Your search keyword '"He, Yantao"' showing total 6 results

1. Next generation GLP-1/GIP/glucagon triple agonists normalize body weight in obese mice.

Author

Knerr, Patrick J., Mowery, Stephanie A., Douros, Jonathan D., Premdjee, Bhavesh, Hjøllund, Karina Rahr, He, Yantao, Kruse Hansen, Ann Maria, Olsen, Anette K., Perez-Tilve, Diego, DiMarchi, Richard D., and Finan, Brian

Abstract

Pharmacological strategies that engage multiple mechanisms-of-action have demonstrated synergistic benefits for metabolic disease in preclinical models. One approach, concurrent activation of the glucagon-like peptide-1 (GLP-1), glucose-dependent insulinotropic peptide (GIP), and glucagon (Gcg) receptors (i.e. triagonism), combines the anorectic and insulinotropic activities of GLP-1 and GIP with the energy expenditure effect of glucagon. While the efficacy of triagonism in preclinical models is known, the relative contribution of GcgR activation remains unassessed. This work aims to addresses that central question. Herein, we detail the design of unimolecular peptide triagonists with an empirically optimized receptor potency ratio. These optimized peptide triagonists employ a protraction strategy permitting once-weekly human dosing. Additionally, we assess the effects of these peptides on weight-reduction, food intake, glucose control, and energy expenditure in an established DIO mouse model compared to clinically relevant GLP-1R agonists (e.g. semaglutide) and dual GLP-1R/GIPR agonists (e.g. tirzepatide). Optimized triagonists normalize body weight in DIO mice and enhance energy expenditure in a manner superior to that of GLP-1R mono-agonists and GLP-1R/GIPR co-agonists. These pre-clinical data suggest unimolecular poly-pharmacology as an effective means to target multiple mechanisms contributing to obesity and further implicate GcgR activation as the differentiating factor between incretin receptor mono- or dual-agonists and triagonists. • Details the design of unimolecular peptide triagonists for GLP-1R/GIPR/GCGR. • Optimal weight-loss is achieved when receptor potency ratio is weighted toward GCGR vs GLP-1R or GIPR. • These agonists are protracted for once-weekly human dosing. • Optimized triagonists normalizes body weight & enhance energy expenditure in mice. • Efficacy of optimized triagonists is superior to GLP-1R & GLP-1R/GIPR agonists. [ABSTRACT FROM AUTHOR]

Published

2022

2. A potent and selective inhibitor for the UBLCP1 proteasome phosphatase.

Author

He, Yantao, Guo, Xing, Yu, Zhi-Hong, Wu, Li, Gunawan, Andrea M., Zhang, Yan, Dixon, Jack E., and Zhang, Zhong-Yin

Subjects

*PROTEASOME inhibitors, *DRUG synergism, *PHOSPHATASES, *SMALL molecules, *DENATURATION of proteins, *UBIQUITIN

Abstract

The ubiquitin-like domain-containing C-terminal domain phosphatase 1 (UBLCP1) has been implicated as a negative regulator of the proteasome, a key mediator in the ubiquitin-dependent protein degradation. Small molecule inhibitors that block UBLCP1 activity would be valuable as research tools and potential therapeutics for human diseases caused by the cellular accumulation of misfold/damaged proteins. We report a salicylic acid fragment-based library approach aimed at targeting both the phosphatase active site and its adjacent binding pocket for enhanced affinity and selectivity. Screening of the focused libraries led to the identification of the first potent and selective UBLCP1 inhibitor 13 . Compound 13 exhibits an IC 50 of 1.0 μM for UBLCP1 and greater than 5-fold selectivity against a large panel of protein phosphatases from several distinct families. Importantly, the inhibitor possesses efficacious cellular activity and is capable of inhibiting UBLCP1 function in cells, which in turn up-regulates nuclear proteasome activity. These studies set the groundwork for further developing compound 13 into chemical probes or potential therapeutic agents targeting the UBLCP1 phosphatase. [ABSTRACT FROM AUTHOR]

Published

2015

3. Bicyclic benzofuran and indole-based salicylic acids as protein tyrosine phosphatase inhibitors

Author

He, Yantao, Zeng, Li-Fan, Yu, Zhi-Hong, He, Rongjun, Liu, Sijiu, and Zhang, Zhong-Yin

Subjects

*BENZOFURAN, *SALICYLIC acid, *PROTEIN-tyrosine phosphatase, *CHEMICAL inhibitors, *PHOSPHORYLATION, *DIABETES

Abstract

Abstract: Protein tyrosine phosphatases (PTPs) constitute a large and structurally diverse family of signaling enzymes that control the cellular levels of protein tyrosine phosphorylation. Malfunction of PTP activity has significant implications in many human diseases, and the PTP protein family provides an exciting array of validated diabetes/obesity (PTP1B), oncology (SHP2), autoimmunity (Lyp), and infectious disease (mPTPB) targets. However, despite the fact that PTPs have been garnering attention as novel therapeutic targets, they remain largely an untapped resource. The main challenges facing drug developers by the PTPs are inhibitor specificity and bioavailability. Work over the last ten years has demonstrated that it is feasible to develop potent and selective inhibitors for individual members of the PTP family by tethering together small ligands that can simultaneously occupy both the active site and unique nearby peripheral binding sites. Recent results with the bicyclic salicylic acid pharmacophores indicate that the new chemistry platform may provide a potential solution to overcome the bioavailability issue that has plagued the PTP drug discovery field for many years. Structural analysis of PTP-inhibitor complexes reveals molecular determinants important for the development of more potent and selective PTP inhibitors, thus offering hope in the medicinal chemistry of a largely unexploited protein class with a wealth of attractive drug targets. [Copyright &y& Elsevier]

