Your search keyword '"A.C. Mueller"' showing total 186 results

1. Prognostic and Predictive Performance of a 24-Gene Post-Operative Radiation Therapy Outcomes Score (PORTOS) in a Phase 3 Randomized Trial of Dose-Intensified Salvage Radiotherapy after Radical Prostatectomy (SAKK 09/10)

Author

A. Dal Pra, D.R. Zwahlen, V.Y. Liu, S. Hayoz, D.E. Spratt, E. Davicioni, Y. Liu, J.A. Proudfoot, C. Schär, T. Hölscher, P. Gut, B. Polat, G. Hildebrandt, A.C. Mueller, L. Plasswilm, F.Y. Feng, A. Pollack, G. Thalmann, D.M. Aebersold, and P. Ghadjar

Subjects

Cancer Research, Radiation, Oncology, Radiology, Nuclear Medicine and imaging

Published

2022

2. Review of Assimilating Spaceborne Global Navigation Satellite System Remote Sensing Data for Tropical Cyclone Forecasting.

Author

Bai, Weihua, Wang, Guanyi, Huang, Feixiong, Sun, Yueqiang, Du, Qifei, Xia, Junming, Wang, Xianyi, Meng, Xiangguang, Hu, Peng, Yin, Cong, Tan, Guangyuan, and Wu, Ruhan

Subjects

GLOBAL Positioning System, REMOTE sensing, TROPICAL cyclones, SURFACE of the earth, CYCLONE forecasting, INFORMATION retrieval

Abstract

Global Navigation Satellite System (GNSS) Radio Occultation (RO) and GNSS Reflectometry (GNSS-R) are the two major spaceborne GNSS remote sensing (GNSS-RS) techniques, providing observations of atmospheric profiles and the Earth's surface. With the rapid development of GNSS-RS techniques and spaceborne missions, many experiments and studies were conducted to assimilate those observational data into numerical weather-prediction models for tropical cyclone (TC) forecasts. GNSS RO data, known for its high precision and all-weather observation capability, is particularly effective in forecasting mid-to-upper atmospheric levels. GNSS-R, on the other hand, plays a significant role in improving TC track and intensity predictions by observing ocean surface winds under high precipitation in the inner core of TCs. Different methods were developed to assimilate these remote sensing data. This review summarizes the results of assimilation studies using GNSS-RS data for TC forecasting. It concludes that assimilating GNSS RO data mainly enhances the prediction of precipitation and humidity, while assimilating GNSS-R data improves forecasts of the TC track and intensity. In the future, it is promising to combine GNSS RO and GNSS-R data for joint retrieval and assimilation, exploring better effects for TC forecasting. [ABSTRACT FROM AUTHOR]

Published

2025

3. Prenatal Exposure to Dibutyl Phthalate and Its Negative Health Effects on Offspring: In Vivo and Epidemiological Studies.

Author

Quelhas, Ana R., Mariana, Melissa, and Cairrao, Elisa

Subjects

MALE reproductive organs, DIBUTYL phthalate, NAIL care, HYGIENE products, GENITALIA

Abstract

Dibutyl phthalate (DBP) is a low-molecular-weight phthalate commonly found in personal care products, such as perfumes, aftershaves, and nail care items, as well as in children's toys, pharmaceuticals, and food products. It is used to improve flexibility, make polymer products soft and malleable, and as solvents and stabilizers in personal care products. Pregnancy represents a critical period during which both the mother and the developing embryo can be significantly impacted by exposure to endocrine disruptors. This article aims to elucidate the effects of prenatal exposure to DBP on the health and development of offspring, particularly on the reproductive, neurological, metabolic, renal, and digestive systems. Extensive research has examined the effects of DBP on the male reproductive system, where exposure is linked to decreased testosterone levels, reduced anogenital distance, and male infertility. In terms of the female reproductive system, DBP has been shown to elevate serum estradiol and progesterone levels, potentially compromising egg quality. Furthermore, exposure to this phthalate adversely affects neurodevelopment and is associated with obesity, metabolic disorders, and conditions such as hypospadias. These findings highlight how urgently stronger laws prohibiting the use of phthalates during pregnancy are needed to lower the risks to the fetus's health and the child's development. [ABSTRACT FROM AUTHOR]

