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- 详细信息
- 文献和实验
- 技术资料
- 英文名:
NOMO-1
- 库存:
1x10^6/瓶
- 供应商:
上海酶研
- 肿瘤类型:
无
- 细胞类型:
NOMO-1
- 品系:
NOMO-1
- 组织来源:
人白血病细胞
- 相关疾病:
详询
- 物种来源:
人
- 免疫类型:
详询
- 细胞形态:
贴壁/悬浮
- 是否是肿瘤细胞:
否
- 器官来源:
人白血病细胞
- 运输方式:
顺丰快递
- 年限:
5年
- 生长状态:
生长良好
- 规格:
瓶
NOMO-1、NOMO-1、NOMO-1细胞、NOMO-1细胞、NOMO-1人白血病细胞
Part of: Cancer Dependency Map project (DepMap) (includes Cancer Cell Line Encyclopedia - CCLE).
Part of: COSMIC cell lines project.
Population: Japanese.
Doubling time: 55 hours (PubMed=25984343); ~35 hours (DSMZ=ACC-542).
Microsatellite instability: Stable (MSS) (Sanger).
Omics: Deep exome analysis.
Omics: Deep quantitative phosphoproteome analysis.
Omics: DNA methylation analysis.
Omics: shRNA library screening.
Omics: SNP array analysis.
Omics: Transcriptome analysis by microarray.
Omics: Transcriptome analysis by RNAseq.
Derived from site: In situ; Bone marrow; UBERON=UBERON_0002371.
Source(s): Cosmic-CLP=908451; DSMZ=ACC-542; JCRB=IFO50474; PubMed=25877200
Markers:
Amelogenin X
CSF1PO 11,12
D2S1338 17,23
D3S1358 15,17
D5S818 11,13
D7S820 8,10
D8S1179 13,14
D13S317 8,10
D16S539 9,11
D18S51 17,21.2 (DSMZ=ACC-542)
17,22 (PubMed=25877200)
D19S433 13,14
D21S11 29,32.2
FGA 21,22
Penta D 9,12
Penta E 15,17
TH01 6,9
TPOX 8,12
vWA 17,18
Run an STR similarity search on this cell line
Publications
DOI=10.3960/jslrt1961.28.19
Ogura M., Hamaguchi M.
Coagulation and fibrinolysis system of a human monocytic leukemia cell line, NOMO-1.
Nihon Monaikei Gakkai Kaishi 28:19-26(1988)
PubMed=1699657
Towatari M., Ito Y., Morishita Y., Tanimoto M., Kawashima K., Morishima Y., Andoh T., Saito H.
Enhanced expression of DNA topoisomerase II by recombinant human granulocyte colony-stimulating factor in human leukemia cells.
Cancer Res. 50:7198-7202(1990)
PubMed=1701357
Morishita Y., Kataoka T., Towatari M., Ito T., Inoue H., Ogura M., Morishima Y., Saito H.
Up-regulation of transferrin receptor gene expression by granulocyte colony-stimulating factor in human myeloid leukemia cells.
Cancer Res. 50:7955-7961(1990)
PubMed=9738977; DOI=10.1111/j.1349-7006.1998.tb03275.x; PMCID=PMC5921886
Takizawa J., Suzuki R., Kuroda H., Utsunomiya A., Kagami Y., Joh T., Aizawa Y., Ueda R., Seto M.
Expression of the TCL1 gene at 14q32 in B-cell malignancies but not in adult T-cell leukemia.
Jpn. J. Cancer Res. 89:712-718(1998)
DOI=10.1016/B978-0-12-221970-2.50457-5
Drexler H.G.
The leukemia-lymphoma cell line factsbook.
(In book) ISBN 9780122219702; pp.1-733; Academic Press; London; United Kingdom (2001)
PubMed=14671638; DOI=10.1038/sj.leu.2403236
Drexler H.G., Quentmeier H., MacLeod R.A.F.
Malignant hematopoietic cell lines: in vitro models for the study of MLL gene alterations.
Leukemia 18:227-232(2004)
PubMed=20164919; DOI=10.1038/nature08768; PMCID=PMC3145113
Bignell G.R., Greenman C.D., Davies H.R., Butler A.P., Edkins S., Andrews J.M., Buck G., Chen L., Beare D., Latimer C., Widaa S., Hinton J., Fahey C., Fu B.-Y., Swamy S., Dalgliesh G.L., Teh B.T., Deloukas P., Yang F.-T., Campbell P.J., Futreal P.A., Stratton M.R.
Signatures of mutation and selection in the cancer genome.
