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- 详细信息
- 文献和实验
- 技术资料
- 英文名:
P815
- 库存:
1x10^6/瓶/支
- 供应商:
上海酶研
- 肿瘤类型:
详询
- 细胞类型:
小鼠肥大细胞瘤细胞
- ATCC Number:
详询
- 品系:
P815
- 组织来源:
小鼠肥大细胞瘤细胞
- 相关疾病:
P815
- 物种来源:
哺乳动物
- 免疫类型:
详询
- 细胞形态:
贴壁/悬浮
- 是否是肿瘤细胞:
详询
- 器官来源:
小鼠肥大细胞瘤细胞
- 运输方式:
顺丰快递
- 年限:
5年
- 生长状态:
生长良好
P815/P815细胞系/P815细胞株/P815小鼠肥大细胞瘤细胞
Cell line name P815
Synonyms P-815; P 815
Accession CVCL_2154
Resource Identification Initiative To cite this cell line use: P815 (RRID:CVCL_2154)
Comments Part of: Tumor Immunology Bank (TIB) collection from Salk (transferred to ATCC in 1981).
Doubling time: ~18-22 hours (DSMZ=ACC-1).
Transformant: ChEBI; CHEBI:34342; 3-methylcholanthrene (3-MC; 20-methylcholanthrene; 20-MC; MCA).
Omics: SNP array analysis.
Misspelling: P825; Note=Occasionally.
Sequence variations
Mutation; MGI; MGI:96677; Kit; Simple; p.Asp818Tyr (c.2452G>T) (D814Y); Zygosity=Unspecified (PubMed=7513208; PubMed=10210327).
Disease Mouse mast cell neoplasm (NCIt: C21632)
Species of origin Mus musculus (Mouse) (NCBI Taxonomy: 10090)
Breed/subspecies: DBA/2.
Hierarchy Children:
CVCL_A9JC (P815 Hsp65-IL-2) CVCL_4Z63 (P815 MB) CVCL_4269 (P815-1-1)
CVCL_F735 (P815-X2) CVCL_C0DF (P815.Trh4)
Sex of cell Male
Category Cancer cell line
STR profile Source(s): DSMZ=ACC-1; PubMed=31220119
Markers:
Mouse STR 1-1 16,17
Mouse STR 1-2 14,17,18
Mouse STR 2-1 15
Mouse STR 3-2 13,14
Mouse STR 4-2 20.3
Mouse STR 5-5 13 (PubMed=31220119)
13,14 (DSMZ=ACC-1)
Mouse STR 6-4 17 (DSMZ=ACC-1)
17,18 (PubMed=31220119)
Mouse STR 6-7 12 (PubMed=31220119)
12,13 (DSMZ=ACC-1)
Mouse STR 7-1 27
Mouse STR 8-1 16
Mouse STR 11-2 16,17,18
Mouse STR 12-1 16,17 (DSMZ=ACC-1)
17 (PubMed=31220119)
Mouse STR 13-1 17,18
Mouse STR 15-3 20.3,21.3 (PubMed=31220119)
21.3 (DSMZ=ACC-1)
Mouse STR 17-2 17
Mouse STR 18-3 17 (PubMed=31220119)
17,18 (DSMZ=ACC-1)
Mouse STR 19-2 12
Mouse STR X-1 27 (PubMed=31220119)
27,28 (DSMZ=ACC-1)
Run an STR similarity search on this cell line
Web pages
Publications
PubMed=4208429; DOI=10.1038/249049a0
Ralph P., Nakoinz I.
Lipopolysaccharides inhibit lymphosarcoma cells of bone marrow orgin.
Nature 249:49-51(1974)
PubMed=1234049; DOI=10.1002/eji.1830050208
Kiessling R., Klein E., Wigzell H.
'Natural' killer cells in the mouse. I. Cytotoxic cells with specificity for mouse Moloney leukemia cells. Specificity and distribution according to genotype.
Eur. J. Immunol. 5:112-117(1975)
DOI=10.2220/biomedres.5.19
Yanagisawa M., Hasegawa H., Ichiyama A., Hosoda S., Nakamura W.
Comparison of serotonin-producing murine mastocytomas, P-815 and FMA3: determination of tryptophan hydroxylase, aromatic L-amino acid decarboxylase, and cellular concentration of tryptophan, 5- hydroxytryprophan, 5-hydroxytryptamine and 5-hydroxyindoleacetic acid.