Published

2024

4. Impact of Phenylketonuria on the Serum Metabolome and Plasma Lipidome: A Study in Early-Treated Patients.

Author

Weerd, Jorine C. van der, Wegberg, Annemiek M. J. van, Boer, Theo S., Engelke, Udo F. H., Coene, Karlien L. M., Wevers, Ron A., Bakker, Stephan J. L., Blaauw, Pim de, Groen, Joost, Spronsen, Francjan J. van, and Heiner-Fokkema, M. Rebecca

Subjects

LIQUID chromatography-mass spectrometry, PANTOTHENIC acid, LIPIDOMICS, PHENYLKETONURIA, GLYCEROLIPIDS

Abstract

Background: Data suggest that metabolites, other than blood phenylalanine (Phe), better and independently predict clinical outcomes in patients with phenylketonuria (PKU). Methods: To find new biomarkers, we compared the results of untargeted lipidomics and metabolomics in treated adult PKU patients to those of matched controls. Samples (lipidomics in EDTA-plasma (22 PKU and 22 controls) and metabolomics in serum (35 PKU and 20 controls)) were analyzed using ultra-high-performance liquid chromatography and high-resolution mass spectrometry. Data were subjected to multivariate (PCA, OPLS-DA) and univariate (Mann–Whitney U test, p < 0.05) analyses. Results: Levels of 33 (of 20,443) lipid features and 56 (of 5885) metabolite features differed statistically between PKU patients and controls. For lipidomics, findings include higher glycerolipids, glycerophospholipids, and sphingolipids species. Significantly lower values were found for sterols and glycerophospholipids species. Seven features had unknown identities. Total triglyceride content was higher. Higher Phe and Phe catabolites, tryptophan derivatives, pantothenic acid, and dipeptides were observed for metabolomics. Ornithine levels were lower. Twenty-six metabolite features were not annotated. Conclusions: This study provides insight into the metabolic phenotype of PKU patients. Additional studies are required to establish whether the observed changes result from PKU itself, diet, and/or an unknown reason. [ABSTRACT FROM AUTHOR]

Published

2024

5. Temporal and Spatial Variations in Zebrafish Hairy/E(spl) Gene Expression in Response to Mib1-Mediated Notch Signaling During Neurodevelopment.

Author

Chen, Yi-Chieh, Hsieh, Fu-Yu, Chang, Chia-Wei, Sun, Mu-Qun, and Cheng, Yi-Chuan

Subjects

GENE expression, NEURAL development, BRAIN tumors, SPATIAL variation, NERVOUS system, NOTCH genes

Abstract

Notch signaling is a conserved pathway crucial for nervous system development. Disruptions in this pathway are linked to neurodevelopmental disorders, neurodegenerative diseases, and brain tumors. Hairy/E(spl) (HES) genes, major downstream targets of Notch, are commonly used as markers for Notch activation. However, these genes can be activated, inhibited, or function independently of Notch signaling, and their response to Notch disruption varies across tissues and developmental stages. MIB1/Mib1 is an E3 ubiquitin ligase that enables Notch receptor activation by processing ligands like Delta and Serrate. We investigated Notch signaling disruption using the zebrafish Mib1 mutant line, mib1ta52b, focusing on changes in the expression of Hairy/E(spl) (her) genes. Our findings reveal significant variability in her gene expression across different neural cell types, regions, and developmental stages following Notch disruption. This variability questions the reliability of Hairy/E(spl) genes as universal markers for Notch activation, as their response is highly context-dependent. This study highlights the complex and context-specific nature of Notch signaling regulation. It underscores the need for a nuanced approach when using Hairy/E(spl) genes as markers for Notch activity. Additionally, it provides new insights into Mib1's role in Notch signaling, contributing to a better understanding of its involvement in Notch signaling-related disorders. [ABSTRACT FROM AUTHOR]

Published

2024

6. Isometric Fatigue Resistance of Lumbar Extensors and Cardiovascular Strain in Lower Back Pain Patients Are Associated with Angiotensin-Converting Enzyme and Tenascin-C Gene Polymorphisms.

