General Information of the Ferroptosis Regulator (ID: REG10078)
Regulator Name Protein disulfide-isomerase (P4HB)
Synonyms
ERBA2L, PDI, PDIA1, PO4DB; Cellular thyroid hormone-binding protein; Prolyl 4-hydroxylase subunit beta; p55
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Gene Name P4HB
Gene ID 5034
Regulator Type Protein coding
Uniprot ID P07237
Sequence
MLRRALLCLAVAALVRADAPEEEDHVLVLRKSNFAEALAAHKYLLVEFYAPWCGHCKALA
PEYAKAAGKLKAEGSEIRLAKVDATEESDLAQQYGVRGYPTIKFFRNGDTASPKEYTAGR
EADDIVNWLKKRTGPAATTLPDGAAAESLVESSEVAVIGFFKDVESDSAKQFLQAAEAID
DIPFGITSNSDVFSKYQLDKDGVVLFKKFDEGRNNFEGEVTKENLLDFIKHNQLPLVIEF
TEQTAPKIFGGEIKTHILLFLPKSVSDYDGKLSNFKTAAESFKGKILFIFIDSDHTDNQR
ILEFFGLKKEECPAVRLITLEEEMTKYKPESEELTAERITEFCHRFLEGKIKPHLMSQEL
PEDWDKQPVKVLVGKNFEDVAFDEKKNVFVEFYAPWCGHCKQLAPIWDKLGETYKDHENI
VIAKMDSTANEVEAVKVHSFPTLKFFPASADRTVIDYNGERTLDGFKKFLESGGQDGAGD
DDDLEDLEEAEEPDMEEDDDQKAVKDEL

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Family Protein disulfide isomerase family
Function
This multifunctional protein catalyzes the formation, breakage and rearrangement of disulfide bonds. At the cell surface, seems to act as a reductase that cleaves disulfide bonds of proteins attached to the cell. May therefore cause structural modifications of exofacial proteins. Inside the cell, seems to form/rearrange disulfide bonds of nascent proteins. At high concentrations and following phosphorylation by FAM20C, functions as a chaperone that inhibits aggregation of misfolded proteins. At low concentrations, facilitates aggregation (anti-chaperone activity). May be involved with other chaperones in the structural modification of the TG precursor in hormone biogenesis. Also acts as a structural subunit of various enzymes such as prolyl 4-hydroxylase and microsomal triacylglycerol transfer protein MTTP. Receptor for LGALS9; the interaction retains P4HB at the cell surface of Th2 T helper cells, increasing disulfide reductase activity at the plasma membrane, altering the plasma membrane redox state and enhancing cell migration.

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HGNC ID
HGNC:8548
KEGG ID hsa:5034
Full List of the Ferroptosis Target of This Regulator and Corresponding Disease/Drug Response(s)
P4HB can regulate the following target(s), and cause disease/drug response(s). You can browse detail information of target(s) or disease/drug response(s).
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Unspecific Target [Unspecific Target]
In total 1 item(s) under this target
Experiment 1 Reporting the Ferroptosis Target of This Regulator [1]
Responsed Disease Fibrosarcoma ICD-11: 2B53
Responsed Drug FIPC-1 Investigative
Pathway Response Ferroptosis hsa04216
Cell Process Cell ferroptosis
In Vitro Model
HT-1080 cells Fibrosarcoma Homo sapiens CVCL_0317
A-375 cells Amelanotic melanoma Homo sapiens CVCL_0132
Response regulation Iron-dependent and competitive protein labeling by FIPC-1 was demonstrated in a quantitative chemoproteomic workflow that identified several saturable protein targets in fibrosarcoma cells, including P4HB and NT5DC2.
Fibrosarcoma [ICD-11: 2B53]
In total 1 item(s) under this disease
Experiment 1 Reporting the Ferroptosis-centered Disease Response [1]
Target Regulator Protein disulfide-isomerase (P4HB) Protein coding
Responsed Drug FIPC-1 Investigative
Pathway Response Ferroptosis hsa04216
Cell Process Cell ferroptosis
In Vitro Model
HT-1080 cells Fibrosarcoma Homo sapiens CVCL_0317
A-375 cells Amelanotic melanoma Homo sapiens CVCL_0132
Response regulation Iron-dependent and competitive protein labeling by FIPC-1 was demonstrated in a quantitative chemoproteomic workflow that identified several saturable protein targets in fibrosarcoma cells, including P4HB and NT5DC2.
FIPC-1 [Investigative]
In total 1 item(s) under this drug
Experiment 1 Reporting the Ferroptosis-centered Drug Response [1]
Drug for Ferroptosis Inducer
Response Target Unspecific Target
Responsed Disease Fibrosarcoma ICD-11: 2B53
Pathway Response Ferroptosis hsa04216
Cell Process Cell ferroptosis
In Vitro Model
HT-1080 cells Fibrosarcoma Homo sapiens CVCL_0317
A-375 cells Amelanotic melanoma Homo sapiens CVCL_0132
Response regulation Iron-dependent and competitive protein labeling by FIPC-1 was demonstrated in a quantitative chemoproteomic workflow that identified several saturable protein targets in fibrosarcoma cells, including P4HB and NT5DC2.
References
Ref 1 Reactivity-Based Probe of the Iron(II)-Dependent Interactome Identifies New Cellular Modulators of Ferroptosis. J Am Chem Soc. 2020 Nov 11;142(45):19085-19093. doi: 10.1021/jacs.0c06709. Epub 2020 Oct 30.