piR-823 inhibits cell apoptosis via modulating mitophagy by binding to PINK1 in colorectal cancer

Mitophagy plays a vital role in the maintenance of mitochondrial homeostasis and tumorigenesis. Noncoding RNA piR-823 contributes to colorectal tumorigenesis. In this study, we aim to evaluate piR-823-mediated mitophagy and its mechanistic association with colorectal cancer (CRC). Digital gene expression analysis was performed to explore the potential functions of piR-823. A piR-823 antagomir (Ant-823) was used to inhibit piR-823 expression, and piR-823 mimics (mimics-823) were used to increase piR-823 expression. Mitophagy was measured in vivo and in vitro by immunofluorescence and western blot analysis. JC-1 staining, ATP production, real-time PCR, and western blot analysis were used to measure changes in mitochondrial quality and number. siRNA transfection was used to inhibit mitophagy, and CCCP was used to induce mitophagy. RNA pull-down assays and RNA-binding protein immunoprecipitation assays were conducted to investigate the molecular mechanisms. Here, we found that CRC cells transfected with Ant-823 presented an altered expression of autophagic and mitophagy genes by Digital gene expression analysis. Ant-823 could promote Parkin activation and mitophagy in vitro and in vivo, followed by mitochondrial loss and dysfunction of some mitochondria, whereas mimics-823 exerted the opposite effects in CRC cells. The inhibition of mitophagy by siParkin alleviated Ant-823-induced mitochondrial loss and dysfunction, as well as apoptosis to a certain extent. Furthermore, piR-823 was found to interact with PINK1 and promote its ubiquitination and proteasome-dependent degradation, thus alleviating mitophagy. Finally, these findings were verifed in samples obtained by patients affected by colorectal cancer. In conclusion, we identify a novel mechanism by which piR-823 regulates mitophagy during CRC tumorigenesis by increasing PINK1 degradation. Subject terms: Colorectal cancer, Gastrointestinal cancer     

STE20 phosphorylation of AMPK-related kinases revealed by biochemical purifications combined with genetics

We have recently purified mammalian sterile 20 (STE20)–like kinase 3 (MST3) as a kinase for the multifunctional kinases, AMP-activated protein kinase–related kinases (ARKs). However, unresolved questions from this study, such as remaining phosphorylation activities following deletion of the Mst3 gene from human embryonic kidney cells and mice, led us to conclude that there were additional kinases for ARKs. Further purification recovered Ca²⁺/calmodulin-dependent protein kinase kinases 1 and 2 (CaMKK1 and 2), and a third round of purification revealed mitogen-activated protein kinase kinase kinase kinase 5 (MAP4K5) as potential kinases of ARKs. We then demonstrated that MST3 and MAP4K5, both belonging to the STE20-like kinase family, could phosphorylate all 14 ARKs both in vivo and in vitro. Further examination of all 28 STE20 kinases detected variable phosphorylation activity on AMP-activated protein kinase (AMPK) and the salt-inducible kinase 3 (SIK3). Taken together, our results have revealed novel relationships between STE20 kinases and ARKs, with potential physiological and pathological implications.     

Blood-brain barrier-on-a-chip for brain disease modeling and drug testing

The blood-brain barrier (BBB) is an interface between cerebral blood and the brain parenchyma. As a gate keeper, BBB regulates passage of nutrients and exogeneous compounds. Owing to this highly selective barrier, many drugs targeting brain diseases are not likely to pass through the BBB. Thus, a large amount of time and cost have been paid for the development of BBB targeted therapeutics. However, many drugs validated in in vitro models and animal models have failed in clinical trials primarily due to the lack of an appropriate BBB model. Human BBB has a unique cellular architecture. Different physiologies between human and animal BBB hinder the prediction of drug responses. Therefore, a more physiologically relevant alternative BBB model needs to be developed. In this review, we summarize major features of human BBB and current BBB models and describe organ-on-chip models for BBB modeling and their applications in neurological complications.     

