Abemaciclib (Synonyms: LY2835219)

目錄號: HY-16297A 純度: 99.94%: FAQs
Data Sheet SDS COA 產(chǎn)品使用指南

摩爾計算器

Abemaciclib (LY2835219) 是具有選擇性的 CDK4/6 抑制劑，能夠抑制 CDK4/CDK6 的活性，IC₅₀ 分別為 2 nM 和 10 nM。

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Abemaciclib Chemical Structure

CAS No. : 1231929-97-7

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規(guī)格	價格	是否有貨
5 mg	￥600	In-stock
10 mg	￥900	In-stock
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200 mg	￥1900	In-stock
500 mg	￥3500	In-stock
1 g	￥5600	In-stock
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Customer Review

Other Forms of Abemaciclib:

MCE 顧客使用本產(chǎn)品發(fā)表的 81 篇科研文獻

•Cancer Cell. 2024 Aug 27:S1535-6108(24)00305-2. [Abstract]
•Cell. 2023 Jun 8;186(12):2628-2643.e21. [Abstract]
•Cell. 2018 Nov 1;175(4):984-997.e24. [Abstract]
•Nature. 2017 Aug 24;548(7668):471-475. [Abstract]
•Cancer Discov. 2023 Dec 4. [Abstract]
•Nature Cancer. 2021 Apr;2(4):429-443. [Abstract]