Author

Flück, Martin, Valdivieso, Paola, Giraud, Marie-Noëlle, and Humphreys, Barry Kim

Subjects

LUMBAR pain, GENETIC polymorphisms, ANGIOTENSIN converting enzyme, TENASCIN, PHYSICAL activity

Abstract

Background: We tested whether gene polymorphisms for angiotensin-converting enzyme (ACE, rs1799752) and tenascin-C (TNC, rs2104772) are associated with variability in fatigue resistance and metabolic strain during static lumbar exercise through interactions with chronic nonspecific lower back pain and habitual physical exercise levels (PA). Methods: Forty-eight patients and matched controls performed an isometric endurance test for lumbar extensors. Metabolic strain to longissimus muscle (oxygen saturation, lactate) and cardiovascular system (muscle hemoglobin, blood pressure) and holding time were monitored. Subjects were genotyped for rs1799752 (II, ID, DD) and rs2104772 (AA, AT, TT). Associations of variance with group, genotype, and PA were analyzed under a 5% false discovery rate. Results: The holding time was lower in patients than in controls (150.9 vs. 188.6 s). This difference was associated with both genotypes, as patients with DD-rs1799752-genotype (p = 0.007) and TT-rs2104772-genotype (p = 0.041) showed lower fatigue resistance. Muscle deoxygenation during exercise varied in positive association with the rs2104772-genotype and PA (p = 0.010, η2 = 0.236). Mean arterial blood pressure (p = 0.028, η2 = 0.108) and recovery of hemoglobin concentration (p = 0.003, η2 = 0.907) demonstrated complex group x rs2104772 interactions. Conclusions: Polymorphisms rs1799752 and rs2104772 influence back pain-related variability in lumbar fatigue resistance. rs2104772 was linked to cardiovascular strain during isometric exercise and recovery via muscle perfusion. [ABSTRACT FROM AUTHOR]

Published

2024

7. The Search for Consistency in Residual Symptoms in Major Depressive Disorder: A Narrative Review.

Author

Pastuszak, Michał, Cubała, Wiesław Jerzy, Kwaśny, Aleksander, and Mechlińska, Agnieszka

Subjects

SLEEP interruptions, APPETITE disorders, MENTAL depression, AFFECT (Psychology), COGNITION disorders

Abstract

Residual symptoms are prevalent in major depressive disorder (MDD), encompassing a wide spectrum of symptoms such as sleep disturbances, changes in weight and appetite, cognitive impairment, and anxiety. These symptoms consistently impair daily functioning, diminish quality of life, and forecast disease relapse. Despite their clinical significance, residual symptoms lack a unified definition, potentially leading to confusion with treatment-emergent symptoms and ambiguity across studies, thereby hindering the generalizability of research findings. While some research identifies insomnia and mood disturbances as critical indicators, other studies emphasize different symptoms or find no significant correlation. Inconsistencies in defining residual symptoms, as well as methodological differences across studies, contribute to these conflicting results. While clinicians focus on alleviating negative symptoms to improve functional status, patients often prioritize achieving positive affect and overall well-being as essential components of successful treatment. It necessitates a comprehensive approach to patient care in depression. This review explores the phenomenon of residual symptoms in MDD, focusing on the ambiguity in definitions, clinical characteristics, and their impact on long-term outcomes. The lack of a standardized regulatory or academic definition for residual symptoms leads to varied interpretations among clinicians, underscoring the need for standardized terminology to guide effective treatment strategies and future research. [ABSTRACT FROM AUTHOR]

Published

2024

8. Current Concepts in the Treatment of Early Onset Scoliosis.

Author

Johnson, Alexandra N. and Lark, Robert K.

Subjects

SCOLIOSIS, COMORBIDITY, ALGORITHMS

Abstract

Despite many surgical advances in the treatment of early onset scoliosis (EOS) over the past two decades, this condition remains a challenge to address. While otherwise healthy children can have EOS, many of these patients have complicated comorbidities making proper treatment algorithms extraordinarily difficult. Non-operative measures can be successful when initiated early, but are many times utilized as a delay tactic until growth-friendly operative procedures can be safely performed. This article will summarize the current concepts in the treatment of EOS with a focus on the surgical advances that have recently been made. [ABSTRACT FROM AUTHOR]

Published

2024

9. Transcriptome Analysis Reveals the Immunosuppression in Tiger Pufferfish (Takifugu rubripes) under Cryptocaryon irritans Infection.

