RPMI 1640 培养基
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RPMI 1640 培养基
引用和文献 (44)
Gibco™

RPMI 1640 培养基

RPMI 1640 培养基最初是为了悬浮培养人白血病单层细胞而开发的。Roswell Park Memorial Institute (RPMI) 1640 培养基被发现适用于多种哺乳动物细胞,包括了解更多信息
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货号数量
11875101100 mL
1187512720 x 100 mL
11875093500 mL
1187511910 x 500 mL
118750851000 mL
118751356 x 1000 mL
货号 11875101
价格(CNY)
194.40
飞享价
Ends: 31-Dec-2025
248.00
共减 53.60 (22%)
Each
添加至购物车
数量:
100 mL
Customize this product
价格(CNY)
194.40
飞享价
Ends: 31-Dec-2025
248.00
共减 53.60 (22%)
Each
添加至购物车
RPMI 1640 培养基最初是为了悬浮培养人白血病单层细胞而开发的。Roswell Park Memorial Institute (RPMI) 1640 培养基被发现适用于多种哺乳动物细胞,包括 HeLa 细胞、Jurkat 细胞、 MCF-7 细胞、PC12 细胞、PBMC 细胞、星形胶质细胞和癌细胞。针对广泛的细胞培养应用,我们提供多种组分的 RPMI 1640 改良培养基。使用培养基选择工具查找适合的配方。

这种 RPMI 的改良方式如下:
包含  不含
•L-谷氨酰胺  •HEPES:
•酚红 

可提供完整配方

RPMI 的使用
RPMI 1640 培养基相比其他培养基之所以具有独特的效果,是因为其中含有还原剂谷胱甘肽和高浓度的维生素。RPMI 1640 培养基含有生物素、 维生素 B12 以及 PABA,这些成分是 Eagle’s MEM 和DMEM所不具备的。此外,该培养基之中还含有高浓度的维生素肌醇和胆碱。RPMI 1640 培养基不含蛋白质、脂质或生长因子。因此,RPMI 1640 培养基需要添加剂,通常采用 10% 胎牛血清 (FBS)。RPMI 1640 培养基使用碳酸氢钠缓冲系统 (2.0 g/L),因此需要 5–10% CO2 环境来维持生理 pH 值。

cGMP 生产和质量体系
RPMI 1640 培养基在位于纽约格兰德岛的符合 cGMP 要求的工厂内生产。该工厂是在FDA登记的医疗器械生产商,且通过ISO 13485标准认证。为确保供应链连续性,我们同时提供由我们的苏格兰工厂生产的等同 RPMI 1640 产品 (21875-158)。后者亦是在FDA登记的医疗仪器生产商,且符合ISO 13485标准。
仅用于研究和生产用途。不可用于临床诊断或直接用于人类或动物。
规格
细胞系HeLa、Jurkat、MCF-7、PC-12、PBMC、星形胶质细胞和癌细胞
细胞类型白血病细胞
最大浓度1 X
生产质量cGMP-compliant under the ISO 13485 standard
产品线Gibco
产品类型RPMI 1640 培养基(Roswell Park Memorial Institute 1640 培养基)
数量100 mL
有效期自生产之日起 12 个月
运输条件室温
分类非动物源性
形式液体
血清水平标准血清
无菌无菌过滤
灭菌方法无菌过滤
加有添加剂谷氨酰胺, 酚红
不加添加剂不含 HEPES, 不含丙酮酸钠
Unit SizeEach
内容与储存
储存条件:2-8°C。避光储存
运输条件:环境
有效期:自生产之日起 12 个月

常见问题解答 (FAQ)

加入血清后的培养基可以使用多久?

通常情况下,加入血清后的培养基可使用三个星期。尽管没有正式的研究支持数据,这是我们研究人员的经验。

我的培养基是室温条件下运送来的,但注明应保存于冷藏条件下。这会有影响么?

我们会在常温下运输那些需要在冰箱中长期存放的培养基。我们对代表性的培养基配方进行了研究,结果表明这些培养基在室温下放置一周不会有问题。

我该如何去除细胞培养基中的支原体污染?