Biomed. Res. 5:19-28(1984)
PubMed=3792703; DOI=10.1111/j.1432-0436.1986.tb00568.x
Leenen P.J.M., Jansen A.M.A.C., van Ewijk W.
Murine macrophage cell lines can be ordered in a linear differentiation sequence.
Differentiation 32:157-164(1986)
PubMed=7513208; DOI=10.1182/blood.V83.9.2619.2619
Tsujimura T., Furitsu T., Morimoto M., Isozaki K., Nomura S., Matsuzawa Y., Kitamura Y., Kanakura Y.
Ligand-independent activation of c-kit receptor tyrosine kinase in a murine mastocytoma cell line P-815 generated by a point mutation.
Blood 83:2619-2626(1994)
PubMed=10210327; DOI=10.1016/S0301-472X(98)00075-7
London C.A., Galli S.J., Yuuki T., Hu Z.-Q., Helfand S.C., Geissler E.N.
Spontaneous canine mast cell tumors express tandem duplications in the proto-oncogene c-kit.
Exp. Hematol. 27:689-697(1999)
PubMed=18432777; DOI=10.1002/0471142735.im2004s43
Gajewski T.F., Markiewicz M.A., Uyttenhove C.
The P815 mastocytoma tumor model.
Curr. Protoc. Immunol. 43:20.4.1-20.4.18(2001)
PubMed=25277546; DOI=10.1186/1471-2164-15-847; PMCID=PMC4198738
Didion J.P., Buus R.J., Naghashfar Z., Threadgill D.W., Morse H.C. 3rd, Pardo-Manuel de Villena F.
SNP array profiling of mouse cell lines identifies their strains of origin and reveals cross-contamination and widespread aneuploidy.
BMC Genomics 15:847.1-847.11(2014)
PubMed=31220119; DOI=10.1371/journal.pone.0218412; PMCID=PMC6586308
Almeida J.L., Dakic A., Kindig K., Kone M., Letham D.L.D., Langdon S., Peat R., Holding-Pillai J., Hall E.M., Ladd M., Shaffer M.D., Berg H., Li J.-L., Wigger G., Lund S., Steffen C.R., Fransway B.B., Geraghty B., Natoli M., Bauer B.A., Gollin S.M., Lewis D.W., Reid Y.A.
Interlaboratory study to validate a STR profiling method for intraspecies identification of mouse cell lines.
PLoS ONE 14:E0218412-E0218412(2019)
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文献和实验*发表【中文论文】请标注:由上海酶研生物科技有限公司提供;
*发表【英文论文】请标注:From Shanghai EK-Bioscience Biotechnology Co., Ltd.
一、效应细胞的制备激惹5天后,于无菌条件下取出受鼠引流的腹股沟淋巴结,100目钢网研磨,调整细胞浓度为2×107.ml-1。台盼蓝色要求存活率>95%。二、靶细胞的制备P815细胞株系DBA/2小鼠的肥大细胞瘤细胞株。连续传代培养,调整细胞浓度为2×105/ml或3.33×105/ml(加入α-Lyt2 mAb时的靶细胞浓度),台盼蓝染色成活率>95%。三、LDH释放法测定CTL的功能按表1加样于96孔培养板中,设3个复孔。混匀置二氧化碳培养箱中孵育4h。室温离心,用微量加样器每孔取
-8 EBV转化的绒猴白细胞 CP-88 草鱼胚胎细胞 NISE-Sacy-12 蓖麻蚕卵细胞 ZC-7901 草鱼吻端细胞 RF/6A 猴脉络膜-视网膜细胞(内皮) Mv1Lu 貂肺上皮细胞 二、肿瘤细胞 1.小鼠类 EL4 淋巴瘤 Pcc4 胚癌细胞 EL4IL-2 淋巴瘤 P815 肥大细胞瘤 YAC-1 淋巴瘤 MFC 前胃癌 L1210 淋巴白血病 AtT20 垂体瘤 P388D1 淋巴样瘤 NS
真爱满行囊 我最近在体外细胞做的关于gsk3-beta功能问题,发现药物处理以后,gsk-3-beta的总表达量下调,如果是这样的话 1、我是否能够得出gsk-3-beta的活性下调的结论? 2、是否还有必要做非活性形式的表达量?我的理解是,基础状态下,gsk-3beta维持的是低活性状态,如果总量都下调了,那应该能够得出活性降低的结论了吧? 3、另外,在这种情况下我是否有必要去做gsk-3-beta的216位点的活性形式的表达
技术资料
