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Kathryn Cheah½ÌÊÚΪÏã¸Û¿ÆÑ§Ôº³ÉÔ±¡¢ÊÀ½ç¿ÆÑ§ÔºÔºÊ¿£¬ÊÇһλ·¢ÓýÒÅ´«Ñ§¼Ò¡£ÓÚÓ¢¹ú½£ÇÅ´óѧ»ñµÃ·Ö×ÓÉúÎïѧ²©Ê¿Ñ§Î»£¬ÔøÔÚÓ¢¹úÂü³¹Ë¹ÌØ´óѧºÍµÛ¹ú°©Ö¢Ñо¿»ù½ð»á´Óʲ©Ê¿ºóÑо¿¡£ ÔÚÏã¸Û´óѧ£¬ËýÔøµ£ÈÎÉúÎﻯѧϵÖ÷ÈκÍÉúÖ³¡¢·¢ÓýÓëÉú³¤ÖÐÐÄÖ÷ÈΡ£ ÓÉÓÚ¶Ô»ùÖÊÉúÎïѧµÄ¹±Ï×£¬Ëý±»ÊÚÓèÓ¢¹ú»ùÖÊÉúÎïѧѧ»á½±Õ½²×ù 2022¡£
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Post-doctoral Fellow on Mechanotransduction in Stem Cell Biology in the School of Biomedical Sciences, HKU
Applications are invited for appointment as a Postdoctoral Fellow in the School of Biomedical Sciences, to commence as soon as possible for one or two years, with the possibility of renewal. Applicants should have a Ph.D. degree, preferably in Biology, Biomedical Sciences, Medical Engineering, or a related discipline. Experience in cell and molecular biology would be preferred. Applicants should also be organized, self-motivated, committed to the project schedule, and able to work independently and in a team. The appointee will participate in a multidisciplinary RGC-funded Collaborative Research Fund (CRF) project (see below) relating to the influence of the extracellular matrix on lineage-directed differentiation of human embryonic stem cells to intervertebral disc stem cells. For further information, please get in touch with Professor Kathryn Cheah (kathycheah@hku.hk) or Dr. Cheng-Han Yu (chyu1@hku.hk). The appointee will gain experience in stem cell biology, functional genomics, and single-cell biology. A highly competitive salary commensurate with qualifications and experience will be offered, in addition to annual leave and medical benefits.
Project: Analyses of progenitors and differentiation trajectories in the nucleus pulposus and their relevance in intervertebral disc degeneration
Intervertebral disc disease (IDD) and associated low back pain is an aging disorder of significant clinical burden. A likely disease-causing mechanism of IDD is the impairment of the reparative capacity of the intervertebral disc (IVD) tissues in the spine. The nucleus pulposus (NP) forms the central hydrated gelatinous core of the IVD. In IDD, the NP\'s mechanical strength and shock-absorbing capacity in the disc declines. But there is limited knowledge of the influence of the extracellular environment on the molecular characteristics and function of these cells in maintaining a healthy disc.
In this project, we aim to study the role of extracellular matrix stiffness and mechanotransduction in NP cell differentiation and fate. Mechanical loading of the IVD is a crucial factor inducing cellular stress, matrix stiffening, and fibrosis that contribute to disc degeneration. Stiffened microenvironment can promote cell differentiation, proliferation, and expression of adhesion and ECM proteins. We will determine the impact of altering matrix stiffness after culturing in the stiffness-defined functionalized matrices on the differentiation of human embryonic stem cells to NP cells and their transcriptome and gene regulatory network. The insights will be linked and applied to the ongoing meta-analyses of genomic data on IDD.
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