绝大部分情况下支原体污染无法从培养物中去除,只能弃用。不过也许您的培养物具有独特性,您不希望丢弃而试图去除污染。环丙沙星和Plasmocin据报导适合此种应用。如果对相关实验方案或应用感兴趣,请联系抗生素供应商或参考已发表的文献。请注意支原体很难从培养物中清除,而且容易扩散,所以请对受污染的培养物进行隔离处理,直至支原体被完全清除,另外您的实验室可能也需要彻底净化。

我发现培养物的生长速率变缓。我该如何处理?

尝试更换培养基或血清。比较培养基配方中葡萄糖、氨基酸及其他成份之间的差异。比较新旧批次的血清。增加细胞的初始接种量。最后,让细胞逐步切换到新的培养基。

我的细胞不能贴附于培养容器。我该如何处理?

如果细胞经胰酶过度消化,即可能发生此种情况。尝试使用更短时间或更低浓度的胰酶进行消化处理。支原体污染也可能造成此种问题。分离部分细胞培养物,并检测支原体感染。最后,检查培养基中的粘附因子。

View all RPMI 1640 培养基 FAQs

引用和文献 (44)

引用和文献
Abstract
Receptor-selective effects of endogenous RGS3 and RGS5 to regulate mitogen-activated protein kinase activation in rat vascular smooth muscle cells.
Authors:Wang Qin; Liu Min; Mullah Bashar; Siderovski David P; Neubig Richard R;
Journal:J Biol Chem
PubMed ID:12006602
Regulators of G protein signaling (RGS) proteins compose a highly diverse protein family best known for inhibition of G protein signaling by enhancing GTP hydrolysis by Galpha subunits. Little is known about the function of endogenous RGS proteins. In this study, we used synthetic ribozymes targeted to RGS2, RGS3, RGS5, ... More
Silencing of Transcription of the Human Luteinizing Hormone Receptor Gene by Histone Deacetylase-mSin3A Complex.
Authors: Zhang Ying; Dufau Maria L;
Journal:J Biol Chem
PubMed ID:12091390
'Modification of chromatin structure by histone acetylases and deacetylases is an important mechanism in modulation of eukaryotic gene transcription. The present study investigated regulation of the human luteinizing hormone receptor (hLHR) gene by histone deacetylases. Inhibition of histone deacetylases (HDACs) by trichostatin A (TSA) increased hLHR promoter activity by 40-fold ... More
Distinct Intracellular Signaling in Tumor Necrosis Factor-related Apoptosis-inducing Ligand- and CD95 Ligand-mediated Apoptosis.
Authors: Velthuis Jurjen H L; Rouschop Kasper M A; De Bont Hans J G M; Mulder Gerard J; Nagelkerke J Fred;
Journal:J Biol Chem
PubMed ID:11980895
'Tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) is a potent inducer of apoptosis in tumor cells but not in healthy cells. Similar to CD95 ligand (CD95L), TRAIL signaling requires ligand-receptor interaction; the downstream signaling molecules, such as Fas-associated death domain and caspase-8, also seem similar. Using cells stably expressing TRAIL and ... More
Intercellular calcium signaling occurs between human osteoblasts and osteoclasts and requires activation of osteoclast P2X7 receptors.
Authors: Jørgensen Niklas R; Henriksen Zanne; Sørensen Ole H; Eriksen Erik F; Civitelli Roberto; Steinberg Thomas H;
Journal:J Biol Chem
PubMed ID:11756404
'Signaling between osteoblasts and osteoclasts is important in bone homeostasis. We previously showed that human osteoblasts propagate intercellular calcium signals via two mechanisms: autocrine activation of P2Y receptors, and gap junctional communication. In the current work we identified mechanically induced intercellular calcium signaling between osteoblasts and osteoclasts and among osteoclasts. ... More
Single-cell fluorescence resonance energy transfer analysis demonstrates that caspase activation during apoptosis is a rapid process. Role of caspase-3.
Authors: Rehm Markus; Dussmann Heiko; Janicke Reiner U; Tavare Jeremy M; Kogel Donat; Prehn Jochen H M;
Journal:J Biol Chem
PubMed ID:11964393
'Activation of effector caspases is considered to be the final step in many apoptosis pathways. We transfected HeLa cells with a recombinant caspase substrate composed of cyan and yellow fluorescent protein and a linker peptide containing the caspase cleavage sequence DEVD, and we examined the cleavage kinetics at the single-cell ... More
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