MC1568

Catalog No.S1484 Batch:S148401

Technical Data

Formula	C₁₇H₁₅FN₂O₃
Molecular Weight	314.31	CAS No.	852475-26-4
Solubility (25°C)*	In vitro	DMSO	13 mg/mL (41.36 mM)
		Water	Insoluble
		Ethanol	Insoluble
* <1 mg/ml means slightly soluble or insoluble. * Please note that Selleck tests the solubility of all compounds in-house, and the actual solubility may differ slightly from published values. This is normal and is due to slight batch-to-batch variations. * Room temperature shipping (Stability testing shows this product can be shipped without any cooling measures.)

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Biological Activity

Description

MC1568 is a selective HDAC inhibitor for maize HD1-A with IC50 of 100 nM in a cell-free assay. It is 34-fold more selective for HD1-A than HD1-B.

Targets

HD1-A (Maize) ^[1] (Cell-free assay)	HD1-B (Maize) ^[1] (Cell-free assay)
100 nM	3.4 μM

In vitro

MC1568 is a selective class II (IIa) histone deacetylas (HDAC II) inhibitor with IC50 of 220 nM and 176-fold class II selectivity (against class I). In human breast cancer ZR-75.1 cell lysates, MC1568 (5 μM) shows no inhibitory activity against HDAC1 but is able to inhibit HDAC4. ^[1] In MCF-7 cells, MC1568 (20 μM) increases the accumulation of acetylated H3 and H4 histones, as well as the levels of acetyl-tubulin, which indicates a inhibitory effect of MC1568 on HDAC6. ^[2] In C2C12 cells, MC1568 (5 μM) arrests myogenesis by decreasing myocyte enhancer factor 2D (MEF2D) expression, stabilizing the HDAC4-HDAC3-MEF2D complex, and by inhibiting differentiation-induced MEF2D acetylation. ^[3] MC1568 (5 or 10 μM) interferes with the RAR- and PPARγ-mediated differentiation-inducing signaling pathways. In F9 cells, MC1568 specifically blocks endodermal differentiation despite not affecting retinoic acid-induced maturation of promyelocytic NB4 cells. In 3T3-L1 cells, MC1568 attenuates PPARγ-induced adipogenesis. ^[4]

In vivo

In mice, MC1568 (50 mg/kg) shows an apparent tissue-selective HDAC inhibition. In skeletal muscle and heart, MC1568 inhibits the activity of HDAC4 and HDAC5 without affecting HDAC3 activity, thereby leaving MEF2-HDAC complexes in a repressed state. ^[3] In reporting PPRE-Luc mice, MC1568 (50 mg/kg) impairs PPARγ signaling mostly in the heart and adipose tissues. ^[4] In a recent study of pancreatic explants, MC1568 enhances expression of Pax4, a key factor required for proper β-and δ-cell differentiation and amplifies endocrine β- and δ-cells. ^[5]

Protocol (from reference)

Kinase Assay:^{^[1]}	Maize HD2, HD1-B, and HD1-A Enzyme Inhibition. The enzyme liberats tritiated acetic acid from the substrate, which is quantified by scintillation counting. IC50 values are results of triple determinations. A 50 μL sample of maize enzyme (at 30 °C) is incubated (30 min) with 10 μL of total [³H]acetate-prelabeled chicken reticulocyte histones (2 mg/mL). Reaction is stopped by addition of 50 μL of 1 M HCl/0.4 M acetate and 800 μL of ethyl acetate. After centrifugation (1×10⁴ g, 5 min), an aliquot of 600 μL of the upper phase is counted for radioactivity in 3 mL of liquid scintillation cocktail. MC1568 is tested at a starting concentration of 40 μM, and active substances are diluted further. NaB, VPA, TSA, SAHA, ⁸⁵ TPX, HC-toxin, and tubacin are used as the reference compounds, and blank solvents are used as negative controls.
Cell Assay:^{^[4]}	Cell lines 3T3-L1 cells Concentrations ~10 μM, dissolved in DMSO Incubation Time 8 days Method The 3T3-L1 cells are propagated and differentiated using a cocktail of isobutylmethylxanthine and insulin. From the second day post-confluence and throughout the differentiation period of 8 days, the 3T3-L1 cells are induced by: (1) no induction: at post-confluence and throughout the differentiation period of 8 days, the cells are incubated with DMSO or MC1568. (2) troglitazone: at post-confluence and throughout the differentiation period of 8 days, the cells are induced with 5 μM troglitazone, MC1568 or both. (3): at post-confluence and throughout the differentiation period of 8 days, the cells are incubated with either DMSO or MC1568.
Animal Study:^{^[4]}	Animal Models PPRE-Luc transgenic mouse (C57BL/6) Dosages 50 mg/kg Administration By gavage once a day

References

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Customer Product Validation

: Data from [Proc Natl Acad Sci U S A, 2012, 109(34)]

: Data from [Proc Natl Acad Sci U S A, 2012, 109(34)]

: Data from [PLoS One, 2012, 7(12), e52095]

: Data from [J Biol Chem, 2011, 286, 23842–23851]

Selleck's MC1568 has been cited by 50 publications

Global isonicotinylome analysis identified SMAD3 isonicotinylation promotes liver cancer cell epithelial-mesenchymal transition and invasion [ iScience, 2024, 27(9):110775]	PubMed: 39286495
Selective Inhibition of Histone Deacetylase Class IIa With MC1568 Ameliorates Podocyte Injury [ Front Med (Lausanne), 2022, 9:848938]	PubMed: 35492337
HBV covalently closed circular DNA minichromosomes in distinct epigenetic transcriptional states differ in their vulnerability to damage [ Hepatology, 2021, 10.1002/hep.32245]	PubMed: 34779008
HBV covalently closed circular DNA minichromosomes in distinct epigenetic transcriptional states differ in their vulnerability to damage [ Hepatology, 2021, 10.1002/hep.32245]	PubMed: 34779008
Butyrate and Class I Histone Deacetylase Inhibitors Promote Differentiation of Neonatal Porcine Islet Cells into Beta Cells [ Cells, 2021, 10(11)3249]	PubMed: 34831471
Epigenetic Repression of Chloride Channel Accessory 2 Transcription in Cardiac Fibroblast: Implication in Cardiac Fibrosis [ Front Cell Dev Biol, 2021, 9:771466]	PubMed: 34869368
HDAC8 cooperates with SMAD3/4 complex to suppress SIRT7 and promote cell survival and migration. [ Nucleic Acids Res, 2020, 6;48(6):2912-2923]	PubMed: 31970414
Valproate reverses mania-like behaviors in mice via preferential targeting of HDAC2 [ Mol Psychiatry, 2020, 10.1038/s41380-020-00958-2]	PubMed: 33235333
Valproic acid upregulates the expression of the p75NTR/sortilin receptor complex to induce neuronal apoptosis [ Apoptosis, 2020, 10.1007/s10495-020-01626-0]	PubMed: 32712736
ΔNp63α promotes the expression and nuclear translocation of PTEN, leading to cisplatin resistance in oral cancer cells [ Am J Transl Res, 2020, 12(10):6187-6203]	PubMed: 33194023

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SHIPPING AND STORAGE
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