The anti‐cancer agent <scp>SU4312 u</scp>nexpectedly protects against <scp>MPP<sup>+</sup></scp>‐induced neurotoxicity via selective and direct inhibition of neuronal <scp>NOS</scp>

Cui, Wei; Zhang, Zaijun; Li, Wenming; Hu, Songhua; Mak, Shinghung; Zhang, Huan; Han, Ren-wen; Yuan, Shuai; Li, Sai; Sa, Fei; Xu, Daping; Lin, Zhi‐Xiu; Zuo, Zhong; Rong, Jianhui; Lung, Edmond Dik; Choi, Tony Chunglit; Lee, Simon My; Han, Yifan

doi:10.1111/bph.12004

Cited by 56 publications

(48 citation statements)

References 34 publications

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“…For instance, the VEGFR2 inhibitor SU5416 (which has gone to Phase III clinical trials), is also a potent agonist of the aryl hydrocarbon receptor which regulates immune function 56 . Similarly, SU4312, another VEGFR2 inhibitor, directly inhibits neuronal nitrogen-oxygen synthase in cerebellar granule neurons 57 . Because several of the VEGFR inhibitors used in basic research have been approved for human trials, these molecules are now being closely scrutinized for other functions.…”

Section: Expanding Biological and Signaling Effects Of Autocrine Vegfmentioning

confidence: 99%

Canonical and Noncanonical Vascular Endothelial Growth Factor Pathways

Domigan

Ziyad

Iruela‐Arispe

2015

ATVB

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The last five years have witnessed a significant expansion in our understanding of VEGF signaling. In particular, the process of canonical activation of VEGFR tyrosine kinases by homodimeric VEGF molecules have now been broadened by the realization that heterodimeric ligands and receptors are also active participants in the signaling process. While heterodimer receptors were described two decades ago, their impact, along with the effect of additional cell surface partners and novel autocrine VEGF signaling pathways, are only now starting to be clarified. Furthermore, ligand-independent signaling (non-canonical) has been identified which occurs through galectin and gremlin binding, and upon rise of intracellular levels of reactive oxygen species. Activation of the VEGF receptors in the absence of ligand holds immediate implications for therapeutic approaches that exclusively target VEGF. The present review provides a concise summary of the recent developments in both canonical and non-canonical VEGF signaling and places these findings in perspective to their potential clinical and biological ramifications.

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Section: Expanding Biological and Signaling Effects Of Autocrine Vegfmentioning

confidence: 99%

Canonical and Noncanonical Vascular Endothelial Growth Factor Pathways

Domigan

Ziyad

Iruela‐Arispe

2015

ATVB

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“…Through drug screening in this model, several compounds with neuroprotective effects such as iNOS inhibitors and anticancer agents have been successfully identified [34][35][36][37][38][39].…”

Section: 6 Bhdpc Increased the Expression Of Bcl2 Via Regulation Omentioning

confidence: 99%

Discovery of a novel neuroprotectant, BHDPC, that protects against MPP+/MPTP-induced neuronal death in multiple experimental models

Chong

Zhao

et al. 2015

Free Radical Biology and Medicine

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“…This tyrosine kinase inhibitor is a selective inhibitor of the vascular endothelial growth factor (VEGF) receptors and has been used to treat cancers based on its anti-angiogenic properties 61 . It also has protective effects on neurons 62 . Although retinoids are also reported to have anti-angiogenic 63 and neuroprotective 64 properties, whether there is a correlation between the mechanisms of SU432 and retinoids is unknown.…”

Section: Discussionmentioning

confidence: 99%

Identification of compounds that modulate retinol signaling using a cell-based qHTS assay

Chen

Sakamuru

Huang

et al. 2016

Toxicology in Vitro

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In vertebrates, the retinol (vitamin A) signaling pathway (RSP) controls the biosynthesis and catabolism of all-trans retinoic acid (atRA), which regulates transcription of genes essential for embryonic development. Chemicals that interfere with the RSP to cause abnormal intracellular levels of atRA are potential developmental toxicants. To assess chemicals for the ability to interfere with retinol signaling, we have developed a cell-based RARE (Retinoic Acid Response Element) reporter gene assay to identify RSP disruptors. To validate this assay in a quantitative high-throughput screening (qHTS) platform, we screened the Library of Pharmacologically Active Compounds (LOPAC) in both agonist and antagonist modes. The screens detected known RSP agonists, demonstrating assay reliability, and also identified novel RSP agonists including kenpaullone, niclosamide, PD98059 and SU4312, and RSP antagonists including Bay 11-7085, LY294002, 3,4-Methylenedioxy-β-nitrostyrene, and topoisomerase inhibitors (camptothecin, topotecan, amsacrine hydrochloride, and idarubicin). When evaluated in the P19 pluripotent cell, these compounds were found to affect the expression of the Hoxa1 gene that is essential for embryo body patterning. These results show that the RARE assay is an effective qHTS approach for screening large compound libraries to identify chemicals that have the potential to adversely affect embryonic development through interference with retinol signaling.

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The anti‐cancer agent SU4312 unexpectedly protects against MPP⁺‐induced neurotoxicity via selective and direct inhibition of neuronal NOS

Cited by 56 publications

References 34 publications

Canonical and Noncanonical Vascular Endothelial Growth Factor Pathways

Canonical and Noncanonical Vascular Endothelial Growth Factor Pathways

Discovery of a novel neuroprotectant, BHDPC, that protects against MPP+/MPTP-induced neuronal death in multiple experimental models

Identification of compounds that modulate retinol signaling using a cell-based qHTS assay

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The anti‐cancer agent SU4312 unexpectedly protects against MPP+‐induced neurotoxicity via selective and direct inhibition of neuronal NOS

Cited by 56 publications

References 34 publications

Canonical and Noncanonical Vascular Endothelial Growth Factor Pathways

Canonical and Noncanonical Vascular Endothelial Growth Factor Pathways

Discovery of a novel neuroprotectant, BHDPC, that protects against MPP+/MPTP-induced neuronal death in multiple experimental models

Identification of compounds that modulate retinol signaling using a cell-based qHTS assay

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The anti‐cancer agent SU4312 unexpectedly protects against MPP⁺‐induced neurotoxicity via selective and direct inhibition of neuronal NOS