment for Drug Resistance |
Broth microdilution method assay | |||
| Mechanism Description | Mutational substitutions in the quinolone target enzymes, namely DNA topoisomerase II (GyrA) and topoisomerase IV (ParC), are recognised to be the major mechanisms through which resistance develops. | |||
| Disease Class: Escherichia coli infection [ICD-11: 1A03.0] | [1] | |||
| Resistant Disease | Escherichia coli infection [ICD-11: 1A03.0] | |||
| Resistant Drug | Ciprofloxacin XR | |||
| Molecule Alteration | Missense mutation | p.E84G |
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| Experimental Note | Discovered Using In-vivo Testing Model | |||
| In Vitro Model | Escherichia coli ECIS803 | 562 | ||
| Escherichia coli ATCC 43869 | 562 | |||
| Experiment for Molecule Alteration |
PCR; DNA sequence assay | |||
| Experiment for Drug Resistance |
Broth microdilution method assay | |||
| Mechanism Description | Mutational substitutions in the quinolone target enzymes, namely DNA topoisomerase II (GyrA) and topoisomerase IV (ParC), are recognised to be the major mechanisms through which resistance develops. | |||
Nalidixic acid
| Drug Resistance Data Categorized by Their Corresponding Mechanisms | ||||
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Aberration of the Drug's Therapeutic Target (ADTT)
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| Disease Class: Escherichia coli infection [ICD-11: 1A03.0] | [1] | |||
| Resistant Disease | Escherichia coli infection [ICD-11: 1A03.0] | |||
| Resistant Drug | Nalidixic acid | |||
| Molecule Alteration | Missense mutation | p.S80l |
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| Experimental Note | Discovered Using In-vivo Testing Model | |||
| In Vitro Model | Escherichia coli ECIS803 | 562 | ||
| Escherichia coli ATCC 43869 | 562 | |||
| Experiment for Molecule Alteration |
PCR; DNA sequence assay | |||
| Experiment for Drug Resistance |
Broth microdilution method assay | |||
| Mechanism Description | Mutational substitutions in the quinolone target enzymes, namely DNA topoisomerase II (GyrA) and topoisomerase IV (ParC), are recognised to be the major mechanisms through which resistance develops. | |||
| Disease Class: Escherichia coli infection [ICD-11: 1A03.0] | [1] | |||
| Resistant Disease | Escherichia coli infection [ICD-11: 1A03.0] | |||
| Resistant Drug | Nalidixic acid | |||
| Molecule Alteration | Missense mutation | p.E84G |
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| Experimental Note | Discovered Using In-vivo Testing Model | |||
| In Vitro Model | Escherichia coli ECIS803 | 562 | ||
| Escherichia coli ATCC 43869 | 562 | |||
| Experiment for Molecule Alteration |
PCR; DNA sequence assay | |||
| Experiment for Drug Resistance |
Broth microdilution method assay | |||
| Mechanism Description | Mutational substitutions in the quinolone target enzymes, namely DNA topoisomerase II (GyrA) and topoisomerase IV (ParC), are recognised to be the major mechanisms through which resistance develops. | |||
Ofloxacin
| Drug Resistance Data Categorized by Their Corresponding Mechanisms | ||||
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Epigenetic Alteration of DNA, RNA or Protein (EADR)
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| Disease Class: Escherichia coli infection [ICD-11: 1A03.0] | [1] | |||
| Resistant Disease | Escherichia coli infection [ICD-11: 1A03.0] | |||
| Resistant Drug | Ofloxacin | |||
| Molecule Alteration | Missense mutation | p.S80l |
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| Experimental Note | Discovered Using In-vivo Testing Model | |||
| In Vitro Model | Escherichia coli ECIS803 | 562 | ||
| Escherichia coli ATCC 43869 | 562 | |||
| Experiment for Molecule Alteration |
PCR; DNA sequence assay | |||
| Experiment for Drug Resistance |
Broth microdilution method assay | |||
| Mechanism Description | Mutational substitutions in the quinolone target enzymes, namely DNA topoisomerase II (GyrA) and topoisomerase IV (ParC), are recognised to be the major mechanisms through which resistance develops. | |||
| Disease Class: Escherichia coli infection [ICD-11: 1A03.0] | [1] | |||
| Resistant Disease | Escherichia coli infection [ICD-11: 1A03.0] | |||
| Resistant Drug | Ofloxacin | |||
| Molecule Alteration | Missense mutation | p.E84G |
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| Experimental Note | Discovered Using In-vivo Testing Model | |||
| In Vitro Model | Escherichia coli ECIS803 | 562 | ||
| Escherichia coli ATCC 43869 | 562 | |||
| Experiment for Molecule Alteration |
PCR; DNA sequence assay | |||
| Experiment for Drug Resistance |
Broth microdilution method assay | |||
| Mechanism Description | Mutational substitutions in the quinolone target enzymes, namely DNA topoisomerase II (GyrA) and topoisomerase IV (ParC), are recognised to be the major mechanisms through which resistance develops. | |||
References
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