Author

Chi, Yong, Mukiibi, Robert, Zhang, Hongxiang, Zhang, Haien, Li, Weidong, Robledo, Diego, Chen, Songlin, and Li, Yangzhen

Subjects

CRYPTOCARYON irritans, ALTERNATIVE RNA splicing, LINCRNA, IMMUNOREGULATION, TH2 cells

Abstract

Simple Summary: Parasite diseases are recognized as major concerns in the fugu aquaculture industry in China. While understanding the genetic mechanisms of immune response is a crucial step which can facilitate disease control and selective breeding. In this study, transcriptome analysis was performed to identify key genes and understand the underlying mechanisms associated with Cryptocaryon irritans resistance. Finally, our study provided insights into the immunosuppression in fugu under C. irritans infection. The tiger pufferfish (Takifugu rubripes), also known as fugu, has recently suffered from severe C. irritans infections under aquaculture environment, yet the underlying immune mechanisms against the parasite remain poorly understood. In this study, we conducted a comprehensive transcriptome analysis of the gill tissue from infected and uninfected fish using PacBio long-read (one pooled sample each for seriously infected and healthy individuals, respectively) and Illumina short-read (three pools for mildly infected, seriously infected, and healthy individuals, respectively) RNA sequencing technologies. After aligning sequence data to fugu's reference genome, 47,307 and 34,413 known full-length transcripts were identified and profiled in healthy and infected fish, respectively. Similarly, we identified and profiled 1126 and 803 novel genes that were obtained from healthy and infected fish, respectively. Interestingly, we found a decrease in the number of alternative splicing (AS) events and long non-coding RNAs (lncRNAs) after infection with C. irritans, suggesting that they may be involved in the regulation of the immune response in fugu. There were 687 and 1535 differentially expressed genes (DEGs) in moderately and heavily infected fish, respectively, compared to uninfected fish. Kyoto Encyclopedia of Genes and Genomes (KEGG) analyses showed that immune-related DEGs in the two comparison groups were mainly enriched in cytokine-cytokine receptor interactions, ECM-receptor interactions, T-cell receptor signaling pathways, Th1 and Th2 cell differentiation, and Th17 cell differentiation pathways. Further analysis revealed that a large number of immune-related genes were downregulated in infected fish relative to uninfected ones, such as CCR7, IL7R, TNFRSF21, CD4, COL2A1, FOXP3B, and ITGA8. Our study suggests that C. irritans is potentially a highly efficient parasite that may disrupt the defense mechanisms of fugu against it. In addition, in combination of short-read RNA sequencing and previous genome-wide association analyses, we identified five key genes (NDUFB6, PRELID1, SMOX, SLC25A4, and DENND1B) that might be closely associated with C. irritans resistance. This study not only provides valuable resources of novel genic transcripts for further research, but also provides new insights into the immune mechanisms underlying C. irritans infection response in farmed fugu. [ABSTRACT FROM AUTHOR]

Published

2024

10. Synthesis of Chiral Acyclic Pyrimidine Nucleoside Analogues from DHAP-Dependent Aldolases.

Author

Nigro, Mariano, Sánchez-Moreno, Israél, Benito-Arenas, Raúl, Valino, Ana L., Iribarren, Adolfo M., Veiga, Nicolás, García-Junceda, Eduardo, and Lewkowicz, Elizabeth S.

Subjects

ALDOLASES, ALDEHYDE derivatives, THERMOTOGA maritima, DRUG design, MOLECULAR docking, NUCLEOSIDE derivatives

Abstract

Dihydroxyacetone phosphate (DHAP)-dependent aldolases catalyze the aldol addition of DHAP to a variety of aldehydes and generate compounds with two stereocenters. This reaction is useful to synthesize chiral acyclic nucleosides, which constitute a well-known class of antiviral drugs currently used. In such compounds, the chirality of the aliphatic chain, which mimics the open pentose residue, is crucial for activity. In this work, three DHAP-dependent aldolases: fructose-1,6-biphosphate aldolase from rabbit muscle, rhanmulose-1-phosphate aldolase from Thermotoga maritima, and fuculose-1-phosphate aldolase from Escherichia coli, were used as biocatalysts. Aldehyde derivatives of thymine and cytosine were used as acceptor substrates, generating new acyclic nucleoside analogues containing two new stereocenters with conversion yields between 70% and 90%. Moreover, structural analyses by molecular docking were carried out to gain insights into the diasteromeric excess observed. [ABSTRACT FROM AUTHOR]

Published

2024

11. Synergistic Effect of Co-Administered SARS-CoV-2 Vaccines Improves Immune Responses in BALB/c Mice: A Preliminary Study.

