Osmotic response element binding protein (OREBP) is an essential regulator of urine concentrating mechanism and renal protection

Lam, Ka-man, Amy.

January 2004

Thesis (Ph. D.)--University of Hong Kong, 2005. / Title proper from title frame. Also available in printed format.

Characterization of cre expression in BAC-Pcp2-IRES-Cre transgenic mice

Ng, Hoi-lam, Alam.

January 2005

Thesis (M. Phil.)--University of Hong Kong, 2006. / Title proper from title frame. Also available in printed format.

Role of aldose reductase in pathogenesis of diabetic neuropathy by making use of Thy1-YFP transgenic mice with aldose reductase-mutation

Chen, Yuk-shan.

January 2005

Thesis (M. Phil.)--University of Hong Kong, 2006. / Title proper from title frame. Also available in printed format.

Analysis of abnormal craniofacial and ear development of a transgenic mutant with ectopic hoxb3 expression /

Wong, Yee-man, Elaine.

January 2006

Thesis (Ph. D.)--University of Hong Kong, 2006. / Also available online.

Tissue specific expression studies on a vagal neural crest enhancer element of the mouse Hoxb3 gene in the development of the enteric nervous system /

Chen, Yuk-shan.

January 2000

Thesis (M. Phil.)--University of Hong Kong, 2001. / Includes bibliographical references (leaves 87-102).

Mapping the locus for a novel blind mouse mutant Mcc

Cheng, Man-hei., 鄭文熙.

January 2006

published_or_final_version / Medical Sciences / Master / Master of Medical Sciences

Eye - Abnormalities - Genetic aspects.

Cataract - Genetic aspects.

Transgenic mice.

Generation and characterization of transgenic mice expressing dominantnegative osmotic response element binding protein (OREBP) in the brainneurons

Ho, Shuk-wai, Amy, 何淑慧

January 2007

published_or_final_version / Medical Sciences / Master / Master of Medical Sciences

Carrier proteins.

Transcription factors.

Transgenic mice - Molecular genetics.

Osmoregulation.

Study of abnormal inner ear development in Waardenburg-Shah syndrome using a Sox10-GEP mutant mouse model

Chu, Kit-hang, 朱傑亨

January 2011

Sox10 is a high mobility group (HMG) domain transcription factor which is an important regulator for neural crest development. SOX10 mutations have been identified in Waardenburg-Shah syndrome type 4 (WS4) patients who suffer from sensorineural deafness. However, the mechanisms underlying the hearing defect of SOX10-mediated WS4 are unclear. The aim of this study is to elucidate the function of Sox10 during mouse inner ear development using a mutant mouse model, in order to reveal the underlying basis for SOX10 mutation associated sensorineural deafness in WS4 patients. The mammalian inner ear originates from the otic placode epithelium as well as neural crest cells (NCCs). To understand the role of Sox10 in inner development, I investigated the contribution of cranial NCCs to the cochleovestibular ganglion (CVG) by lineage tracing analysis, using Wnt1-cre;ZEG mice in which all NCCs were marked by GFP. Co-expression of GFP-positive cells with the glial marker BFABP suggested that glial cells in the CVG were derived from NCCs. Furthermore, Sox10-expressing NCCs were found to invade the CVG at 30-somite stage. These results suggest a role of Sox10 in regulating cranial NCCs contribution to CVG glia. In our laboratory we have generated a mouse mutant Sox10EGFP in which the Sox10 N-terminal domain was fused to the EGFP reporter. To investigate the function of Sox10 in NCCs invasion and gliogenesis of CVG, phenotypic analysis of Sox10NGFP mutant mouse were performed. EGFP expression in the CVG and inner ear epithelium of Sox10NGFP/+ embryos recapitulated the dynamic expression pattern of Sox10. Sox10NGFP/NGFP mutants displayed a reduced number of migrating NCCs and lacked NCCs or glia in their CVG. Moreover, loss of glial cell in the developing spiral ganglia of Sox10NGFP/NGFP mice led to disorganized fasciculation and degeneration of axonal filaments. These data suggest that Sox10 is required for maintaining the cranial NC stem cell pool, and is also essential for CVG gliogenesis and normal growth and innervation of spiral ganglion neurons. To study the function of Sox10 in regulating cochlear morphogenesis, morphological and histological analysis of mutant cochlear were performed. As illustrated by paint-filling analysis, Sox10NGFP/NGFP mice developed a shortened cochlear duct, reduced cochlear turning and enlarged endolymph lumen. Sensory hair cell patterning in the organ of Corti was normal in the Sox10 mutant as shown by immunohistochemistry analysis, suggesting that cochlear lumen enlargement was not due to disrupted planar cell polarity (PCP) pathway. To explore the molecular basis of Sox10-mediated cochlear morphogenic defect, expression of genes related to cochlear development were examined by qRT-PCR. Candidate genes included those involved in fluid homeostasis, which are known to affect the size of cochlear lumen. Up-regulated expression of Aquaporin 3, a water channel protein in the cochlear epithelium that facilitates water transport across the cell membrane, was observed in Sox10NGFP/NGFP cochlear. These results suggest that Sox10 may regulate cochlear morphogenesis by controlling endolymph homeostasis. In conclusion, Sox10 is required in multiple processes during inner ear development including NCC invasion, gliogenesis and cochlear morphogenesis, and their abnormal development can lead to sensorineural deafness in WS4 syndrome. / published_or_final_version / Biochemistry / Doctoral / Doctor of Philosophy

Klein-Waardenburg syndrome

Transgenic mice

Labyrinth (Ear)

Deafness - Genetic aspects

Anti-angiogenic gene therapy of hepatocellular carcinoma by AAV-mediated expression of kallistatin and vasostatin

Tse, Lai-yin., 謝禮賢.

January 2005

published_or_final_version / abstract / Molecular Biology / Doctoral / Doctor of Philosophy

Protease inhibitors.

Gene therapy.

Neovascularization.

Liver - Cancer - Treatment.

Transgenic mice.

Tissue-specific expression of cre recombinase in the developing enteric nervous system of a Hoxb3/cre transgenic mouse strain

陳玉儀, Chan, Yuk-yee.

January 2002

published_or_final_version / Medical Sciences / Master / Master of Medical Sciences

Gene expression

Autonomic nervous system.

Homeobox genes.

Transgenic mice - Genetics.