Body Weight-Supported Treadmill Training Ameliorates Motoneuronal Hyperexcitability by Increasing GAD-65/67 and KCC2 Expression via TrkB Signaling in Rats with Incomplete Spinal Cord Injury

Neurochemical Research - Spasticity is a typical consequence after spinal cord injury (SCI). The critical reasons are reducing the synthesis of Gamma-Aminobutyric Acid (GABA), glycine and potassium...     

Electro-Acupuncture Pretreatment Ameliorates Anesthesia and Surgery-Induced Cognitive Dysfunction Via Inhibiting Mitochondrial Injury and nEuroapoptosis in Aged Rats

Neurochemical Research - Postoperative cognitive dysfunction (POCD) remains one of the most common complications following anesthesia and surgery (AS) in the elderly population. Calcium-mediated...     

Expression of Cre recombinase in chondrocytes causes abnormal craniofacial and skeletal development

The cranial base synchondroses are growth centers that drive cranial and upper facial growth. The intersphenoid synchondrosis (ISS) and the spheno-occipital synchondrosis (SOS) are two major synchondroses located in the middle of the cranial base and are maintained at early developmental stages to sustain cranial base elongation. In this study, we report unexpected premature ossification of ISS and SOS when Cre recombinase is activated in a chondrocyte-specific manner. We used a Cre transgenic line expressing Aggrecan enhancer-driven, Tetracycline-inducible Cre (ATC), of which expression is controlled by a Col2a1 promoter. Neonatal doxycycline injection or doxycycline diet fed to breeders was used to activate Cre recombinase. The premature ossification of ISS and/or SOS led to a reduction in cranial base length and subsequently a dome-shaped skull. Furthermore, the mice carrying either heterozygous or homozygous conditional deletion of Tsc1 or Fip200 using ATC mice developed similar craniofacial abnormalities, indicating that Cre activity itself but not conditional deletion of Tsc1 or Fip200 gene, is the major contributor of this phenotype. In contrast, the Col2a1-Cre mice carrying Cre expression in both perichondrium and chondrocytes and the mice carrying the conditional deletion of Tsc1 or Fip200 using Col2a1-Cre did not manifest the same skull abnormalities. In addition to the defective craniofacial bone development, our data also showed that the Cre activation in chondrocytes significantly compromised bone acquisition in femur. Our data calls for the consideration of the potential in vivo adverse effects caused by Cre expression in chondrocytes and reinforcement of the importance of including Cre-containing controls to facilitate accurate phenotype interpretation in transgenic research.

     

不同海拔高原鼠兔个性特征与SERT基因多态性关联

个性特征是指动物个体间稳定、可遗传的行为差异,与相关基因多态性有关,反映了动物对环境的适应模式,探究个性相关基因变异,将有助于更好地理解动物对环境的适应与进化机制。本文以高原鼠兔 (Ochotona curzoniae) 为对象,研究了5个不同海拔地区高原鼠兔的个性 (探究性、勇敢性和温顺性) 差异特征,并检测了个性相关基因5-羟色胺转运体 (SERT) 的单核苷酸多态性 (SNP) 和mRNA表达。结果发现,高海拔地区高原鼠兔的探究性和勇敢性显著高于低海拔地区,而高海拔地区高原鼠兔SERT基因mRNA表达量显著低于低海拔地区,提示不同海拔高原鼠兔个性特征差异可能与SERT基因mRNA表达有所关联。进一步检测不同海拔地区高原鼠兔SERT基因多态性及其分布差异情况,发现该基因存在6个SNP (其中5个位于外显子3,1个位于外显子5 );不同海拔地区鼠兔基因分布差异分析显示外显子5的c.A1063C 同义突变与海拔之间存在显著相关,高海拔地区该位点CC基因型分布频率显著高于低海拔地区;c.A1063C的基因型虽然与探究性、勇敢性无显著相关,但与温顺性显著相关。综上所述,随着海拔升高,高原鼠兔探究性和勇敢性增加,这有利于动物获取更多的食物资源,进而增加其生存机会。与此同时,SERT基因多态性显示与不同海拔地区的生存环境相适应的特征,且与温顺性有关,暗示不同海拔高原鼠兔个性差异可能与SERT基因SNP的差异有关。本研究从基因表达与突变的角度尝试阐述高原鼠兔适应不同海拔环境的行为差异,显示了不同海拔地区高原鼠兔行为生存策略潜在的分子机制。     

Mitochondrial Tim9 protects Tim10 from degradation by the protease Yme1

Translocase of IM (inner membrane; Tim)9 and Tim10 are essential homologue proteins of the mitochondrial intermembrane space (IMS) and form a stable hexameric Tim9–Tim10 complex there. Redox-switch of the four conserved cysteine residues plays a key role during the biogenesis of these proteins and, in turn, the Tim proteins play a vital chaperone-like role during import of mitochondrial membrane proteins. However, the functional mechanism of the small Tim chaperones is far from solved and it is unclear whether the individual proteins play specific roles or the complex functions as a single unit. In the present study, we examined the requirement and role for the individual disulfide bonds of Tim9 on cell viability, complex formation and stability using yeast genetic, biochemical and biophysical methods. Loss of the Tim9 inner disulfide bond led to a temperature-sensitive phenotype and degradation of both Tim9 and Tim10. The growth phenotype could be suppressed by deletion of the mitochondrial i-AAA (ATPases associated with diverse cellular activities) protease Yme1, and this correlates strongly with stabilization of the Tim10 protein regardless of Tim9 levels. Formation of both disulfide bonds is not essential for Tim9 function, but it can facilitate the formation and improve the stability of the hexameric Tim9–Tim10 complex. Furthermore, our results suggest that the primary function of Tim9 is to protect Tim10 from degradation by Yme1 via assembly into the Tim9–Tim10 complex. We propose that Tim10, rather than the hexameric Tim9–Tim10 complex, is the functional form of these proteins.