Author

Jonas, Nshimirimana, Kimani, Josephine, Kimotho, James, Munyao, Matthew Mutinda, and Nzou, Samson Muuo

Subjects

SARS-CoV-2, COVID-19 vaccines, IMMUNE response

Abstract

Various vaccine platforms have been approved for broad use to prevent the transmission of Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infection. However, these vaccines exhibit distinct differences in immunogenicity and efficacy, which decline after vaccination and are further exacerbated by the emergence of virus variants and mutants. This study reports the immunization outcomes against the SARS-CoV-2 virus by assessing the immune responses and safety of different SARS-CoV-2 vaccines co-administered in BALB/c mice. Vaccine combinations comprising mRNA/adenovirus26-vector, mRNA/inactivated, adenovirus26-vector/inactivated, and mRNA/adenovirus26-vector/inactivated vaccines were prepared in optimized doses, and their activities upon immunization evaluated in comparison with individual mRNA, adenovirus26-vectored, and inactivated vaccines. Fourteen- and 28-days post-immunization, we measured spike-specific IgG response using Enzyme-Linked Immunosorbent Assay (ELISA), cytokine expression profiles through Quantitative real-time polymerase chain reaction (RT-PCR), and evaluated safety through histopathological examination. The mRNA/Vector/Inactivated group exhibited slightly higher anti-spike IgG levels, albeit not statistically significant (p > 0.132). Importantly, this regimen induced elevated IL-6 and IFN-γ mRNA expression levels (p < 0.0001) compared to immunization with individual vaccines. In summary, this study demonstrated that co-administering the mRNA/adenovirus26 vector/inactivated SARS-CoV-2 vaccines improved spike-specific IgG response, triggered significantly enhanced IL-6 and IFN-γ mRNA expression levels, and proved safe in mice. [ABSTRACT FROM AUTHOR]

Published

2024

12. Immune Cell Migration to Cancer.

Author

Ryan, Allison T., Kim, Minsoo, and Lim, Kihong

Subjects

CANCER cell migration, CHEMOKINE receptors, CELL migration, CELL receptors, MYELOID cells, MYELOID-derived suppressor cells

Abstract

Immune cell migration is required for the development of an effective and robust immune response. This elegant process is regulated by both cellular and environmental factors, with variables such as immune cell state, anatomical location, and disease state that govern differences in migration patterns. In all cases, a major factor is the expression of cell surface receptors and their cognate ligands. Rapid adaptation to environmental conditions partly depends on intrinsic cellular immune factors that affect a cell's ability to adjust to new environment. In this review, we discuss both myeloid and lymphoid cells and outline key determinants that govern immune cell migration, including molecules required for immune cell adhesion, modes of migration, chemotaxis, and specific chemokine signaling. Furthermore, we summarize tumor-specific elements that contribute to immune cell trafficking to cancer, while also exploring microenvironment factors that can alter these cellular dynamics within the tumor in both a pro and antitumor fashion. Specifically, we highlight the importance of the secretome in these later aspects. This review considers a myriad of factors that impact immune cell trajectory in cancer. We aim to highlight the immunotherapeutic targets that can be harnessed to achieve controlled immune trafficking to and within tumors. [ABSTRACT FROM AUTHOR]

Published

2024

13. Allergenicity and Conformational Diversity of Allergens.

Author

Seidler, Clarissa A., Zeindl, Ricarda, Fernández-Quintero, Monica L., Tollinger, Martin, and Liedl, Klaus R.