Nature 463:893-898(2010)
PubMed=21552520; DOI=10.1371/journal.pone.0019169; PMCID=PMC3084268
Gu T.-L., Nardone J., Wang Y., Loriaux M., Villen J., Beausoleil S.A., Tucker M., Kornhauser J.M., Ren J.-M., MacNeill J., Gygi S.P., Druker B.J., Heinrich M.C., Rush J., Polakiewicz R.D.
Survey of activated FLT3 signaling in leukemia.
PLoS ONE 6:E19169-E19169(2011)
PubMed=22460905; DOI=10.1038/nature11003; PMCID=PMC3320027
Barretina J.G., Caponigro G., Stransky N., Venkatesan K., Margolin A.A., Kim S., Wilson C.J., Lehar J., Kryukov G.V., Sonkin D., Reddy A., Liu M., Murray L., Berger M.F., Monahan J.E., Morais P., Meltzer J., Korejwa A., Jane-Valbuena J., Mapa F.A., Thibault J., Bric-Furlong E., Raman P., Shipway A., Engels I.H., Cheng J., Yu G.-Y.K., Yu J.-J., Aspesi P. Jr., de Silva M., Jagtap K., Jones M.D., Wang L., Hatton C., Palescandolo E., Gupta S., Mahan S., Sougnez C., Onofrio R.C., Liefeld T., MacConaill L.E., Winckler W., Reich M., Li N.-X., Mesirov J.P., Gabriel S.B., Getz G., Ardlie K., Chan V., Myer V.E., Weber B.L., Porter J., Warmuth M., Finan P., Harris J.L., Meyerson M.L., Golub T.R., Morrissey M.P., Sellers W.R., Schlegel R., Garraway L.A.
The Cancer Cell Line Encyclopedia enables predictive modelling of anticancer drug sensitivity.
Nature 483:603-607(2012)
PubMed=25984343; DOI=10.1038/sdata.2014.35; PMCID=PMC4432652
Cowley G.S., Weir B.A., Vazquez F., Tamayo P., Scott J.A., Rusin S., East-Seletsky A., Ali L.D., Gerath W.F.J., Pantel S.E., Lizotte P.H., Jiang G.-Z., Hsiao J., Tsherniak A., Dwinell E., Aoyama S., Okamoto M., Harrington W., Gelfand E.T., Green T.M., Tomko M.J., Gopal S., Wong T.C., Li H.-B., Howell S., Stransky N., Liefeld T., Jang D., Bistline J., Meyers B.H., Armstrong S.A., Anderson K.C., Stegmaier K., Reich M., Pellman D., Boehm J.S., Mesirov J.P., Golub T.R., Root D.E., Hahn W.C.
Parallel genome-scale loss of function screens in 216 cancer cell lines for the identification of context-specific genetic dependencies.
Sci. Data 1:140035-140035(2014)
PubMed=25877200; DOI=10.1038/nature14397
Yu M., Selvaraj S.K., Liang-Chu M.M.Y., Aghajani S., Busse M., Yuan J., Lee G., Peale F.V., Klijn C., Bourgon R., Kaminker J.S., Neve R.M.
A resource for cell line authentication, annotation and quality control.
Nature 520:307-311(2015)
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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.
慢性粒细胞白血病,简称慢粒,为慢性白血病中最常见一种类型。慢粒起病缓慢,早期多无明显症状,往往在体格检查或其他疾病就诊时偶然发现脾肿大或白细胞异常而获得确诊。 在我国,慢性白血病中以慢粒最为常见,患者年龄在30-40岁者居多,20岁以下罕见。慢粒在临床上可分为慢性期,加速期及急变期。病人出现急性白血病的临床及血液等表现,称之为慢粒急变。多数患者中数生存期为3-4年。慢粒发生急变后预后极差。 临床表现 1.起病缓慢,部分病人早期可以没有任何症状。 2.乏力
佚名 毛细胞 白血病 (hairy cell leukemia)是一种少见的慢性白血病,其主要特点为白血病细胞胞浆形成细长的突起,形似绒毛,在扫描电镜(图11-8)、透射电镜或相差显微镜下清晰可见,在一般光学显微镜下也可见到,故称毛细胞。关于毛细胞的来源意见不一。过去曾认为毛细胞来源于单核巨噬细胞。细胞标记研究证明绝大多数毛细胞
白血病时粒细胞的改变: ①胞体:大小不等、畸形。 ②胞浆:Auer小体,颗粒粗大、增多医学`教育网搜集整理。 Auer小体:是在细胞浆内出现结构均匀一致的红色细棒状小体。产生原因是嗜天青颗粒融合而成。常见于急性非淋巴细胞性白血病细胞浆内。 ③胞核:畸形、切迹、折叠、凹陷、扭曲、分叶等。如急淋时核易破碎,核分裂象增多。 ④核浆比:增大、发育不平衡(M2b)。 ⑤核仁:大、数量增多、亦可不清楚。
技术资料