•Nat Metab. 2020 Jan;2(1):41-49. [Abstract]
•Bioact Mater. 8 September 2021.
•Adv Funct Mater. 2021 Apr 30.
•Sci Transl Med. 2018 Jul 18;10(450). pii: eaaq1093. [Abstract]
•EMBO J. 2024 Aug 19. [Abstract]
•Clin Cancer Res. 2024 May 8. [Abstract]
•Cancer Res. 2023 Jun 29;CAN-23-0705. [Abstract]
•Nat Commun. 2022 Aug 10;13(1):4689. [Abstract]
•Adv Sci (Weinh). 2022 Aug 2;e2201834. [Abstract]
•Cancer Res. 2022 May 16;82(10):1890-1908. [Abstract]
•J Exp Clin Cancer Res. 2022 Apr 21;41(1):149. [Abstract]
•Blood Cancer J. 2022 Jan 11;12(1):5. [Abstract]
•EMBO J. 2022 Jan 5;e108946. [Abstract]
•Nat Commun. 2021 Nov 16;12(1):6607. [Abstract]
•Nat Commun. 2021 Aug 25;12(1):5112. [Abstract]
•Adv Sci (Weinh). 2020 Aug 4;7(18):2000906. [Abstract]
•Cancer Res. 2019 Oct 15;79(20):5245-5259. [Abstract]
•Nat Commun. 2019 Jun 28;10(1):2860. [Abstract]
•Mol Cell. 2017 Oct 19;68(2):336-349.e6. [Abstract]
•Nat Commun. 2017 Jun 27;8:15916. [Abstract]
•Cancer Res. 2017 May 1;77(9):2488-2499. [Abstract]
•Cancer Res. 2016 Nov 15;76(22):6723-6734. [Abstract]
•Sci Data. 2024 Sep 19.
•Cell Rep. 2022 Dec 20;41(12):111826. [Abstract]
•Cell Rep. 2022 Sep 13;40(11):111331. [Abstract]
•ACS Appl Mater Interfaces. 2022 May 11;14(18):20628-20640. [Abstract]
•Br J Cancer. 2022 Jan 14. [Abstract]
•Cell Death Dis. 2020 Oct 28;11(10):925. [Abstract]
•Cell Chem Biol. 2019 Aug 15;26(8):1067-1080.e8. [Abstract]
•Cell Death Dis. 2019 Mar 20;10(4):271. [Abstract]
•Int J Biol Sci. 2019 Jan 1;15(3):522-532. [Abstract]
•Cell Rep. 2017 Oct 31;21(5):1386-1398. [Abstract]
•J Med Chem. 2023 Mar 6. [Abstract]
•JCI Insight. 2021 Dec 21;e154402. [Abstract]
•NPJ Precis Oncol. 2021 Mar 19;5(1):20. [Abstract]
•Breast Cancer Res. 2019 Dec 26;21(1):150. [Abstract]
•Mol Oncol. 2017 Aug;11(8):1035-1049. [Abstract]
•Mol Cancer Ther. 2024 Jun 19. [Abstract]
•Sci Rep. 2024 May 8;14(1):10582. [Abstract]
•Sci Rep. 2022 Jul 20;12(1):12420. [Abstract]
•Int J Mol Sci. 2022 Feb 24;23(5):2493. [Abstract]
•Front Oncol. 2021 Jul 13;11:704042. [Abstract]
•Commun Biol. 2021 Mar 25;4(1):399. [Abstract]
•Int J Mol Sci. 2021 Jan 8;22(2):E575. [Abstract]
•Sci Rep. 2019 Oct 22;9(1):15099. [Abstract]
•Nutrition. 2019 Apr;60:217-226. [Abstract]
•Biochem Pharmacol. 2017 Jan 15;124:29-42. [Abstract]
•Transl Lung Cancer Res. 2024 May 31;13(5):1032-1046. [Abstract]
•Heliyon. 2023 Sep 13.
•J Cell Biochem. 2023 Aug 11. [Abstract]
•Naunyn Schmiedebergs Arch Pharmacol. 2023 Feb 4. [Abstract]
•Biochem Biophys Res Commun. 20 December 2021.
•Fundam Clin Pharmacol. 2021 Feb 1. [Abstract]
•R Soc Open Sci. 2019 Jan 23;6(1):181714. [Abstract]
•Biochem Biophys Res Commun. 2018 Sep 26;504(1):231-237. [Abstract]
•Eur J Drug Metab Pharmacokinet. 2021 Jul 18;1-11. [Abstract]
•Biomed Chromatogr. 2020 Jun;34(6):e4825. [Abstract]
•SSRN. 2023 Sep 29.
•bioRxiv. 2023 Jul 17.
•bioRxiv. 2023 Jul 19.
•University of Gothenburg. 2023 Jun 27.
•bioRxiv. 2023 Jan 25.
•SSRN. 2022 Nov 21.
•Leuk Res. September 2022, 106920.
•J Oncol. 2022 Jun 23;2022:8724933. [Abstract]
•Biochem Biophys Rep. 27, September 2021, 101099
•Department of Biochemistry. 2020 Oct.
•STAR Protocols. 2020 Jun 3;1(1):100024. [Abstract]
•bioRxiv. 2020 Jun.
•Patent. US20200108066A1
•J Oncol. 2019 Jun 2;2019:5952836. [Abstract]
•Biochim Biophys Acta. 2017 Nov 20;1865(2):354-363. [Abstract]
•Oncotarget. 2017 Jul 27;8(56):95116-95134. [Abstract]
•Oncotarget. 2017 Jun 27;8(40):67422-67438. [Abstract]
•Harvard Medical School LINCS LIBRARY

: Abemaciclib purchased from MCE. Usage Cited in: Nature. 2017 Aug 24;548(7668):471-475. [Abstract]; Western blot of SKBR3, BT474, MDA-MB-453, and MDA-MB-361 cells treated with DMSO, GW572016, or Abemaciclib for 48?h. Western blot of MDA-MB-453 cells pretreated with DMSO or Abemaciclib (500?nM) for 0, 1, or 7 days before exposure to Staurosporine (500?nM) for 4?h.

: Abemaciclib purchased from MCE. Usage Cited in: Cancer Res. 2017 May 1;77(9):2488-2499. [Abstract]; Treatment with PD 0332991 and Abemaciclib shows an induction of S241 P-PDK1 as early as 1 h after drug exposure without an increased in total PDK1 protein.

: Abemaciclib purchased from MCE. Usage Cited in: Mol Oncol. 2017 Aug;11(8):1035-1049. [Abstract]; Effects of CDK4/6 inhibitors on AMPK phosphorylation and apoptosis-related signals. After 24 h of drug treatment, the cells are subjected to western blot analysis. AMPK phosphorylation level is quantified by the ratio of band intensities of phospho-AMPKα vs. AMPKα.

