Steric structure–activity relationship of cyproheptadine derivatives as inhibitors of histone methyltransferase Set7/9

Set7/9 is a histone lysine methyltransferase, but it is also thought to be involved in a wide variety of pathophysiological functions. We previously identified cyproheptadine, which has a characteristic butterfly-like molecular conformation with bent tricyclic dibenzosuberene and chair-form N-methylpiperidine moieties, as a Set7/9 inhibitor. In this work, we synthesized several derivatives in order to examine the steric structure–inhibitory activity relationship. We found that even a small change of molecular shape due to reduction or replacement of the 10,11-olefinic bond of the tricyclic ring generally resulted in a drastic decrease of the inhibitory activity. Our results should be useful not only for development of more potent and selective inhibitors, but also for the construction of novel inhibitor scaffolds.     

一种改进的图象模糊增强技术

本文简要地讨论了传统模糊增强算法的原理,并详细讨论了这种算法所存在的缺陷。针对传统模糊增强算法的缺陷,本文提出了一种改进的模糊增强算法。实验证明,改进的的算法在图象的处理质量上得到了提高。     

Spp1 at the crossroads of H3K4me3 regulation and meiotic recombination

In Saccharomyces cerevisiae, all H3K4 methylation is performed by a single Set1 Complex (Set1C) that is composed of the catalytic (Set1) and seven other subunits (Swd1, Swd2, Swd3, Bre2, Sdc1, Spp1 and Shg1). It has been known for quite some time that trimethylated H3K4 (H3K4me3) is enriched in the vicinity of meiotic double-strand breaks (DSBs), but the link between H3K4me3 and the meiotic nuclease Spo11 was uncovered only recently. The PHD-containing subunit Spp1, by interacting with H3K4me3 and Mer2, was shown to promote the recruitment of potential meiotic DSB sites to the chromosomal axis allowing their subsequent cleavage by Spo11. Therefore, Spp1 emerged as a key regulator of the H3K4 trimethylation catalyzed by Set1C and of the formation of meiotic DSBs. These findings illustrate the remarkable multifunctionality of Spp1, which not only regulates the catalytic activity of the enzyme (Set1), but also interacts with the deposited mark, and mediates its biological effect (meiotic DSB formation) independently of the complex. As it was previously described for Swd2, and now for Spp1, we anticipate that other Set1C subunits, in addition to regulating H3K4 methylation, may participate in diverse biological functions inside or outside of the complex.     

急性髓系白血病患者HtrA2基因、Set基因表达与疗效和预后的关系研究

摘要 目的：探讨急性髓系白血病（AML）患者HtrA2基因、Set基因表达与疗效和预后的关系。方法：选择2017年6月~2019年6月来我院进行治疗的90例病历资料完整的初诊为AML患者作为本次研究对象,作为AML组,另选取同时期来我院进行健康体检的90例志愿者作为对照组。检测HtrA2基因、Set基因在两组受试者外周血中的表达;分析HtrA2基因、Set基因的表达与AML患者年龄、性别、白细胞计数、NCCN预后分型和疗效的关系。结果：HtrA2基因在AML组中表达水平低于对照组,Set基因在AML组中表达水平高于对照组（P<0.05）。HtrA2基因的表达和年龄、性别、白细胞计数无关（P>0.05）;Set基因的表达和年龄、性别无关（P>0.05）,与白细胞计数有关（P<0.05）。HtrA2基因在NCCN不同的预后分组中的表达差异无统计学意义（P>0.05）;Set基因在NCCN不同的预后分组中的表达差异有统计学意义（P<0.05）。HtrA2基因和Set基因在不同疗效患者中的表达差异有统计学意义（P<0.05）。结论：AML患者HtrA2基因表达下降,Set基因表达升高,Set基因和HtrA2基因具有评估AML疗效的潜力,Set基因可辅助评估AML患者的预后。     

Resetting blood pressure by a closed-loop implanted chip system in normotensive rats

A closed-loop implanted chip system was designed to control blood pressure without using drugs. The chip system instantaneously reset blood pressure by stimulating the left aortic depressor nerve according to the feedback signals of arterial blood pressure. The relationship between pressure signals and frequency of stimulation was identified in vitro and in vivo, and the efficiency of the chip system was evaluated in normal anesthetized Wistar rats. To determine whether the depressor effect of the chip was primarily independent on the bradycardia induced by the resetting, the effects of methyl atropine (1.5 g/kg, iv.) and bilateral vagotomy on depressor effect induced by the chip system were determined, respectively. The results indicated that the chip system worked well. The frequency of stimulus linearly increased following the elevation of pressure from 70 to 160 mm Hg. The frequency of the stimulus reached its maximum (100 Hz) when pressure exceeded 160 mm Hg, and the stimulation stopped when MAP was below 70 mm Hg. There were significant decreases in mean arterial pressure (MAP, -20.0+/-4.4 mm Hg) and heart rate (HR, -43.0+/-10.5 bpm) during the resetting in rats. After resetting, both MAP and HR recovered in a minute without any significant rebound. Pretreatment with either methyl atropine or bilateral vagotomy abolished the bradycardia effect but produced no significant effect on hypotension. The results demonstrated that the chip system successfully reset blood pressure in rats, and that the hypotension induced by the chip system was primarily independent on the bradycardia effect.     

