Signaling Pathways
Signal transduction pathways constitute a precisely regulated network through which cells perceive external stimuli and initiate intracellular responses. Core research in this field focuses on the mechanisms of molecular signal transmission and regulation within cells and typically encompasses three fundamental stages: signal initiation, signal propagation through cascades, and downstream effector responses. Key molecules—including proteins, nucleic acids, and small molecules—interact with high specificity and are subject to tight regulation (e.g., protein phosphorylation, molecular activation/inhibition). These processes underpin the full spectrum of cellular activities, including proliferation, differentiation, metabolism, apoptosis, and immune responses. While accurate regulation of these pathways is essential for maintaining organismal homeostasis, their dysregulation is a major driver of the onset and progression of diseases such as cancer, neurodegenerative disorders, and autoimmune diseases.
APExBIO is strongly committed to advancing life science research by providing a comprehensive portfolio of small-molecule tools designed to support the elucidation of signaling mechanisms and the identification of key regulatory targets—critical steps for deciphering disease etiology and developing innovative therapies. Our offerings span all major signal transduction pathways, including classical pathways (e.g., PI3K/Akt, MAPK, NF-κB), emerging modalities (e.g., ferroptosis, cuproptosis, pyroptosis), and research on pathway crosstalk. With tens of thousands of products—including inhibitors, activators, and modulators—we robustly support research in oncology, immunology, neuroscience, epigenetics, and other key fields.
Every APExBIO product undergoes rigorous functional validation and purity testing, ensuring suitability for diverse research applications such as pathway mechanism studies, target identification and validation, drug activity evaluation, cell-based assays, and animal model development. We complement our high-quality tools with comprehensive support: each product is supplied with detailed chemical property reports, biological activity data, standardized usage guidelines, and extensive literature citations in high-impact journals. In addition, we provide end-to-end assistance—from product selection and experimental protocol optimization to technical troubleshooting—enabling researchers to rely on tool quality, focus on core scientific questions, and accelerate progress in signal transduction research and translational medicine.
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BA1327 HexetidineSummary: Hexetidine (NSC-17764) is an orally active antimicrobial agent with broad antibacterial and antifungal activity. - BA1377 HalazoneSummary: An organic chloramine broad-spectrum bactericidal disinfectant, whose core bioactivities are water disinfection/sterilization and modulation of neuronal sodium channel function.
- BA1486 A40926Summary: A40926, the precursor of dalbavancin, has core bioactivity in inhibiting the growth of Gram-positive bacteria and Neisseria gonorrhoeae, with its target being the bacterial cell wall synthesis pathway.
- BA1665 OteseconazoleSummary: Oteseconazole (VT-1161) is a potent and selective tetrazole CYP51 (lanosterol 14α-demethylase) inhibitor, with core bioactivity of inhibiting the growth of Candida and other fungi.
- BA1710 TriacetinSummary: A short-chain triacylglycerol with core bioactivities including antitumor effects, metabolic regulation, and anti-adipogenesis
- BA1790 HaloproginSummary: Haloprogin is an effective antifungal agent with activity against dermatophytes, Candida, and a limited range of Gram-positive bacteria.
- BA1816 EntecavirSummary: Potent and selective inhibitor of HBV DNA polymerase (reverse transcriptase), with core bioactivity of inhibiting replication of chronic hepatitis B virus (HBV).
- BA1823 BifendateSummary: Bifendate (DDB) is a synthetic intermediate of Schisandrin C, with core biological activities focused on hepatoprotection, regulation of lipid metabolism, and inhibition of autophagy.