人类活动对普氏原羚分布的影响

根据卫星遥感（ＴＭ）影像与野外——ＧＰＳ（全球定位系统）定位的实地考察资料,结合数字化的地形图、植被图与土地利用图、交通图,利用地理信息系统软件——生态信息系统（ＥＩＳ）建立了地理信息系统模型,采用生境评价方法ＨＥＰ就人类活动对青海湖地区普氏原羚生境的影响进行了分析。影响普氏原羚生境适合度的因素主要为基质类型、坡度、水源远近、植被类型与人类活动。当不考虑人类活动影响时,普氏原羚活动区的面积为７９５５ｋｍ ２,最佳生境为典型草原,其次为灌丛沙地,折合适宜生境面积４６６４ｋｍ ２。由于交通、居民点、农业用地等土地利用的影响,普氏原羚仅分布在草地沙地边缘,其适宜分布区迅速减小,生境的适合度等级出现明显变化,最适生境缺损,折合最适生境面积５１１ｋｍ ２。只占原来适合生境面积１１％ 。典型草原围栏与人为放牧影响,普氏原羚实际分布区面积只有３５０ｋｍ ２,讨论了普氏原羚的保护对策。     

Attention allocation on mobile app interfaces when human interacts with them

With the popularity of smartphones and the pervasion of mobile apps, people spend more and more time to interact with a diversity of apps on their smartphones, especially for young population. This raises a question: how people allocate attention to interfaces of apps during using them. To address this question, we, in this study, designed an experiment with two sessions (i.e., Session1: browsing original interfaces; Session 2: browsing interfaces after removal of colors and background) integrating with an eyetracking system. Attention fixation durations were recorded by an eye-tracker while participants browsed app interfaces. The whole screen of smartphone was divided into four even regions to explore fixation durations. The results revealed that participants gave significantly longer total fixation duration on the bottom left region compared to other regions in the session (1) Longer total fixation duration on the bottom was preserved, but there is no significant difference between left side and right side in the session2. Similar to the finding of total fixation duration, first fixation duration is also predominantly paid on the bottom area of the interface. Moreover, the skill in the use of mobile phone was quantified by assessing familiarity and accuracy of phone operation and was investigated in the association with the fixation durations. We found that first fixation duration of the bottom left region is significantly negatively correlated with the smartphone operation level in the session 1, but there is no significant correlation between them in the session (2) According to the results of ratio exploration, the ratio of the first fixation duration to the total fixation duration is not significantly different between areas of interest for both sessions. The findings of this study provide insights into the attention allocation during browsing app interfaces and are of implications on the design of app interfaces and advertisements as layout can be optimized according to the attention allocation to maximally deliver information.     

超速离心机制备冷冻干燥保存菌种

利用超速离心机原有的冷冻系统和真空系统进行冷冻干燥的方法冻干保存了３０种国际标准菌种,４℃保存一年后,随机检测了其中的１８种,全部存活良好。用本法还可以制备出１、２、３、１０ｍｌ不同容量的冷冻干燥生物制剂,适用于中批量各种冻干生物制剂的生产和研究。一机两用,省资金,省用房,提高了机器的利用率。     

中华通草蛉成虫越冬体色变化与滞育的关系

对自然条件下中华通草蛉成虫越冬体色变化与滞育关系的系统研究表明,成虫在越冬过程中都经历了一个较明显的体色变化过程,主要表现在体躯底色从绿色到土黄色及体背面滞育斑由褐色到红褐色的改变,据此将成虫体色分成5个级别,在越冬过程中约80%个体体色经历了在生殖型体色（1级）和滞育型体色（4,5级）之间的明显变化,约有20%个体体色维持在2、3级,在越冬前,成虫滞育斑出现后其卵巢不再发育或者发育受抑而逐渐停止发育,滞育斑的出现是成虫开始滞育的重要标志;越冬后,随着成虫体色由滞育型向生殖型的转变,当大多数个体体色变为3级以下时,卵巢开始发育,这些结果说明,中华通草蛉越冬成虫体色的变化是其滞育越冬的一个重要形态指标,越冬前后体色的改变,标志着成虫滞育的开始和结束。