: Abemaciclib purchased from MCE. Usage Cited in: Biochem Pharmacol. 2017 Jan 15;124:29-42. [Abstract]; Effect of LY2835219 on the expression of ABCB1 or ABCG2 in MDR cells. The protein level of ABCB1 and ABCG2 on MDR cells after 0, 0.1, 0.2 and 0.4 μM LY2835219 stimulation for 48h are measured by Western blot analysis, and mRNA level are measured by PCR (GAPDH as loading control).

: Abemaciclib purchased from MCE. Usage Cited in: Oncotarget. 2017 Jul 27;8(56):95116-95134. [Abstract]; Abemaciclib causes increased PARP cleavage in RCC. In 786-O cells Abemaciclib exposure results in increased PARP cleavage. This effect is more rapid and pronounced when Abemaciclib is combined with SU 11248.

: Abemaciclib purchased from MCE. Usage Cited in: Oncotarget. 2017 Jul 27;8(56):95116-95134. [Abstract]; Abemaciclib causes increased PARP cleavage in RCC. In Caki-1 cells Abemaciclib exposure results in increased PARP cleavage. This effect is more rapid and pronounced when Abemaciclib is combined with SU 11248.

: Abemaciclib purchased from MCE. Usage Cited in: Oncotarget. 2017 Jun 27;8(40):67422-67438. [Abstract]; GTSE1 protein and mRNA levels in MDA-MB-157 and MDA-MB-231 cell lines treated respectively with Abemaciclib 0.5 μM for 24h. Data are presented as mean±SEM of three independent experiments.

: Abemaciclib purchased from MCE. Usage Cited in: Cancer Res. 2016 Nov 15;76(22):6723-6734. [Abstract]; The effects of the CDK inhibitor Abemaciclib, PD 0332991 and Ribocilib on Trop2 ICD cleavage. CDK inhibitors decrease Trop2 ICD abundance after the 2^nd day of CDK inhibitor treatment.

Abemaciclib 相關(guān)產(chǎn)品

•相關(guān)化合物庫:

•同靶點產(chǎn)品:

•同靶點蛋白產(chǎn)品:

查看 CDK 亞型特異性產(chǎn)品:

查看所有亞型

CDK1 CDK2 CDK3 CDK4 CDK5 CDK6 CDK7 CDK8 CDK9 CDK11 CDK12 CDK13 CDK14 CDK16 CDK19 CDC CLK Pho85

生物活性
實驗參考方法
純度 & 產(chǎn)品資料
參考文獻

生物活性

Abemaciclib (LY2835219) is a selective CDK4/6 inhibitor with IC₅₀ values of 2 nM and 10 nM for CDK4 and CDK6, respectively.

IC₅₀ & Target^[3]

Cdk4/cyclin D1

2 nM (IC₅₀)

CDK6/cyclinD1

10 nM (IC₅₀)

CDK9/cyclinT1

57 nM (IC₅₀)

CDK5/p35

287 nM (IC₅₀)

Cdk5/p25

355 nM (IC₅₀)

CDK2/cyclinE

504 nM (IC₅₀)

CDK7/Mat1/cyclinH1

3910 nM (IC₅₀)

CDK1/cyclinB1

1627 nM (IC₅₀)

PIM1

50 nM (IC₅₀)

PIM2

3400 nM (IC₅₀)

HIPK2

31 nM (IC₅₀)

DYRK2

61 nM (IC₅₀)

CK2

117 nM (IC₅₀)

GSK3b

192 nM (IC₅₀)

JNK3

389 nM (IC₅₀)

FLT3 (D835Y)

403 nM (IC₅₀)

FLT3

3960 nM (IC₅₀)

DRAK1

659 nM (IC₅₀)

體外研究
(In Vitro)

Abemaciclib reduces cell viability with the IC₅₀ values ranging from 0.5 μM to 0.7 μM, inhibits Akt and ERK signaling but not mTOR activation at head and neck squamous cell carcinoma (HNSCC) cells^[1]. Abemaciclib shows inhibition on A375R1-4, M14R, and SH4R with EC₅₀ values ranging from 0.3 to 0.6 μM; Abemaciclib inhibits the proliferation of the parental A375 and resistant A375RV1 and A375RV2 cells with similar potencies with IC₅₀ values of 395, 260, and 463 nM, respectively^[2]. Abemaciclib inhibits CDK4 and CDK6 with low nanomolar potency, inhibits Rb phosphorylation resulting in a G1 arrest and inhibition of proliferation, and its activity is specific for Rb-proficient cells^[3].

