Fibrosis
Fibrosis
Lysyl oxidase family proteins have been recognized as having key roles in fibrogenesis1-3 and suggested to be attractive targets for antifibrotic treatment4. Inhibition of lysyl oxidase activity alleviates fibrosis by reducing fibrillar collagen cross-linking, thus potentially impeding the formation of Idiopathic pulmonary fibrosis (IPF)4-6. Furthermore, our analyses revealed that 70-75% of the lung fibrosis patients are high LOX-expressing compared to normal lung, thus proving the high therapeutic potential of targeting lysyl oxidase enzymes for treatment of pulmonary fibrosis.
Refrences
- Hewitt, R.J., Puttur, F., Gaboriau, D.C.A., Fercoq, F., Fresquet, M., Traves, W.J., et al. Lung extracellular matrix modulates KRT5(+) basal cell activity in pulmonary fibrosis. Nat Commun 2023;14:6039.
- Chaudhari, N., Findlay, A. D., Stevenson, A. W., Clemons, T. D., Yao, Y., Joshi, A., et al. Topical application of an irreversible small molecule inhibitor of lysyl oxidases ameliorates skin scarring and fibrosis. Nat Commun 2022;13(1):5555
- Klepfish, M., Gross, T., Vugman, M., Afratis, N.A., Havusha-Laufer, S., Brazowski, E., et al. LOXL2 Inhibition Paves the Way for Macrophage-Mediated Collagen Degradation in Liver Fibrosis. Front Immunol 2020;11:480.
- Schilter, H., Findlay, A. D., Perryman, L., Yow, T. T., Moses, J., Zahoor, A., et al. The lysyl oxidase like 2/3 enzymatic inhibitor, PXS-5153A, reduces crosslinks and ameliorates fibrosis. J Cell Mol Med 2019;23(3):1759-1770.
- Chen, L., Li, S.,Li, W. LOX/LOXL in pulmonary fibrosis: potential therapeutic targets. J Drug Target 2019;27:790-796.
- Wen, X., Liu, Y., Bai, Y., Li, M., Fu, Q.,Zheng, Y. LOXL2, a copper-dependent monoamine oxidase, activates lung fibroblasts through the TGF-beta/Smad pathway. Int J Mol Med 2018;42:3530-3541.
- Yang, J., Savvatis, K., Kang, J.S., Fan, P., Zhong, H., Schwartz, K., et al. Targeting LOXL2 for cardiac interstitial fibrosis and heart failure treatment. Nat Commun 2016:7:13710.