Published

2012

4. New quality weight used for phase unwrapping in color fringe reflection method.

Author

He, Yantao, Zhu, Yongjian, Qin, Guofeng, Qin, Yunbai, Jiang, F., Zheng, Kunkun, and Zhong, Jianping

Subjects

*PHASE-shifting interferometry, *STANDARD deviations, *ROTATIONAL symmetry

Abstract

• Use of three-step phase-shifting for single color fringe. • A new quality weight is proposed for quality-guiding the phase unwrapping. • An experimental method with lower reconstruction error is proposed. The fringe -reflection technology has been widely applied in the fields of industrial inspection and measurements. In the present study, three-step phase-shifting is developed using the color fringe-reflection approach to inspect a work-piece surface with rotational symmetry characteristics, and an improved experiment is proposed. In addition, by combining Robert gradient with fringe modulation, a new quality weight, referred to as 'Modulation-Robert gradient variance' (MRGV), is proposed for quality-guiding the phase-unwrapping (PU) algorithm. In comparison to the traditional quality weights, MRGV presented higher noise immunity and lower PU error in the root mean square (RMS). In addition, in terms of defect detection, MRGV performed better than the other weights. Finally, after MRGV-guided PU conduction, the proposed experiment method is used in combination with an improved Southwell integration algorithm to realize the 3D reconstruction. The reconstruction error is approximately 3.09% lower than that presented by certain other methods. Furthermore, the results indicated that the combination of the proposed method and the new quality weight could effectively detect the defects and offer an accurate measurement of a rotationally symmetrical surface to a certain extent. [ABSTRACT FROM AUTHOR]

Published

2021

5. Akt2 inhibits the activation of NFAT in lymphocytes by modulating calcium release from intracellular stores

Author

Martin, Victoria A., Wang, Wen-Horng, Lipchik, Andrew M., Parker, Laurie L., He, Yantao, Zhang, Sheng, Zhang, Zhong-Yin, and Geahlen, Robert L.

Subjects

*ENZYME inhibitors, *LYMPHOCYTES, *INTRACELLULAR calcium, *ANTIGEN receptors, *PHOSPHOLIPASE C, *TRANSCRIPTION factors, *CELL communication

Abstract

Abstract: The engagement of antigen receptors on lymphocytes leads to the activation of phospholipase C-γ, the mobilization of intracellular calcium and the activation of the NFAT transcription factor. The coupling of antigen receptors to the activation of NFAT is modulated by numerous cellular effectors including phospho-inositide 3-kinase (PI3K), which is activated following receptor cross-linking. The activation of PI3K has both positive and negative effects on the receptor-mediated activation of NFAT. An increase in the level and activity of Akt2, a target of activated PI3K, potently inhibits the subsequent activation of NFAT. In contrast, an elevation in Akt1 has no effect on signaling. Signaling pathways operating both upstream and downstream of inositol 1,4,5-trisphosphate (IP3)-stimulated calcium release from intracellular stores are unaffected by Akt2. An increase in the level of Akt2 has no significant effect on the initial amplitude, but substantially reduces the duration of calcium mobilization. The ability of Akt2 to inhibit prolonged calcium mobilization is abrogated by the administration of a cell permeable peptide that blocks the interaction between Bcl-2 and the IP3 receptor. Thus, Akt2 is a negative regulator of NFAT activation through its ability to inhibit calcium mobilization from the ER. [Copyright &y& Elsevier]

Published

2012

6. Negative Regulation of Stat3 by Activating PTPN11 Mutants Contributes to the Pathogenesis of Noonan Syndrome and Juvenile Myelomonocytic Leukemia.

Author

Zhang, Wenjun, Chan, Rebecca J., Chen, Hanying, Yang, Zhenyun, He, Yantao, Zhang, Xian, Luo, Yong, Yin, Fuqing, Moh, Akira, MiIler, Lucy C., Payne, R. Mark, Zhang, Zhong-Yin, Fu, Xin-Yuan, and Shou, Weinian

Subjects

*HUMAN chromosome abnormalities, *GENETIC disorders, *MULTIPLE birth, *LEUKEMIA, *MYELOPROLIFERATIVE neoplasms, *HEMATOPOIETIC stem cells

Abstract

Noonan syndrome (NS) is an autosomal dominant congenital disorder characterized by multiple birth defects including heart defects and myeloproliferative disease (MPD). Approximately 50% of NS patients have germline gain-of-function mutations in PTPNJ1, which encodes the protein-tyrosine phosphatase, Shp2. We provide evidence that conditional ablation of Stat3 in hematopoietic cells and cardiac valvular tissues leads to myeloid progenitor hyperplasia and pulmonary stenosis due to the leaflet thickening, respectively. Consistently, STAT3 activation is significantly compromised in peripheral blood cells from NS patients bearing Shp2-activating mutations. Biochemical and functional analyses demonstrate that activated Shp2 is able to down-regulate Tyr(P)-Stat3 and that constitutively active Stat3 rescues activating mutant Shp2-induced granulocyte-macrophage colony-stimulating factor hypersensitivity in bone marrow cells. Collectively, our work demonstrates that Stat3 is an essential signaling component potentially contributing to the pathogenesis of NS and juvenile myelomonocytic leukemia caused by PTPN11 gain-of-function mutations. [ABSTRACT FROM AUTHOR]

Published

2009