MCE has not independently confirmed the accuracy of these methods. They are for reference only.

體內(nèi)研究
(In Vivo)

Abemaciclib (45 mg/kg, p.o.) in combination with RAD001 causes a cooperative antitumor effect in HNSCC xenograft tumor^[1]. Abemaciclib (45 or 90 mg/kg, p.o.) shows significant tumor growth inhibition in an A375 xenograft model^[2].

MCE has not independently confirmed the accuracy of these methods. They are for reference only.

Clinical Trial

分子量

506.59

Formula

C₂₇H₃₂F₂N₈

CAS 號

1231929-97-7

性狀

固體

顏色

Off-white to yellow

運輸條件

Room temperature in continental US; may vary elsewhere.

儲存方式

4°C, protect from light

*In solvent : -80°C, 6 months; -20°C, 1 month (protect from light)

溶解性數(shù)據(jù)

細胞實驗：

DMSO 中的溶解度 : 2.94 mg/mL (5.80 mM; 超聲助溶 (<80°C); 吸濕的 DMSO 對產(chǎn)品的溶解度有顯著影響，請使用新開封的 DMSO)

H₂O 中的溶解度 : < 0.1 mg/mL (insoluble)

配制儲備液

濃度溶劑體積質(zhì)量	1 mg	5 mg	10 mg

1 mM	1.9740 mL	9.8699 mL	19.7398 mL
5 mM	0.3948 mL	1.9740 mL	3.9480 mL
10 mM	---	---	---

查看完整儲備液配制表

* 請根據(jù)產(chǎn)品在不同溶劑中的溶解度選擇合適的溶劑配制儲備液；一旦配成溶液，請分裝保存，避免反復(fù)凍融造成的產(chǎn)品失效。
儲備液的保存方式和期限：-80°C, 6 months; -20°C, 1 month (protect from light)。-80°C儲存時，請在6個月內(nèi)使用，-20°C儲存時，請在1個月內(nèi)使用。

摩爾計算器
稀釋計算器

Mass (g) = Concentration (mol/L) × Volume (L) × Molecular Weight (g/mol)

Concentration _(start) × Volume _(start) = Concentration _(final) × Volume _(final)

This equation is commonly abbreviated as: C₁V₁ = C₂V₂

濃度 _(start)

體積 _(start)

濃度 _(final)

體積 _(final)

動物實驗：

以下溶解方案，請直接配制工作液。建議現(xiàn)用現(xiàn)配，在短期內(nèi)盡快用完。以下溶劑前顯示的百分比是指該溶劑在您配制終溶液中的體積占比；如在配制過程中出現(xiàn)沉淀、析出現(xiàn)象，可以通過加熱和/或超聲的方式助溶。

方案一

請依序添加每種溶劑： 0.5% Hydroxyethyl cellulose in Water
Solubility: 3.33 mg/mL (6.57 mM); 懸濁液; 超聲助溶

動物溶解方案計算器

請輸入動物實驗的基本信息：

給藥劑量

mg/kg

動物的平均體重

每只動物的給藥體積

μL

動物數(shù)量

只

由于實驗過程有損耗，建議您多配一只動物的量

計算結(jié)果

工作液所需濃度 : mg/mL

純度 & 產(chǎn)品資料

純度: 99.94%

選擇批次：

Data Sheet (618 KB) SDS (419 KB)

COA (282 KB) LCMS (90 KB) 元素分析報告 (205 KB)

產(chǎn)品使用指南 (1538 KB)