The neurodynamics underlying attentional control in set shifting tasks

In this work we address key phenomena observed with classical set shifting tasks as the “Wisconsin Card Sorting Test” or the “Stroop” task: Different types of errors and increased response times reflecting decreased attention. A component of major importance in these tasks is referred to as the “attentional control” thought to be implemented by the prefrontal cortex which acts primarily by an amplification of task relevant information. This mode of operation is illustrated by a neurodynamical model developed for a new kind of set shifting experiment: The Wisconsin-Delayed-Match-to-Sample task combines uninstructed shifts as investigated in Wisconsin-like tasks with a Delayed-Match-to-Sample paradigm. These newly developed WDMS experiments in conjunction with the neurodynamical simulations are able to explain the reason for decreased attention in set shifting experiments as well the different consequences of decreased attention in tasks requiring bivalent yes/no responses compared to tasks requiring multivalent responses. Electronic supplementary material  The online version of this article (doi: ) contains supplementary material, which is available to authorized users.

Sequence-based marker development in wheat: advances and applications to breeding

In the past two decades, the wheat community has made remarkable progress in developing molecular resources for breeding. A wide variety of molecular tools has been established to accelerate genetic and physical mapping for facilitating the efficient identification of molecular markers linked to genes and QTL of agronomic interest. Already, wheat breeders are benefiting from a wide range of techniques to follow the introgression of the most favorable alleles in elite material and develop improved varieties. Breeders soon will be able to take advantage of new technological developments based on Next Generation Sequencing. In this paper, we review the molecular toolbox available to wheat scientists and breeders for performing fundamental genomic studies and breeding. Special emphasis is given on the production and detection of single nucleotide polymorphisms (SNPs) that should enable a step change in saturating the wheat genome for more efficient genetic studies and for the development of new selection methods. The perspectives offered by the access to an ordered full genome sequence for further marker development and enhanced precision breeding is also discussed. Finally, we discuss the advantages and limitations of marker-assisted selection for supporting wheat improvement.     

circRNA-associated ceRNA network construction reveals the circRNAs involved in the progression and prognosis of breast cancer

Recently, increasing evidences show that circular RNAs (circRNAs) are important regulators of various diseases, especially cancer. However, the regulatory role and the potential mechanism of action of circRNAs in breast cancer remain largely unknown. In this study, weighted gene co-expression network analysis was conducted with the differentially expressed miRNAs and mRNAs in breast cancer from The Cancer Genome Atlas database to identify the key modules associated with the carcinogenesis of breast cancer. In the significant turquoise and brown modules, 22 miRNAs and 1877 mRNAs were identified, respectively. Then, We compared and predicted the target genes and performed survival analysis to identify the miRNAs and mRNAs related to the prognosis of breast cancer. A circRNA-related competitive endogenous RNA network was identified by database co-screening, and deleted in liver cancer 1 (DLC1) was identified as a key gene. Finally, to assess how genes in key modules and key genes contribute to the development of breast cancer, relevant pathway information was obtained through DAVID and Gene Set Enrichment Analysis. These data demonstrated that three circRNAs (hsa-circ-0083373, hsa-circ-0083374, and hsa-circ-0083375) that regulate DLC1 expression via hsa-mir-511 and are involved in the pathogenesis and development of breast cancer.     

A correct formulation for a spatially implicit predator-prey metacommunity model

In order to mitigate the problem of increasing model complexity with increasing number of occupation states in spatially implicit metacommunity models, the assumption of independency among species distributions is often required. In the present paper, we show that this approach only works correctly if set relations among patch occupancy states are considered adequately. This is illustrated by means of a well-known, although incorrectly formulated, predator-prey metacommunity model devised by Bascompte and Solé [1]. We demonstrate that this model shows anomalous dynamical behavior caused by inconsistence between the model formulation and its assumptions. In order to formalize our finding we develop a corrected model formulation that accounts for the principles of set theory so that the sum of the system compartments change rate is nulled. Applying this method successfully rules out the occurrence of anomalous dynamical behavior found in the original model. Finally we discuss the implications of our findings for the accuracy of model predictions.