遮荫对‘保佳红’桃树叶片快速叶绿素荧光诱导动力学曲线的影响

以3年生桃品种‘保佳红’为试材,于不同生育时期采用人工遮阴的方法,在叶片生长的不同时期分别设置100%(CK)、80%、60%、40%和20% 自然光照的5个光照强度处理,利用快速叶绿素荧光诱导动力学曲线分析技术,研究了不同光强对桃树叶片快速叶绿素荧光诱导动力学曲线及其参数的影响。结果表明：（1）桃树各生长时期的叶片最大荧光值均随着光照强度的减弱而依次升高。（2）在PSⅡ能量分配比率方面,遮阴下的叶片提高了用于电子传递的量子比率(φ_Eo),降低了用于热耗散的的量子比率(φ_Do)。（3）在PSⅡ反应中心活性方面,遮阴使得单位反应中心吸收的光能(ABS/RC)、捕获的光能(TRo/RC)、用于传递电子的能量(ETo/RC)和用于热耗散的能量(DIo/RC)均下降。（4）各时期不同光强处理的最大光化学效率F_v/F_m均在中午时段出现下降,且光照强度越大,降幅越大,说明桃叶在中午会出现强光抑制。研究认为：在遮阴条件下,桃叶天线色素吸收和捕获的光能减少,PSⅡ反应中心活性降低,但其可以通过增加能量在电子传递方面的分配比率来提高对光能的利用。     

Combination of inflammation-related cytokines promotes long-term muscle stem cell expansion

Muscle stem cells (MuSCs, satellite cells) are the major contributor to muscle regeneration. Like most adult stem cells, long-term expansion of MuSCs in vitro is difficult. The in vivo muscle regeneration abilities of MuSCs are quickly lost after culturing in vitro, which prevents the potential applications of MuSCs in cell-based therapies. Here, we establish a system to serially expand MuSCs in vitro for over 20 passages by mimicking the endogenous microenvironment. We identified that the combination of four pro-inflammatory cytokines, IL-1α, IL-13, TNF-α, and IFN-γ, secreted by T cells was able to stimulate MuSC proliferation in vivo upon injury and promote serial expansion of MuSCs in vitro. The expanded MuSCs can replenish the endogenous stem cell pool and are capable of repairing multiple rounds of muscle injuries in vivo after a single transplantation. The establishment of the in vitro system provides us a powerful method to expand functional MuSCs to repair muscle injuries.     

利用线性混合效应模型模拟杉木人工林枝条生物量

基于福建省将乐林场45株人工杉木解析木的572组枝条生物量数据,采用线性混合效应模型方法,建立杉木人工林枝条总生物量和枝、叶生物量的预测模型,并利用独立样本数据对模型进行检验.结果表明： 线性混合效应模型比传统多元线性回归模型的拟合精度高.不同随机效应参数的组合,其混合模型的精度不同.考虑异方差结构的混合模型能够消除数据间的异方差性,其精度更高,其中,对于枝条总生物量和叶生物量模型,以指数函数作为异方差结构时的模型精度最高;对于枝生物量模型,以常数加幂函数作为异方差结构时的模型精度最高.模型检验结果表明：对于杉木人工林枝条生物量预测模型,考虑随机效应和异方差结构的线性混合模型的检验精度比传统多元线性回归模型的精度有明显提高.     

Angiomotin binding-induced activation of Merlin/NF2 in the Hippo pathway

The tumor suppressor Merlin/NF2 functions upstream of the core Hippo pathway kinases Lats1/2 and Mst1/2, as well as the nuclear E3 ubiquitin ligase CRL4^DCAF1. Numerous mutations of Merlin have been identified in Neurofibromatosis type 2 and other cancer patients. Despite more than two decades of research, the upstream regulator of Merlin in the Hippo pathway remains unknown. Here we show by high-resolution crystal structures that the Lats1/2-binding site on the Merlin FERM domain is physically blocked by Merlin''s auto-inhibitory tail. Angiomotin binding releases the auto-inhibition and promotes Merlin''s binding to Lats1/2. Phosphorylation of Ser518 outside the Merlin''s auto-inhibitory tail does not obviously alter Merlin''s conformation, but instead prevents angiomotin from binding and thus inhibits Hippo pathway kinase activation. Cancer-causing mutations clustered in the angiomotin-binding domain impair angiomotin-mediated Merlin activation. Our findings reveal that angiomotin and Merlin respectively interface cortical actin filaments and core kinases in Hippo signaling, and allow construction of a complete Hippo signaling pathway.     

猪链球菌2型Ⅳ型分泌系统组分VirD4与毒力相关性分析

摘要:【目的】构建猪链球菌2型强毒株05ZYH33毒力岛89 K上的Ⅳ型分泌系统组分VirD4敲除突变株,初步分析其活性和毒力,为进一步研究猪链球菌2 型在逃避宿主天然免疫杀伤中的作用提供基础。【方法】以05ZYH33基因组为模板,PCR扩增VirD4基因上下游同源臂,以穿梭质粒pSET1为模板,PCR扩增氯霉素抗性基因Cm,通过重叠PCR技术搭建上述3个片段并连接至温敏载体pSET4s,构建基因敲除载体pSET4s∷VirD4;通过同源重组构建基因敲除突变株ΔVirD4;通过体外全血杀伤实验、CD1小鼠竞争感染及攻毒实验 对突变株和野生株的毒力进行比较分析。【结果】获得了基因敲除突变株ΔVirD4,通过对比发现其毒力与野生株相比有所降低。【结论】猪链球菌2型Ⅳ型分泌系统组分VirD 与其毒力相关,并在早期抵抗天然免疫细胞杀伤中发挥一定作用。     

A Dynamic Model of Chemoattractant-Induced Cell Migration

Cell migration refers to a directional cell movement in response to chemoattractant stimulation. In this work, we developed a cell-migration model by mimicking in vivo migration using optically manipulated chemoattractant-loaded microsources. The model facilitates a quantitative characterization of the relationship among the protrusion force, cell motility, and chemoattractant gradient for the first time (to our knowledge). We verified the correctness of the model using migrating leukemia cancer Jurkat cells. The results show that one can achieve the ideal migrating capacity by choosing the appropriate chemoattractant gradient and concentration at the leading edge of the cell.