NIPBL Antibody
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货号:CSB-PA015817GA01HU
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规格:¥3,900
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其他:
产品详情
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Uniprot No.:Q6KC79
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基因名:NIPBL
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别名:CDLS antibody; Colon tumor susceptibility 2 antibody; Delangin antibody; DKFZp434L1319 antibody; FLJ11203 antibody; FLJ12597 antibody; FLJ13354 antibody; FLJ13648 antibody; FLJ44854 antibody; IDN 3 antibody; IDN 3 protein antibody; IDN 3 protein isoform A antibody; IDN 3 protein isoform B antibody; IDN 3B antibody; IDN3 B antibody; IDN3 protein antibody; IDN3 protein isoform A antibody; IDN3 protein isoform B antibody; IDN3B antibody; Mis 4 antibody; Mis4 antibody; Nipbl antibody; NIPBL_HUMAN antibody; Nipped B homolog (Drosophila) antibody; Nipped B homolog antibody; Nipped B like antibody; Nipped B like protein antibody; Nipped-B-like protein antibody; Scc 2 antibody; SCC 2 homolog antibody; Scc2 antibody; SCC2 homolog antibody; Sister chromatid cohesion protein Mis4 antibody
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宿主:Rabbit
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反应种属:Human,Mouse,Rat
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免疫原:Human NIPBL
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免疫原种属:Homo sapiens (Human)
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抗体亚型:IgG
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纯化方式:Antigen Affinity purified
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浓度:It differs from different batches. Please contact us to confirm it.
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保存缓冲液:PBS with 0.1% Sodium Azide, 50% Glycerol, pH 7.3. -20°C, Avoid freeze / thaw cycles.
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产品提供形式:Liquid
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应用范围:ELISA,WB
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Protocols:
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储存条件:Upon receipt, store at -20°C or -80°C. Avoid repeated freeze.
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货期:Basically, we can dispatch the products out in 1-3 working days after receiving your orders. Delivery time maybe differs from different purchasing way or location, please kindly consult your local distributors for specific delivery time.
相关产品
靶点详情
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功能:Plays an important role in the loading of the cohesin complex on to DNA. Forms a heterodimeric complex (also known as cohesin loading complex) with MAU2/SCC4 which mediates the loading of the cohesin complex onto chromatin. Plays a role in cohesin loading at sites of DNA damage. Its recruitment to double-strand breaks (DSBs) sites occurs in a CBX3-, RNF8- and RNF168-dependent manner whereas its recruitment to UV irradiation-induced DNA damage sites occurs in a ATM-, ATR-, RNF8- and RNF168-dependent manner. Along with ZNF609, promotes cortical neuron migration during brain development by regulating the transcription of crucial genes in this process. Preferentially binds promoters containing paused RNA polymerase II. Up-regulates the expression of SEMA3A, NRP1, PLXND1 and GABBR2 genes, among others.
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基因功能参考文献:
- Mutations in NIPBL result in the dysregulation of many genes responsible for normal heart development likely resulting in the variety of structural cardiac defects observed in the CdLS population. PMID: 29348408
- Frameshift Mutation in NIPBL gene is associated with Cornelia de Lange Syndrome. PMID: 29531005
- In Chinese patients with Cornelia de Lange syndrome, a heterozygous mutation in exon 20 of the NIPBL gene in proband 2, and a heterozygous mutation in intron 38 of the NIPBL gene in proband 3 were found, and RT-PCR revealed a splicing mutation in exon 38, generating both normal transcript and an aberrant alternatively spliced transcript with exon 38 deletion. PMID: 29452578
- Downregulation of cohesin loading factor NIPBL arrested breast cancer cells in vitro in the G0/G1 phase of the cell cycle and induced apoptosis and autophagy. PMID: 28987049
- Using fluorescence recovery after photobleaching (FRAP) and single-molecule tracking in human cells, the s show that Scc2 binds dynamically to chromatin, principally through an association with cohesin. PMID: 28914604
- s have identified a novel distal enhancer regulating both NIPBL and NIPBL-AS1. PMID: 29261648
- Nipbl seems to have also additional roles, for instance as transcription factor.This chapter summarizes our current knowledge on kollerin function and the recent studies on the genomic localization of Scc2, highlighting and critically discussing controversial data. PMID: 27797076
- The findings suggest similarities in the behavioral phenotype between those with and without the NIPBL mutation once differences in self help skills are controlled for. PMID: 28425213
- We conclude that SMC1A variants can result in a phenotype resembling CdLS and a phenotype resembling Rett syndrome. Resemblances between the SMC1A group and the NIPBL group suggest that a disturbed cohesin function contributes to the phenotype, but differences between these groups may also be explained by other underlying mechanisms such as moonlighting of the cohesin genes. PMID: 28548707
- NIPBL has evolved a sophisticated response to damaged DNA that is influenced by the form of damage, suggesting a highly dynamic role for NIPBL in maintaining genomic stability. PMID: 28167679
- 37 novel nipped-B-like protein (NIPBL) mutations were identified in Cornelia de Lange syndrome patients, including 34 in leukocytes and 3 in buccal cells only. PMID: 26701315
- Pathological variant specific of the isoform A of NIPBL was identified in two patients with Cornelia de Lange Syndrome. PMID: 28241484