Published

2024

14. Viral RNA in Mosquitoes (Diptera: Culicidae) Collected between 2019 and 2021 in Germany.

Author

Rau, Janine, Köchling, Katharina, Schäfer, Mandy, Tews, Birke A., Wylezich, Claudia, Schaub, Günter A., Werner, Doreen, and Kampen, Helge

Subjects

AEDES aegypti, WEST Nile fever, MOSQUITO control, WEST Nile virus, MOSQUITOES, DIPTERA, RNA

Abstract

Due to globalisation and climate change, mosquito-borne pathogens are emerging in new areas on all continents, including Europe, which has recently faced outbreaks of dengue, chikungunya and West Nile fever. The present study complements previous investigations to evaluate the circulation of mosquito-borne viruses in Germany, with the aim of identifying potential vector species and risk areas. Mosquitoes collected from 2019 to 2021 and identified to species or species group level were screened for viruses of the families Flaviviridae, Peribunyaviridae and the genus Alphavirus of the family Togaviridae. In total, 22,528 mosquitoes were examined, thus providing the most comprehensive study on West Nile virus (WNV) circulation so far in the German mosquito population. Usutu virus (USUV) RNA was detected in six samples, Sindbis virus (SINV) RNA in 21 samples and WNV RNA in 11 samples. Samples containing RNA of USUV and WNV consisted of mosquitoes collected in the East German federal states of Brandenburg, Saxony and Saxony-Anhalt, while samples with RNA of SINV originated from more widespread locations. Although minimum infection rates have remained relatively low, the intensity of virus circulation appears to be increasing compared to previous studies. Continuous mosquito screening contributes to the early detection of the introduction and spread of mosquito-borne pathogens. [ABSTRACT FROM AUTHOR]

Published

2023

15. Comparison of Antibody Responses against Two Molecules from Ascaris lumbricoides : The Allergen Asc l 5 and the Immunomodulatory Protein Al-CPI.

Author

Ahumada, Velky, Zakzuk, Josefina, Aglas, Lorenz, Coronado, Sandra, Briza, Peter, Regino, Ronald, Ferreira, Fátima, and Caraballo, Luis

Subjects

ANTIBODY formation, ASCARIS lumbricoides, IMMUNOGLOBULINS, IMMUNOGLOBULIN E, RECOMBINANT proteins, CYSTEINE proteinase inhibitors, MOLECULES

Abstract

Simple Summary: Helminth infections may have different effects on human health, including risk or protection from other diseases. Ascariasis (caused by Ascaris lumbricoides), the most common soil-transmitted helminthiasis, can induce allergic responses, and also immunosuppression. During ascariasis, antibodies for many A. lumbricoides antigens are produced; however, there is no clear information about the concurrent IgE, IgG4 and IgG production as well as their influences on the actual allergic reactions. In this study, we evaluated antibody responses to two A. lumbricoides molecules, rAsc l 5 and rAl-CPI (an anti-inflammatory product), in an A. lumbricoides endemic population and explored their relationship with the infection and asthma. Our results show that both molecules induce specific antibodies, but, in contrast to rAl-CPI, rAsc l 5 activates cells associated with allergic reactions in some individuals. All together, these data suggest that these molecules have differences in the elicited immune response. Immunity to Ascaris lumbricoides influences the pathogenesis of allergic diseases. Antibody responses to its proteins have been found to be associated with asthma presentation; however, helminth products that induce immunosuppression have been reported, which also raise specific antibodies. We aimed to evaluate antibody responses (IgE, IgG4 and IgG) to two A. lumbricoides molecules, Asc l 5 and Al-CPI (an anti-inflammatory Cysteine Protease Inhibitor), in an endemic population, exploring their relationships with the infection and asthma. The two molecules were produced as recombinant proteins in E. coli expression systems. Specific antibodies were detected by ELISA. Lower human IgE, but higher IgG4 and IgG antibody levels were observed for Al-CPI than for rAsc l 5. The IgE/IgG4 isotype ratio was significantly higher for Asc l 5 than for Al-CPI. In humans Al-CPI did not induce basophil activation as has been previously described for Asc l 5. In mice, Al-CPI induced fewer IgE responses, but more IgG2a antibody titers than rAsc l 5. Our results suggest that these molecules elicit different patterns of immune response to A. lumbricoides. [ABSTRACT FROM AUTHOR]

Published

2023

16. Impact of Semiochemicals Binding to Fel d 1 on Its 3D Conformation and Predicted B-Cell Epitopes Using Computational Approaches.

