| DC67403 |
KRAS ligand 4
Featured
|
KRAS ligand 4 (compound 2) is a SOS1-targeting bifunctional molecular glue that suppresses oncogenic signaling by degrading key KRAS pathway components, evidenced by reduced pERK and pS6 levels. It demonstrates broad-spectrum activity against diverse KRAS mutations, disrupting proliferation across resistant cancer models. |
|
| DC67404 |
QS-57
Featured
|
QS-57 is a bifunctional degrader that combines BRD4-targeting PROTAC activity with 14-3-3 molecular glue properties. |
|
| DC67405 |
Acetyl-cyclosporin A aldehyde
Featured
|
Acetyl-cyclosporin A aldehyde is a chemically modified derivative of cyclosporin A (HY-B0579), featuring an acetyl group and a reactive aldehyde moiety. The parent compound, cyclosporin A, is a dual-function molecule that both inhibits calmodulin signaling and binds cyclophilin, thereby blocking NF-AT nuclear translocation and inducing mitochondrial dysfunction. |
|
| DC67406 |
EM12-FS
Featured
|
EM12-FS is a bifunctional CRBN modulator that engages cereblon at His353 while functioning as a molecular glue to induce NTAQ1 degradation. Demonstrating favorable pharmacokinetics, it exhibits a human plasma half-life of 196 minutes, supporting its therapeutic potential. |
|
| DC67407 |
IKZF1-degrader-1
Featured
|
IKZF1-degrader-1 (Compound 9-B) is a highly potent molecular glue that achieves sub-nanomolar degradation of IKZF1 (DC50 = 0.134 nM), demonstrating significant therapeutic potential for targeting IKZF1-dependent malignancies. |
|
| DC67410 |
MRT-10350
Featured
|
|
|
| DC67411 |
MRT-7612
Featured
|
|
|
| DC67412 |
MRT-3486
Featured
|
|
|
| DC67413 |
MRT-23227
Featured
|
|
|
| DC67415 |
4’-α-C-Methyluridine
Featured
|
4’-α-C-Methyluridine represents a structurally modified uridine analog with significant pharmacological potential. As a nucleoside derivative, it shares structural similarities with uridine—a compound recognized for its antiepileptic properties—while offering enhanced metabolic stability through its methyl modification. |
|
| DC60818 |
mono-Boc-Br MK-6240 Precursor
Featured
|
mono-Boc-Br MK-6240 Precursor is the precusor of MK-6240.. (18)F]-MK-6240 is a tau positron emission tomography (PET) tracer for neurofibrillary tangles (NFTs), exhibiting high specificity and selectivity for binding to NFTs . |
|
| DC67417 |
BAY 3389934
Featured
|
BAY 3389934 represents an innovative dual-action anticoagulant that simultaneously inhibits both Factor IIa (thrombin) and Factor Xa in the coagulation cascade. This unique mechanism provides comprehensive anticoagulation while demonstrating organ-protective properties in severe infections. |
|
| DC67418 |
Ulacamten
Featured
|
Ulacamten is a novel, highly selective cardiac myosin inhibitor that directly targets the contractile machinery of heart muscle cells. |
|
| DC67419 |
PF-07853578
Featured
|
PF-07853578 (Example 11) is a highly potent and selective targeted protein degrader that effectively reduces PNPLA3 levels with an EC50 of 8 nM. |
|
| DC67420 |
AZD2389
Featured
|
AZD2389 represents a novel, orally bioavailable fibroblast activation protein (FAP) inhibitor with significant therapeutic potential. |
|
| DC67421 |
Enozertinib
Featured
|
Enozertinib is a next-generation EGFR tyrosine kinase inhibitor demonstrating potent antineoplastic effects against EGFR-driven malignancies. |
