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Amyotrophic lateral sclerosis (ALS) is a devastating degenerative disease characterized by progressive loss of motor neurons in the motor cortex, brainstem, and spinal cord. Although defined as a motor disorder, ALS can arise concurrently with frontotemporal lobal dementia (FTLD). ALS begins focally but disseminates to cause paralysis and death. About 10% of ALS cases are caused by gene mutations, and more than 40 ALS-associated genes have been identified. While important questions about the biology of this disease remain unanswered, investigations of ALS genes have delineated pathogenic roles for (a) perturbations in protein stability and degradation, (b) altered homeostasis of critical RNA- and DNA-binding proteins, (c) impaired cytoskeleton function, and (d) non-neuronal cells as modifiers of the ALS phenotype. The rapidity of progress in ALS genetics and the subsequent acquisition of insights into the molecular biology of these genes provide grounds for optimism that meaningful therapies for ALS are attainable.

Urea removal from an aqueous solution is considered a challenge in the biological process. The state of complete kidney destruction is known as an end-stage renal disease (ESRD). Kidney transplant and hemodialysis are the most common methods for confronting ESRD. More recently, wearable artificial kidney (WAK) devices have shown a significant improvement in urea removal performance. However, low efficiency in physical adsorbents is a barrier in developing them. For the first time, the urea adsorption capacity of five types of last-generation covalent organic framework (COF) nanosheets (NSs) was investigated in this study by applying molecular dynamics (MD) simulation tools. To this end, different analyses have been performed to evaluate the performance of each nanoparticle. The MD all-atom (AA) results demonstrated that all introduced COF NSs had urea removal capacity. Among the five NSs, TPA-COF was shown to have the best outcomes. Moreover, coarse-grained (CG) and density functional theory (DFT) simulations were conducted, and the results show that the TPA-COF nanoparticle modified with –OH functional group has even better properties for urea adsorption. The present molecular study sheds new light on COF NSs as an adsorbent for urea removal.

Women in developing countries are a key element of development, especially in terms of environmental conservation. Environmental issues have deep social concepts and are changing under the influence of social systems. Women, as one of the basic pillars of a social system, play a fundamental role in development and the environment conservation, which depends on empowering women. Social factors can affect environment conservation directly or indirectly, and the rural women empowerment can be assumed as a mediator variable in this relationship. This study aims to examine the mediation effect of rural women empowerment on the relationship between social factors and environment conservation by combining empowerment and eco-feminist theories. Based on a cross-sectional survey, a sample of 384 rural women was randomly selected and interviewed in the Chaharmahal and Bakhtiari Province, located in the southwest of Iran. The direct structural model revealed that women’s position in the family, their husband's behavior, and women’s participation (as predicting variables) significantly explained 31% of the variation of the environment conservation variable. Moreover, the mediation structural model showed that the rural women empowerment variable had a mediating role in the relationship between women’s position in the family, husband's behavior, plus women’s participation and environmental conservation. The results suggested that these social predictors determine 20% of the women empowerment variable variations and 45% of the environment conservation variance when the women empowerment was introduced as the third variable in the structural model.

N-methyl-D-aspartate receptors (NMDARs) are widely distributed in the central nervous system (CNS) and play critical roles in neuronal excitability in the CNS. Both clinical and preclinical studies have revealed that the abnormal expression or function of these receptors can underlie the pathophysiology of seizure disorders and epilepsy. Accordingly, NMDAR modulators have been shown to exert anticonvulsive effects in various preclinical models of seizures, as well as in patients with epilepsy. In this review, we provide an update on the pathologic role of NMDARs in epilepsy and an overview of the NMDAR antagonists that have been evaluated as anticonvulsive agents in clinical studies, as well as in preclinical seizure models.

