| 產(chǎn)品介紹 |
background:
Fanconi Anemia (FANC) is a human autosomal-recessive cancer susceptibility disorder characterized by congenital defects, progressive bone marrow failure, and cellular hypersensitivity to mitomycin C (MMC). The FANC subunit D2 protein is vital for cellular resistance to DNA cross-linking and the arrest of DNA synthesis after ionizing radiation. DNA damage activates the monoubiquitination of FANC D2, targeting nuclear foci containing the BRCA 1 protein.
Function:
Required for maintenance of chromosomal stability. Promotes accurate and efficient pairing of homologs during meiosis. Involved in the repair of DNA double-strand breaks, both by homologous recombination and single-strand annealing. May participate in S phase and G2 phase checkpoint activation upon DNA damage. Plays a role in preventing breakage and loss of missegregating chromatin at the end of cell division, particularly after replication stress. Required for the targeting, or stabilization, of BLM to non-centromeric abnormal structures induced by replicative stress. Promotes BRCA2/FANCD1 loading onto damaged chromatin. May also be involved in B-cell immunoglobulin isotype switching.
Subunit:
Interacts directly with FANCE and FANCI. Interacts with USP1 and MEN1. The ubiquitinated form specifically interacts with BRCA1 and BLM. Both the nonubiquitinated and the monoubiquitinated forms interact with BRCA2; this interaction is mediated by phosphorylated FANCG and the complex also includes XCCR3. The ubiquitinated form specifically interacts with MTMR15/FAN1 (via UBZ-type zinc finger), leading to recruit MTMR15/FAN1 to sites of DNA damage. Interacts with DCLRE1B/Apollo.
Subcellular Location:
Nucleus. Note=Concentrates in nuclear foci during S phase and upon genotoxic stress. At the onset of mitosis, excluded from chromosomes and diffuses into the cytoplasm, returning to the nucleus at the end of cell division. Observed in a few spots localized in pairs on the sister chromatids of mitotic chromosome arms and not centromeres, one on each chromatids. These foci coincide with common fragile sites and could be sites of replication fork stalling. The foci are frequently interlinked through BLM-associated ultra-fine DNA bridges. Following aphidicolin treatment, targets chromatid gaps and breaks.
Tissue Specificity:
Highly expressed in germinal center cells of the spleen, tonsil, and reactive lymph nodes, and in the proliferating basal layer of squamous epithelium of tonsil, esophagus, oropharynx, larynx and cervix. Expressed in cytotrophoblastic cells of the placenta and exocrine cells of the pancreas (at protein level). Highly expressed in testis, where expression is restricted to maturing spermatocytes.
Post-translational modifications:
Monoubiquitinated on Lys-561 during S phase and upon genotoxic stress by FANCL in complex with E2 ligases UBE2T or UBE2W (isoform 1 and isoform 2). Deubiquitinated by USP1 as cells enter G2/M, or once DNA repair is completed. Monoubiquitination requires the joint intervention of the FANC core complex, including FANCA, FANCB, FANCC, FANCE, FANCF, FANCG, and FANCM, and proteins involved in cell cycle checkpoints and DNA repair, including RPA1, ATR, CHEK1 and BRCA1, and is mediated by FANCL/PHF9. Ubiquitination is required for binding to chromatin, interaction with BRCA1, BRCA2 and MTMR15/FAN1, DNA repair, and normal cell cycle progression, but not for phosphorylation on Ser-222 or interaction with MEN1.
Phosphorylated in response to various genotoxic stresses by ATM and/or ATR. Upon ionizing radiation, phosphorylated by ATM on Ser-222 and Ser-1404. Phosphorylation on Ser-222 is required for S-phase checkpoint activation, but not for ubiquitination, foci formation, or DNA repair. In contrast, phosphorylation by ATR on other sites may be required for ubiquitination and foci formation.
Defects in FANCD2 are a cause of Fanconi anemia complementation group D type 2 (FANCD2) [MIM:227646]. A disorder affecting all bone marrow elements and resulting in anemia, leukopenia and thrombopenia. It is associated with cardiac, renal and limb malformations, dermal pigmentary changes, and a predisposition to the development of malignancies. At the cellular level it is associated with hypersensitivity to DNA-damaging agents, chromosomal instability (increased chromosome breakage) and defective DNA repair.
Database links:
Entrez Gene: 2177 Human
Entrez Gene: 211651 Mouse
Entrez Gene: 312641 Rat
Omim: 613984 Human
SwissProt: Q9BXW9 Human
SwissProt: Q80V62 Mouse
SwissProt: Q6IV68 Rat
Unigene: 208388 Human
Unigene: 160061 Mouse
Unigene: 203979 Rat
Important Note:
This product as supplied is intended for research use only, not for use in human, therapeutic or diagnostic applications.
FANCD2是一種在DNA損傷修復(fù)過(guò)程中起重要作用的蛋白質(zhì),其作作用在于通過(guò)修補(bǔ)DNA損傷或促進(jìn)有缺陷細(xì)胞自殺來(lái)預(yù)防癌癥���,所以低水平的FANCD2會(huì)導(dǎo)致DNA損傷���,從而誘發(fā)癌癥。
有學(xué)者認(rèn)為:FANCD2是個(gè)重要的抵御癌癥蛋白�,而香煙會(huì)破壞它的制造過(guò)程當(dāng)然還可能包含有其他蛋白,但至少FANCD2是關(guān)鍵的主要蛋白����,因?yàn)楹蟹浅8咚紽ANCD2的細(xì)胞能夠抵御香煙的毒害作用�����。
FANCD2蛋白在保護(hù)肺細(xì)胞抵御香煙威脅時(shí)有重要作用����;FANCD2蛋白是負(fù)責(zé)修復(fù)受損DNA的重要蛋白��,而受香煙燃燒產(chǎn)生的煙霧影響的肺細(xì)胞很少產(chǎn)生FANCD2蛋白�����,沒(méi)有FANCD2蛋白�,受損的DNA導(dǎo)致腫瘤細(xì)胞增殖擴(kuò)散并無(wú)法控制。研究結(jié)果表明���,F(xiàn)ANCD2蛋白在保護(hù)肺細(xì)胞抵御香煙威脅時(shí)有重要作用���,也可解釋為什麼香煙燃燒產(chǎn)生的煙霧對(duì)肺細(xì)胞具有如此大的危害。
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