|
| DC67422 |
Alixorexton( ALKS 2680)
Featured
|
Alixorexton is a selective orexin-2 receptor (OX2R) agonist demonstrating significant metabolic modulation potential. |
|
| DC67423 |
BMS-986238
Featured
|
BMS-986238 represents an advanced macrocyclic peptide therapeutic that demonstrates potent and selective inhibition of PD-L1 immune checkpoint signaling. |
|
| DC67424 |
RP-1664
Featured
|
RP-1664 is a novel, orally bioavailable inhibitor that selectively targets polo-like kinase 4 (PLK4) with high potency. |
|
| DC67425 |
BMS-986458
Featured
|
BMS-986458 represents a breakthrough in targeted protein degradation as a first-in-class, orally available PROTAC® molecule that specifically degrades B-cell lymphoma 6 (BCL6). |
|
| DC67426 |
PRT3789
Featured
|
PRT3789 is a first-in-class proteolysis-targeting chimera (PROTAC) that selectively degrades SMARCA2 (BRM) while exhibiting minimal activity against its closely related paralog SMARCA4 (BRG1). |
|
| DC67427 |
FG-2101
Featured
|
FG-2101 represents a next-generation antibacterial agent as a potent, orally bioavailable non-hydroxamate inhibitor of LpxC – a key enzyme in Gram-negative bacterial lipopolysaccharide biosynthesis. |
|
| DC60819 |
MSD199
Featured
|
MSD199 is a potent, and selective Nav1.8 inhibitor with IC50 of 4.7 nM in Qube automated patch-clamp assay, >2000-fold selective over all other Nav isoforms. |
|
| DC60820 |
TAS3351
Featured
|
TAS3351 is a fourth-generation EGFR-TKI overcoming T790M and C797S-mediated resistance in NSCLC with common mutations. TAS3351 exhibites almost comparable inhibitory potency against cellular phosphorylation of EGFR harboring ex19del or L858R with or without C797S and/or T790M while sparing wild type EGFR activity. |
|
| DC60821 |
Lipid TOT-5
Featured
|
TOT-5, a tri-oleoyl-Tris ionizable lipid (pKa 6.2), enables splenic B cell-targeted mRNA delivery via 15% DSPC-incorporated LNPs. Its charge-neutral, hydrophobic surface minimizes hepatic ApoE uptake and enhances complement C3 adsorption, facilitating CD21/35-mediated uptake by marginal zone B cells. In vivo, intravenous 15%DSPC-LNPs showed 8-fold higher spleen-to-liver luciferase expression vs 3%DSPC, with anti-CD21/35 blocking 60% B cell uptake. Intramuscular administration induced robust OVA-specific IgG (10^5 titer) and CTL responses (3.5% tetramer+ CD8+ T cells) while reducing hepatotoxicity (ALT/AST levels ≤40 U/L vs SM-102-LNPs' 80-120 U/L). Cryo-ET confirmed stable lamellar structures (80-100 nm, ζ-potential -2 mV). This formulation achieves safe, ligand-free splenic targeting for mRNA vaccines. |
|
| DC67428 |
AMG-193
Featured
|
AMG 193 represents a novel class of targeted cancer therapeutics as an orally bioavailable, methylthioadenosine (MTA)-dependent PRMT5 inhibitor. |
|
| DC67429 |
(5-METHOXY-3-OXO-2,3-DIHYDRO-1H-ISOINDOL-1-YL)ACETIC ACID
Featured
|
|
|
| DC67430 |
1H-Benzimidazol-6-amine,2-(4-thiazolyl)-
Featured
|
|
|
| DC67431 |
TPBM
Featured
|
TPBM represents a novel class of selective estrogen receptor α (ERα) modulators with a unique mechanism of action. |
.gif)
|
| DC67432 |
Acriflavinium chloride
Featured
|
|
|
DC Chemicals' products qualify for U.S. tariff exemptions. We guarantee no price increases due to customs duties and maintain stable supply, continuing to deliver reliable research solutions to our American clients.