參考文獻

[1]. Ku BM, et al. The CDK4/6 inhibitor LY2835219 has potent activity in combination with mTOR inhibitor in head and neck squamous cell carcinoma. Oncotarget.?2016 Mar 22;7(12):14803-13. [Content Brief]

[2]. Yadav V, et al. The CDK4/6 inhibitor LY2835219 overcomes PLX4032 resistance resulting from MAPK reactivation and cyclin D1 upregulation. Mol Cancer Ther. 2014 Oct;13(10):2253-63. [Content Brief]

[3]. Gelbert LM, et al. Preclinical characterization of the CDK4/6 inhibitor LY2835219: in-vivo cell cycle-dependent/independent anti-tumor activities alone/in combination with NSC 613327. Invest New Drugs. 2014 Oct;32(5):825-37. [Content Brief]

Cell Assay ^[1]	Cells are seeded in a 96-well plate, allowed to adhere overnight, and treated with DMSO control (0.1% v/v) or the indicated compounds for 72 h. Cell viability and proliferation are determined using a Cell Counting Kit according to the manufacturer's instructions. The interaction between Abemaciclib and mTOR inhibitor is determined using CompuSyn. Combination index (CI) values of 1 indicates and additive drug interaction, whereas a CI of <1 is synergistic and a CI of >1 is antagonistic. MCE has not independently confirmed the accuracy of these methods. They are for reference only.
Animal Administration ^[1]	Six-week-old BALB/c female nude mice are injected subcutaneously with OSC-19 (1×10⁶) cells. When tumor sizes reach approximately 100 mm³, mice are randomized by tumor size and subjected to each treatment. At least 5 mice per treatment group are included. Each group of mice is dosed via daily oral gavage with vehicle, Abemaciclib (45 mg/kg/d or 90 mg/kg/d), RAD001 (5 mg/kg/d), or a combination of both. The Abemaciclib is dissolved in 1% HEC in 20 mM phosphate buffer (pH2.0). Tumor size and body weight are measured twice weekly. Tumor volumes are calculated using the following formula: V=(L×W²)/2. Mice are gavaged a final time on day 14 and sacrificed the following day. The tumors are removed for Western blot and immunohistochemistry. MCE has not independently confirmed the accuracy of these methods. They are for reference only.
參考文獻	[1]. Ku BM, et al. The CDK4/6 inhibitor LY2835219 has potent activity in combination with mTOR inhibitor in head and neck squamous cell carcinoma. Oncotarget.?2016 Mar 22;7(12):14803-13. [Content Brief] [2]. Yadav V, et al. The CDK4/6 inhibitor LY2835219 overcomes PLX4032 resistance resulting from MAPK reactivation and cyclin D1 upregulation. Mol Cancer Ther. 2014 Oct;13(10):2253-63. [Content Brief] [3]. Gelbert LM, et al. Preclinical characterization of the CDK4/6 inhibitor LY2835219: in-vivo cell cycle-dependent/independent anti-tumor activities alone/in combination with NSC 613327. Invest New Drugs. 2014 Oct;32(5):825-37. [Content Brief]

Abemaciclib 相關(guān)分類

完整儲備液配制表

可選溶劑	濃度溶劑體積質(zhì)量	1 mg	5 mg	10 mg	25 mg

DMSO	1 mM	1.9740 mL	9.8699 mL	19.7398 mL	49.3496 mL
DMSO	5 mM	0.3948 mL	1.9740 mL	3.9480 mL	9.8699 mL

Help & FAQs

Do most proteins show cross-species activity?
Species cross-reactivity must be investigated individually for each product. Many human cytokines will produce a nice response in mouse cell lines, and many mouse proteins will show activity on human cells. Other proteins may have a lower specific activity when used in the opposite species.

Keywords:

Abemaciclib1231929-97-7LY2835219LY 2835219LY-2835219CDKCyclin dependent kinaseInhibitorinhibitorinhibit

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Abemaciclib (Synonyms: LY2835219)

Customer Review

Other Forms of Abemaciclib:

MCE 顧客使用本產(chǎn)品發(fā)表的 81 篇科研文獻