Ying-Chieh Wong

Tandem cyclization of α-cyano α-alkynyl aryl ketones induced by tert-butyl hydroperoxide and tetrabutylammonium iodide.

The radical cascade protocol of the α-cyano α-TMS/aryl-capped alkynyl aryl ketones promoted by tert-butyl hydroperoxide under catalysis with tetrabutylammonium iodide in refluxing benzene has been developed, leading to the construction of a variety of highly functionalized [6,6,5] tricyclic frameworks in an efficient manner.

Discovery of 1‐(2,4‐Dichlorophenyl)‐4‐ethyl‐5‐(5‐(2‐(4‐(trifluoromethyl)phenyl)ethynyl)thiophen‐2‐yl)‐N‐(piperidin‐1‐yl)‐1H‐pyrazole‐3‐carboxamide as a Potential Peripheral Cannabinoid‐1 Receptor Inverse Agonist

Cannabinoid-1 receptor (CB1R) is one of the most abundant neuroregulatory receptors in the brain, and it is involved in regulating feeding and appetite. In addition to expression in brain, this receptor is also found in the peripheral organs, such as adipose tissues, muscle, and liver. In sharp contrast, the structurally closely related cannabinoid-2 receptor (CB2R) is expressed almost exclusively in the immune system and is primarily involved in immune regulation and neurodegeneration. The therapeutic potential of CB1R antagonists has been extensively reviewed, and at least one compound (1; also called rimonabant or SR141716A) has shown clinical evidence of weight reducing action. However, after its launch in 2006, it was subsequently withdrawn (2008) in Europe due to severe psychiatric effects including depression, anxiety and stress disorders. Currently, only two drugs, orlistat and sibutramine, are available for the long-term treatment of obesity; however, both have met with moderate success because of their limited weight-loss efficacy and many accompanying adverse effects, including high blood pressure and flatulence.

Discovery of 1-(2,4-Dichlorophenyl)-N-(piperidin-1-yl)-4-((pyrrolidine-1-sulfonamido)methyl)-5-(5-((4-(trifluoromethyl)phenyl)ethynyl)thiophene-2-yl)-1H-pyrazole-3-carboxamide as a Novel Peripherally Restricted Cannabinoid-1 Receptor Antagonist with Significant Weight-Loss Efficacy in Diet-Induced Obese Mice

After extensive synthetic efforts, we found that many structurally diverse bioisosteres could be generated via derivatizing the C-4 alkyl chain on the pyrazole ring of compound 3 (B/P = 1/33) with different electronegative groups. Especially when a sulfonamide or sulfamide moiety was added, resulting compounds exhibited not only potent CB1R activity but also a desired tPSA value over 90 Å(2), a threshold considered to possess a low probability to cross BBB, leading to the identification of compound 4 (B/P = 1/64) as a peripherally restricted CB1R antagonist. Apart from its significant weight-loss efficacy in DIO mice, compound 4 also displays 163 clean off-target profiles and is currently under development for treating obesity and the related metabolic syndrome.

Function-oriented development of CXCR4 antagonists as selective human immunodeficiency virus (HIV)-1 entry inhibitors.

Motivated by the pivotal role of CXCR4 as an HIV entry co-receptor, we herein report a de novo hit-to-lead effort on the identification of subnanomolar purine-based CXCR4 antagonists against HIV-1 infection. Compound 24, with an EC50 of 0.5 nM against HIV-1 entry into host cells and an IC50 of 16.4 nM for inhibition of radioligand stromal-derived factor-1α (SDF-1α) binding to CXCR4, was also found to be highly selective against closely related chemokine receptors. We rationalized that compound 24 complementarily interacted with the critical CXCR4 residues that are essential for binding to HIV-1 gp120 V3 loop and subsequent viral entry. Compound 24 showed a 130-fold increase in anti-HIV activity compared to that of the marketed CXCR4 antagonist, AMD3100 (Plerixafor), whereas both compounds exhibited similar potency in mobilization of CXCR4(+)/CD34(+) stem cells at a high dose. Our study offers insight into the design of anti-HIV therapeutics devoid of major interference with SDF-1α function.

Conia-ene annulation of the α-cyano β-TMS-capped alkynyl cycloalkanone system and its synthetic application

Under catalysis with ZnI(2), an effective annulation process of ω-silylacetylenic α-cyano ketones, leading to the formation of various bicyclic frameworks characterized with a TMS-containing methylenecyclopentane ring, has been developed.

Autoxidative annulation cascade of the α-cyano β-TMS-capped alkynyl cycloalkanone system.

The autoxidative annulation cascade promoted by an α-cyano β-TMS-capped alkynyl cycloalkanone system under catalysis with pyridine in one oxygen atmosphere has proven to be highly viable. On the basis of this newly developed protocol, a variety of highly functionalized bicyclic frameworks can be effectively constructed.

Discovery of novel stem cell mobilizers that target the CXCR4 receptor.

The chemokine CXCL12 (also known as stromal cell-derived factor-1, SDF-1) consists of 68 amino acids and is a highly positively charged member of the CXC chemokines. It was originally cloned from bone marrow stromal cell lines and was found to act as a growth factor for progenitor B cells. The physiological function of SDF-1 is mediated by the CXCR4 receptor, a G-protein-coupled seven-transmembrane receptor (GPCR), and is broadly expressed in a variety of human tissues, particularly those of the immune and central nervous systems. CXCR4 was also identified as the main co-receptor by which T-lymphotropic HIV strains enter target cells. Although the initial interest in CXCR4 antagonists was focused on their potential application in the treatment of HIV infection, 6] it is now recognized that the SDF-1/CXCR4 axis is also involved in many diseases such as rheumatoid arthritis, asthma, leukemia, and tumor metastasis ; it also helps in recruiting stem cells to sites of injury. AMD3100 (plerixafor, Mozobil), the first highly potent and specific CXCR4 antagonist, was originally intended to treat HIV infection, but failed in phase II clinical trials. Nevertheless, it

Stem Cell Mobilizers Targeting Chemokine Receptor CXCR4: Renoprotective Application in Acute Kidney Injury

We have discovered a novel series of quinazoline-based CXCR4 antagonists. Of these, compound 19 mobilized CXCR4(+) cell types, including hematopoietic stem cells and endothelial progenitor cells, more efficiently than the marketed 1 (AMD3100) with subcutaneous administration at the same dose (6 mg/kg) in mice. This series of compounds thus provides a set of valuable tools to study diseases mediated by the CXCR4/SDF-1 axis, including myocardial infarction, ischemic stroke, and cancer metastasis. More importantly, treatment with compound 19 significantly lowered levels of blood urea nitrogen and serum creatinine in rats with renal ischemia-reperfusion injury, providing evidence for its therapeutic potential in preventing ischemic acute kidney injury. CXCR4 antagonists such as 19 might also be useful to increase circulating levels of adult stem cells, thereby exerting beneficial effects on damaged and/or inflamed tissues in diseases that currently are not treated by standard approaches.

CCDC 968701: Experimental Crystal Structure Determination

Related Article: Jing-Kai Huang, Ying-Chieh Wong, Tzu-Ting Kao, Chen-Tso Tseng, Kak-Shan Shia|2016|J.Org.Chem.|81|10759|doi:10.1021/acs.joc.6b01837