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1. ¹ãÆ×¿¹²¡¶¾ÒªÁì
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PLoS ONE 2011, 6(7): e22572. doi:10.1371/journal.pone.0022572
Broad-Spectrum Antiviral Therapeutics
Rider TH, Zook CE, Boettcher TL, et al.
Currently there are relatively few antiviral therapeutics, and most which do exist are highly pathogen-specific or have other disadvantages. We have developed a new broad-spectrum antiviral approach, dubbed Double-stranded RNA (dsRNA) Activated Caspase Oligomerizer (DRACO) that selectively induces apoptosis in cells containing viral dsRNA, rapidly killing infected cells without harming uninfected cells. We have created DRACOs and shown that they are nontoxic in 11 mammalian cell types and effective against 15 different viruses, including dengue flavivirus, Amapari and Tacaribe arenaviruses, Guama bunyavirus, and H1N1 influenza. We have also demonstrated that DRACOs can rescue mice challenged with H1N1 influenza. DRACOs have the potential to be effective therapeutics or prophylactics for numerous clinical and priority viruses, due to the broad-spectrum sensitivity of the dsRNA detection domain, the potent activity of the apoptosis induction domain, and the novel direct linkage between the two which viruses have never encountered.

2. ÔÚÌåÍâµ¥ÏòÓ¦Á¦ÓÕµ¼Ñª¹ÜÄÚÆ¤Ï¸°ûÐγÉѪ¹ÜÑù½á¹¹
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Tissue Engineering Part A, 2011; 110811095013006 DOI: 10.1089/ten.tea.2011.0214 Mechanoregulation of Vascularization in Aligned Tissue-Engineered Muscle: A Role for Vascular Endothelial Growth Factor
Daisy W.J. van der Schaft, Ariane C.C. van Spreeuwel, Hans C. van Assen, et al.
Skeletal muscle tissue engineering has major promise for regenerative treatment of patients suffering from muscle loss due to, for example, traumatic injury, but faces considerable challenges to progress toward clinical application. In the present study the creation of an aligned prevascularized muscle tissue was addressed. We hypothesized that an aligned vascularized three-dimensional (3D) muscle tissue can be induced in vitro by merely using uniaxial stress. The present study showed that not only do endothelial cells and muscle cells independently align in the direction of uniaxial stress in a hydrogel-based 3D culture system, but also, more importantly, the endothelial cells in the co-cultured 3D constructs organized into vascular structures. Strikingly, in these cultures no additional growth factors were needed to induce vascular formation of the endothelial cells. Vascular endothelial growth factor (VEGF) production by the muscle cells was stimulated by the uniaxial stress that develops in the tissue when constrained in one direction. This stress accompanied by VEGF production appeared to play a key role in the organization of the endothelial cells into vessel-like structures.

3. ͨ¹ý·­ÒëºóºÏ³ÉÁ×ËáË¿°±ËáÀ©Õ¹´ó³¦¸Ë¾úÒÅ´«ÃÜÂë
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O-Á×ËáË¿°±ËáÊÇÕæºËϸ°ûÁ×ËữÂѰ××éÖк¬Á¿×î¶àµÄÁ×Ëữ°±»ùËᣨSep£©£¬²»ÔÚÒÅ´«ÃÜÂëÖбàÂ룬¶øÊÇÔÚ·­ÒëºóºÏ³É¡£ÃÀ¹ú¿ÆÑ§¼Ò±¨µÀÁËÒ»¸ö¹¤³Ìϵͳ£¬Í¨¹ýÓµÓÐtRNASep¡¢SepRSºÍÉè¼ÆÖÆÔìµÄEF-Tu £¨EF-Sep£©µÄ´ó³¦¸Ë¾ú±äÖÖ½«Ë¿°±ËáÌØÒìÐԵĹ²·­ÒëÕûºÏµ½ÂѰ׵Äí§ÒâλÖá£ÒÀÀµ¹¤³ÌÔÙÔìEF-TuÀ´ËÉ¿ªÆäÖÊÁ¿¿ØÖƹ¦Ð§ÔÊÐíSep-tRNASepµÄÍŽáÀ´À©Õ¹ÒÅ´«ÃÜÂë¡£

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Science, 2011; 333 (6046): 1151-1154 DOI: 10.1126/science.1207203
Expanding the Genetic Code of Escherichia coli with Phosphoserine
Hee-Sung Park, Michael J. Hohn, Takuya Umehara, et al. 
O-Phosphoserine (Sep), the most abundant phosphoamino acid in the eukaryotic phosphoproteome, is not encoded in the genetic code, but synthesized posttranslationally. Here, we present an engineered system for specific cotranslational Sep incorporation (directed by UAG) into any desired position in a protein by an Escherichia coli strain that harbors a Sep-accepting transfer RNA (tRNASep), its cognate Sep¨CtRNA synthetase (SepRS), and an engineered EF-Tu (EF-Sep). Expanding the genetic code rested on reengineering EF-Tu to relax its quality-control function and permit Sep-tRNASep binding. To test our system, we synthesized the activated form of human mitogen-activated ERK activating kinase 1 (MEK1) with either one or two Sep residues cotranslationally inserted in their canonical positions (Sep218, Sep222). This system has general utility in protein engineering, molecular biology, and disease research.

