Normal Leptin Expression, Lower Adipogenic Ability, Decreased Leptin Receptor and Hyposensitivity to Leptin in Adolescent Idiopathic Scoliosis

Leptin has been suggested to play a role in the etiology of Adolescent Idiopathic Scoliosis (AIS), however, the leptin levels in AIS girls are still a discrepancy, and no in vitro study of leptin in AIS is reported. We took a series of case-control studies, trying to understand whether Leptin gene polymorphisms are involved in the etiology of the AIS or the change in leptin level is a secondary event, to assess the level of leptin receptor, and to evaluate the differences of response to leptin between AIS cases and controls. We screened all exons of Leptin gene in 45 cases and 45 controls and selected six tag SNPs to cover all the observed variations. Association analysis in 446 AIS patients and 550 healthy controls showed no association between the polymorphisms of Leptin gene and susceptibility/severity to AIS. Moreover, adipogenesis assay of bone mesenchymal stem cells (MSCs) suggested that the adipogenic ability of MSCs from AIS girls was lower than controls. After adjusting the differentiation rate, expressions of leptin and leptin receptor were similar between two groups. Meanwhile, osteogenesis assay of MSC showed the leptin level was similar after adjusting the differentiation rate, but the leptin receptor level was decreased in induced AIS osteoblasts. Immunocytochemistry and western blot analysis showed less leptin receptors expressed in AIS group. Furthermore, factorial designed studies with adipogenesis and osteogenesis revealed that the MSCs from patients have no response to leptin treatment. Our results suggested that Leptin gene variations are not associated with AIS and low serum leptin probably is a secondary outcome which may be related to the low capability of adipogenesis in AIS. The decreased leptin receptor levels may lead to the hyposensitivity to leptin. These findings implied that abnormal peripheral leptin signaling plays an important role in the pathological mechanism of AIS

Multifaceted SlyD from Helicobacter pylori: implication in [NiFe] hydrogenase maturation

SlyD belongs to the FK506-binding protein (FKBP) family with both peptidylprolyl isomerase (PPIase) and chaperone activities, and is considered to be a ubiquitous cytosolic protein-folding facilitator in bacteria. It possesses a histidine- and cysteine-rich C-terminus binding to selected divalent metal ions (e.g., Ni2+, Zn2+), which is important for its involvement in the maturation processes of metalloenzymes. We have determined the solution structure of C-terminus-truncated SlyD from Helicobacter pylori (HpSlyDΔC). HpSlyDΔC folds into two well-separated, orientation-independent domains: the PPIase-active FKBP domain and the chaperone-active insert-in-flap (IF) domain. The FKBP domain consists of a four-stranded antiparallel β-sheet with an α-helix on one side, whereas the IF domain folds into a four-stranded antiparallel β-sheet accompanied by a short α-helix. Intact H. pylori SlyD binds both Ni2+ and Zn2+, with dissociation constants of 2.74 and 3.79 μM respectively. Intriguingly, binding of Ni2+ instead of Zn2+ induces protein conformational changes around the active sites of the FKBP domain, implicating a regulatory role of nickel. The twin-arginine translocation (Tat) signal peptide from the small subunit of [NiFe] hydrogenase (HydA) binds the protein at the IF domain. Nickel binding and the recognition of the Tat signal peptide by the protein suggest that SlyD participates in [NiFe] hydrogenase maturation processes

Learning English through workplace communication : linguistic devices for interpersonal meaning in textbooks in Hong Kong

202105 bcvcAccepted ManuscriptSelf-fundedPublishe

Discovering maximal motif cliques in large heterogeneous information networks

We study the discovery of cliques (or "complete" subgraphs) in heterogeneous information networks (HINs). Existing clique-finding solutions often ignore the rich semantics of HINs. We propose motif clique, or m-clique, which redefines subgraphs completeness with respect to a given motif. A motif essentially a small subgraph pattern, is a fundamental building block of an HIN. The m-clique concept is general and allows us to analyse "complete" subgraphs in an HIN with respect to desired high-order connection patterns. We further investigate the maximal m-clique enumeration problem (MMCE), which finds all maximal m-cliques not contained in any other m-cliques. Because MMCE is NP-hard, developing an accurate and efficient solution for MMCE is not straightforward. we thus present the META algorithm, which employs advanced pruning strategies to effectively reduce the search space. We also design fast techniques to avoid generating duplicated maximal m-clique instances. Our extensive experiments on large real and synthetic HINs how that META is highly effective and efficient

An end-to-end dynamic posture perception method for soft actuators based on distributed thin flexible porous piezoresistive sensors

202311 bckwVersion of RecordOthersGuangdong Science and Technology Research Council; Innovation and Technology Fund, HKSARPublishe

Granulin-epithelin precursor interacts with heparan sulfate on liver cancer cells

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