Author

Durairaj, Rajesh, Pageat, Patrick, and Bienboire-Frosini, Cécile

Subjects

B cells, LIGAND binding (Biochemistry), EPITOPES, SEMIOCHEMICALS, MOLECULAR dynamics

Abstract

The major cat allergen Fel d 1 is a tetrameric glycoprotein from the secretoglobin superfamily. Fel d 1's biological role is unknown, but it has been previously shown that it participates in semiochemical binding/transportation. Fel d 1 has linear epitopes, but its conformational epitope sites remain unclear. In this study, we predicted the B-cell epitopes of Fel d 1 and explored semiochemical dynamics with epitopes using bioinformatics tools. The epitope residues were tabulated for chains 1 and 2 and the heterodimers of Fel d 1. The residual interactions of Fel d 1 with IgE were evaluated, and the prominent epitope sites were predicted. The molecular dynamics simulation (MDS) of Fel d 1 was performed with seven reported semiochemicals to evaluate the Fel d 1–ligand complex stability and decipher the semiochemical effect on Fel d 1 conformational epitopes. Fel d 1–lauric acid, Fel d 1–oleic acid, and Fel d 1–progesterone showed more stability and less fluctuation than other compounds. Fel d 1–linoleic acid and Fel d 1–pregnenolone displayed the most unstable complex with fluctuations. The effects of conformational changes on epitopes are discussed. All the ligand complexes drive substantial fluctuation towards the functionally exposed IgE-binding epitopes. Fel d 1 could be examined for its ligand-binding and conformational changes caused by mutations of B-cell epitopes. [ABSTRACT FROM AUTHOR]

Published

2023

17. Mechanical Analysis and Testing of Conduction-Cooled Superconducting Magnet for Levitation Force Measurement Application.

Author

Liu, Liyuan, Chen, Wei, Zhuang, Huimin, Chi, Fei, Wang, Gang, Zhang, Gexiang, Jiang, Jing, Yang, Xinsheng, and Zhao, Yong

Subjects

MAGNETIC suspension, SUPERCONDUCTING magnets, SUPERCONDUCTING coils, HIGH temperature superconductors, LEVITATION, ENERGY storage, MAGNETIC fields, STRAINS & stresses (Mechanics)

Abstract

High-temperature superconductors have great potential for various engineering applications such as a flywheel energy storage system. The levitation force of bulk YBCO superconductors can be drastically increased by increasing the strength of the external field. Therefore, a 6T conduction-cooled superconducting magnet has been developed for levitation force measurement application. Firstly, to protect the magnet from mechanical damage, reliable stress analysis inside the coil is paramount before the magnet is built and tested. Therefore, a 1/4 two-dimensional (2D) axisymmetric model of the magnet was established, and the mechanical stress in the whole process of winding, cooling down and energizing of the magnet was calculated. Then, the charging, discharging, and preliminary levitation force performance tests were performed to validate the operating stability of the magnet. According to the simulation results, the peak stresses of all coil models are within the allowable value and the winding maintains excellent mechanical stability in the superconducting magnet. The test results show that the superconducting magnet can be charged to its desired current of 150 A without quenching and maintain stable operation during the charging and discharging process. What is more, the superconducting magnet can meet the requirements for the levitation force measurement of both low magnetic field and high magnetic field. [ABSTRACT FROM AUTHOR]

Published

2023

18. Association of Gene Variants with Seasonal Variation in Muscle Strength and Aerobic Capacity in Elite Skiers.

Author

Gasser, Benedikt, Frey, Walter O., Valdivieso, Paola, Scherr, Johannes, Spörri, Jörg, and Flück, Martin

Subjects

ANAEROBIC capacity, AEROBIC capacity, ELITE athletes, MUSCLE strength, GENETIC variation, SARCOPENIA, ISOKINETIC exercise