4. ´úл×ÛºÏÖ¢²¡ÈËÖ¬·¾×éÖ¯µ÷ÀíÒì³£¸üÒ×Ôì³ÉÌÇÄò²¡ºÍÐÄѪ¹Ü¼²²¡
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The Journal of Clinical Endocrinology & Metabolism, 2011 DOI: 10.1210/jc.2011-1577
Adipose Tissue Dysregulation in Patients with Metabolic Syndrome
Andrew A. Bremer, Sridevi Devaraj, Alaa Afify, and Ishwarlal Jialal.
Context: The metabolic syndrome (MetS) is associated with increased risk of diabetes and cardiovascular disease (CVD). Numerous groups have shown increased circulating biomarkers of inflammation in MetS. However, there are scanty data on the cellular sources contributing to this low-grade inflammation.
Objective: The aim of this study was to determine the role of sc adipose tissue (SAT) biology in nascent MetS without concomitant diabetes or CVD.
Patients and Methods: Subjects with MetS and controls were recruited after informed consent. Fasting blood was collected, and SAT was obtained by biopsy.
Results: Circulating biomarkers of inflammation and insulin resistance, high-sensitivity C-reactive protein (hsCRP), IL-6, IL-1¦Â, leptin, serum amyloid A, and retinol-binding protein-4 (RBP-4) concentrations were significantly higher in the MetS subjects than controls, whereas adiponectin concentrations were lower. In SAT, leptin, RBP-4, CRP, serum amyloid A, plasminogen activator inhibitor-1, IL-1, IL-6, IL-8, and monocyte chemotactic protein-1 (MCP-1) levels were significantly higher in MetS than controls. These differences except for RBP-4 persisted after adjusting for waist circumference. In addition, there were significantly increased numbers of macrophages infiltrating the SAT of MetS and increased numbers of crown-like structures compared with controls. hsCRP correlated positively with homeostasis model assessment and SAT MCP-1 and negatively with adiponectin. Homeostasis model assessment correlated positively with plasminogen activator inhibitor-1, RBP-4, and SAT MCP-1.
Conclusions: We make the novel observation that SAT of MetS has increased macrophage recruitment with cardinal crown-like structure features and contributes to the increased cellular inflammation that produces increased levels of biomarkers that are correlated with both insulin resistance and low-grade inflammation. These aberrations could contribute to the progression of MetS and the increased risk for diabetes and CVD.

5. Í»´¥Ð¡ÄҵķÖ×Ó×é³ÉÓÐËù²î±ð
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Neuron, 2011; 71 (3): 474 DOI:10.1016/j.neuron.2011.06.010
v-SNARE Composition Distinguishes Synaptic Vesicle Pools
Zhaolin Hua, Sergio Leal-Ortiz, Sarah M. Foss, et al. 
Synaptic vesicles belong to two distinct pools, a recycling pool responsible for the evoked release of neurotransmitter and a resting pool unresponsive to stimulation. The uniform appearance of synaptic vesicles has suggested that differences in location or cytoskeletal association account for these differences in function. We now find that the v-SNARE tetanus toxin-insensitive vesicle-associated membrane protein (VAMP7) differs from other synaptic vesicle proteins in its distribution to the two pools, providing evidence that they differ in molecular composition. We also find that both resting and recycling pools undergo spontaneous release, and when activated by deletion of the longin domain, VAMP7 influences the properties of release. Further, the endocytosis that follows evoked and spontaneous release differs in mechanism, and specific sequences confer targeting to the different vesicle pools. The results suggest that different endocytic mechanisms generate synaptic vesicles with different proteins that can endow the vesicles with distinct properties.

6. Hsp90-Cdc37ÅóÙ­¸´ºÏÎïµ÷ÀíÏßÁ£Ìå×ÔÍÌÊÉ
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Molecular Cell, 2011; 43 (4): 572 DOI: 10.1016/j.molcel.2011.06.018
Hsp90-Cdc37 Chaperone Complex Regulates Ulk1- and Atg13-Mediated Mitophagy
Joung Hyuck Joo, Frank C. Dorsey, Aashish Joshi, et al.
Autophagy, the primary recycling pathway of cells, plays a critical role in mitochondrial quality control under normal growth conditions and in the response to cellular stress. The Hsp90-Cdc37 chaperone complex coordinately regulates the activity of select kinases to orchestrate many facets of the stress response. Although both maintain mitochondrial integrity, the relationship between Hsp90-Cdc37 and autophagy has not been well characterized. Ulk1, one of the mammalian homologs of yeast Atg1, is a serine-threonine kinase required for mitophagy. Here we show that the interaction between Ulk1 and Hsp90-Cdc37 stabilizes and activates Ulk1, which in turn is required for the phosphorylation and release of Atg13 from Ulk1, and for the recruitment of Atg13 to damaged mitochondria. Hsp90-Cdc37, Ulk1, and Atg13 phosphorylation are all required for efficient mitochondrial clearance. These findings establish a direct pathway that integrates Ulk1- and Atg13-directed mitophagy with the stress response coordinated by Hsp90 and Cdc37.
 

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