- Subsequent quantitative PCR analysis demonstrated a 30% decrease of the total NIPBL mRNA levels associated with the frameshift transcript PMID: 26925417
- NIPBL gene mutation is associated with Thrombocytopenia in Cornelia de Lange syndrome. PMID: 26437745
- This study provides insight into the molecular pathology of Cornelia de Lange syndrome by establishing a relationship between NIPBL and HDAC8 mutations and PKR activation. PMID: 26725122
- NIPBL expression conferred poor prognosis and resistance to chemotherapy in non-small cell lung cancer PMID: 25963978
- Scc2 normally promotes a gene expression program that supports translational fidelity. . translational dysfunction may contribute to the human disorder Cornelia de Lange syndrome, which is caused by mutations in NIPBL, the human ortholog of SCC2. PMID: 26176819
- There was an increased frequncy of NIPBL mutations in a cohort of prenatal ultrasound detected phenotypes of Cornelia de Lange syndrome. PMID: 24218399
- A new Sanger sequencing reveals new hidden mutations in NIPBL gene not detected with conventional approach. PMID: 25196272
- analysis of the mutation spectrum of NIPBL in in Chinese patients with Cornelia de Lange syndrome PMID: 25447906
- Nine mutations affecting splice-sites in the NIPBL gene and four new splicing isoforms DeltaE10, DeltaE12, DeltaE33,34, and B' was identified in twelve CdLS patients. PMID: 24918291
- defects of NIPBL might lead to cohesin-loading defects and thereby alter gene expression and second, NIPBL deficiency might affect genes directly via its role at the respective promoters. PMID: 24550742
- Results show that NIPBL has a function in modulating chromatin architecture that is not dependent on SMC3/cohesin or CTCF in classical Cornelia de Lange syndrome. PMID: 23760082
- Letter/Case Report: novel NIPBL mutation giving rise to Cornelia de Lange syndrome and intrauterine fetal death. PMID: 24189319
- Canonical WNT pathway and CCND1 downregulation was observed in NIPBL-mutated patient-specific fibroblasts. PMID: 24136230
- In B cells from Cornelia de Lange Syndrome, found strong correlation between heterozygous loss-of-function mutations in cohesin loading protein NIPBL and a shift toward microhomology-based end joining during IG class switch recombination. PMID: 24145515
- These data suggest that NBPBL is frequently inactived in gastric and colorectal neoplasms with microsatellite instability. PMID: 23912250
- In the present study, conducted on a group of 64 unrelated Polish Cornelia de Lange syndrome patients, 25 various NIPBL sequence variants, including 22 novel point mutations, were detected. PMID: 23254390
- Somatic mosaicism for an NIPBL mutation is frequent (10/44; 23%) clinically in reliably diagnosed Cornelia de Lange syndrome individuals. PMID: 23505322
- NIPBL, SMC1A, and SMC3 mutation-positive patients were equally likely to have congenital heart diseases in Cornelia de lange syndrome. PMID: 22965847
- The mutational analysis in Chinese patients with Cornelia de Lange syndrome revealed splice-site mutations in NIPBL in 2 out of 4 patients. PMID: 22857006
- Large deletions/duplications in the NIPBL gene are detected in Cornelia de Lange patients. PMID: 22353942
- Our findings suggest a potential clinical utility to testing for copy number variations involving NIPBL when clinically diagnosed CdLS cases are mutation-negative by DNA-sequencing studies. PMID: 22241092
- In patient with Cornelia de Lange syndrome, a large deletion encompassing exons 35 to 47 of the NIPBL gene was identified. PMID: 20727427
- Development of NIPBL locus-specific database using LOVD: from novel mutations to further genotype-phenotype correlations in Cornelia de Lange Syndrome. PMID: 20824775
- The identification of 14 additional mutations of the cohesin complex genes NIPBL and SMC1A in a cohort of 30 unrelated patients with Cornelia de Lange syndrome, is reported. PMID: 20358602
- NIPBL mutation is associated with Cornelia de Lange syndrome. PMID: 20124326
- identified mutations in one gene, NIPBL, in four sporadic and two familial cases of Cornelia de Lange syndrome PMID: 15146186
- results show that NIPBL mutations are present in only 35% of Cornelia de Lange syndrome cases, strongly suggesting the genetic heterogeneity of this syndrome PMID: 15591270
- Mutations in NIPBL, the human homologue of the Drosophila Nipped-B gene, were found to cause De Lange syndrome. PMID: 16236812
- So far, two genes (NIPBL and SMC1L1) have been identified causing Cornelia de Lange syndrome (CdLS) or CdLS-like phenotypes. PMID: 17106445
- Large NIPBL deletion in a patient with Cornelia de Lange Syndrome. PMID: 17264868
- NIPBL mutations in Cornelia de Lange syndrome: truncating, splice-site, missense, in-frame deletion & regulatory; truncating mutations most frequent in patients with high clinical score; most splice-site & all missense mutations in low-medium score group PMID: 17661813
- This study identified duplications Cornelia de Lange syndrome (CdLS) on chromosomes 5 or X using genome wide array comparative genomic hybridisation (aCGH). The duplicated regions contain either the NIPBL or the SMC1A genes. PMID: 19052029
- Transcription in severely affected Cornelia de Lange Syndrome probands has identified a unique profile of dysregulated gene expression that correlates with phenotypic severity. PMID: 19468298
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相关疾病:Cornelia de Lange syndrome 1 (CDLS1)
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亚细胞定位:Nucleus. Chromosome.
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蛋白家族:SCC2/Nipped-B family
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组织特异性:Widely expressed. Highly expressed in heart, skeletal muscle, fetal and adult liver, fetal and adult kidney. Expressed at intermediates level in thymus, placenta, peripheral leukocyte and small intestine. Weakly or not expressed in brain, colon, spleen an
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数据库链接:
HGNC: 28862
OMIM: 122470
KEGG: hsa:25836
STRING: 9606.ENSP00000282516
UniGene: Hs.481927
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