Since the discovery of Cu/Zn superoxide dismutase (SOD1) gene mutation, in 1993, as the first genetic abnormality in amyotrophic lateral sclerosis (ALS), over 50 genes have been identified as either cause or modifier in ALS and ALS/frontotemporal dementia (FTD) spectrum disease. Mutations in C9orf72, SOD1, TAR DNA binding protein 43 (TARDBP), and fused in sarcoma (FUS) genes are the four most common ones. During the last three decades, tremendous effort has been made worldwide to reveal biological pathways underlying the pathogenesis of these gene mutations in ALS/FTD. Accordingly, targeting etiologic genes (i.e., gene therapies) to suppress their toxic effects have been investigated widely. It includes four major strategies: (i) removal or inhibition of abnormal transcribed RNA using microRNA or antisense oligonucleotides (ASOs), (ii) degradation of abnormal mRNA using RNA interference (RNAi), (iii) decrease or inhibition of mutant proteins (e.g., using antibodies against misfolded proteins), and (iv) DNA genome editing with methods such as clustered regularly interspaced short palindromic repeats (CRISPR)/CRISPR-associated protein (CRISPR/Cas). The promising results of these studies have led to the application of some of these strategies into ALS clinical trials, especially for C9orf72 and SOD1. In this paper, we will overview advances in gene therapy in ALS/FTD, focusing on C9orf72, SOD1, TARDBP, and FUS genes.

Postmodernism has served as a turning point in the human evolution of thought, and thus, it has challenged a number of assumptions central to social, political, historical, cultural, and literary fields. Accordingly, postmodernism has not left the study of democracy untouched, and in this essay, I aim to study the ways that postmodernism has affected the political, social, and literary democracies. To this end, I develop a conceptual comparative study of postmodernism and democracy with a focus on their overlaps and drawbacks. The comparative study of postmodernism and democracy opens up the space for the introduction of “postmodern democracies” as more inclusive, collective, and comprehensive frameworks of democracy.

The rapid growth of online animation platforms has led to an unprecedented volume of user–content interaction data, posing new challenges for scalable modeling of sequential behaviors and real-time service intelligence. Understanding how users consume animation content over time is essential and challenging for tasks such as personalized recommendation, intelligent caching, and adaptive service orchestration in cloud environments. Considering this challenge, this paper presents CloudSeqAnim, a cloud-oriented sequential behavior modeling framework designed to support large-scale animation content services. In concrete, CloudSeqAnim integrates lightweight sequence representation, temporal dependency modeling, and cloud-based service coordination to enable efficient analysis of long interaction sequences. To validate the feasibility of our proposed CloudSeqAnim framework, we have designed a set of simulation experiments based on the well-known time-series prediction dataset, i.e., Foursquare dataset. Experimental results on the dataset demonstrate that our proposed CloudSeqAnim framework achieves competitive accuracy and favorable efficiency compared with representative sequential baselines, while maintaining scalability suitable for cloud deployment.

Lithium has been a mainstay of therapy for patients with bipolar disorders for several decades. However, it may exert a variety of adverse effects that can affect patients’ compliance. Sexual and erectile dysfunction has been reported in several studies by patients who take lithium as monotherapy or combined with other psychotherapeutic agents. The exact mechanisms underlying such side effects of lithium are not completely understood. It seems that both central and peripheral mechanisms are involved in the lithium-related sexual dysfunction. Here, we had an overview of the epidemiology of lithium-related sexual and erectile dysfunction in previous clinical studies as well as possible pathologic pathways that could be involved in this adverse effect of lithium based on the previous preclinical studies. Understanding such mechanisms could potentially open a new avenue for therapies that can overcome lithium-related sexual dysfunction and improve patients’ adherence to the medication intake.

Since the discovery of the chromosome 9 open reading frame 72 (C9orf72) repeat expansion mutation in 2011 as the most common genetic abnormality in amyotrophic lateral sclerosis (ALS, also known as Lou Gehrig’s disease) and frontotemporal dementia (FTD), progress in understanding the signaling pathways related to this mutation can only be described as intriguing. Two major theories have been suggested—(i) loss of function or haploinsufficiency and (ii) toxic gain of function from either C9orf72 repeat RNA or dipeptide repeat proteins (DPRs) generated from repeat-associated non-ATG (RAN) translation. Each theory has provided various signaling pathways that potentially participate in the disease progression. Dysregulation of the immune system, particularly glial cell dysfunction (mainly microglia and astrocytes), is demonstrated to play a pivotal role in both loss and gain of function theories of C9orf72 pathogenesis. In this review, we discuss the pathogenic roles of glial cells in C9orf72 ALS/FTD as evidenced by pre-clinical and clinical studies showing the presence of gliosis in C9orf72 ALS/FTD, pathologic hallmarks in glial cells, including TAR DNA-binding protein 43 (TDP-43) and p62 aggregates, and toxicity of C9orf72 glial cells. A better understanding of these pathways can provide new insights into the development of therapies targeting glial cell abnormalities in C9orf72 ALS/FTD.