Abstract

Background: The training of elite skiers follows a systematic seasonal periodization with a preparation period, when anaerobic muscle strength, aerobic capacity, and cardio-metabolic recovery are specifically conditioned to provide extra capacity for developing ski-specific physical fitness in the subsequent competition period. We hypothesized that periodization-induced alterations in muscle and metabolic performance demonstrate important variability, which in part is explained by gene-associated factors in association with sex and age. Methods: A total of 34 elite skiers (20.4 ± 3.1 years, 19 women, 15 men) underwent exhaustive cardiopulmonary exercise and isokinetic strength testing before and after the preparation and subsequent competition periods of the World Cup skiing seasons 2015–2018. Biometric data were recorded, and frequent polymorphisms in five fitness genes, ACE-I/D (rs1799752), TNC (rs2104772), ACTN3 (rs1815739), and PTK2 (rs7460, rs7843014), were determined with specific PCR reactions on collected DNA. Relative percentage changes of cardio-pulmonary and skeletal muscle metabolism and performance over the two seasonal periods were calculated for 160 data points and subjected to analysis of variance (ANOVA) to identify hypothesized and novel associations between performance alterations and the five respective genotypes and determine the influence of age × sex. A threshold of 0.1 for the effect size (h2) was deemed appropriate to identify relevant associations and motivate a post hoc test to localize effects. Results: The preparation and competition periods produced antidromic functional changes, the extent of which varied with increasing importance for anaerobic strength, aerobic performance, cardio-metabolic efficiency, and cardio-metabolic/muscle recovery. Only peak RER (−14%), but not anaerobic strength and peak aerobic performance, and parameters characterizing cardio-metabolic efficiency, differed between the first and last studied skiing seasons because improvements over the preparation period were mostly lost over the competition period. A number of functional parameters demonstrated associations of variability in periodic changes with a given genotype, and this was considerably influenced by athlete "age", but not "sex". This concerned age-dependent associations between periodic changes in muscle-related parameters, such as anaerobic strength for low and high angular velocities of extension and flexion and blood lactate concentration, with rs1799752 and rs2104772, whose gene products relate to sarcopenia. By contrast, the variance in period-dependent changes in body mass and peak VO2 with rs1799752 and rs2104772, respectively, was independent of age. Likely, the variance in periodic changes in the reliance of aerobic performance on lactate, oxygen uptake, and heart rate was associated with rs1815739 independent of age. These associations manifested at the post hoc level in genotype-associated differences in critical performance parameters. ACTN3 T-allele carriers demonstrated, compared to non-carriers, largely different periodic changes in the muscle-associated parameters of aerobic metabolism during exhaustive exercise, including blood lactate and respiration exchange ratio. The homozygous T-allele carriers of rs2104772 demonstrated the largest changes in extension strength at low angular velocity during the preparation period. Conclusions: Physiological characteristics of performance in skiing athletes undergo training period-dependent seasonal alterations the extent of which is largest for muscle metabolism-related parameters. Genotype associations for the variability in changes of aerobic metabolism-associated power output during exhaustive exercise and anaerobic peak power over the preparation and competition period motivate personalized training regimes. This may help to predict and maximize the benefit of physical conditioning of elite skiers based on chronological characteristics and the polymorphisms of the ACTN3, ACE, and TNC genes investigated here. [ABSTRACT FROM AUTHOR]

Published

2023

19. HIV–Host Cell Interactions.

Author

Masenga, Sepiso K., Mweene, Bislom C., Luwaya, Emmanuel, Muchaili, Lweendo, Chona, Makondo, and Kirabo, Annet

Subjects

HIV infections, HIV, ANTIGENIC variation, ANTIRETROVIRAL agents, MOLECULAR interactions, DRUG development

Abstract

The development of antiretroviral drugs (ARVs) was a great milestone in the management of HIV infection. ARVs suppress viral activity in the host cell, thus minimizing injury to the cells and prolonging life. However, an effective treatment has remained elusive for four decades due to the successful immune evasion mechanisms of the virus. A thorough understanding of the molecular interaction of HIV with the host cell is essential in the development of both preventive and curative therapies for HIV infection. This review highlights several inherent mechanisms of HIV that promote its survival and propagation, such as the targeting of CD4+ lymphocytes, the downregulation of MHC class I and II, antigenic variation and an envelope complex that minimizes antibody access, and how they collaboratively render the immune system unable to mount an effective response. [ABSTRACT FROM AUTHOR]

Published

2023

20. Individual Epitope-Specific CD8 + T Cell Immune Responses Are Shaped Differently during Chronic Viral Infection.

Author

Klein, Sebastian, Mischke, Jasmin, Beruldsen, Finn, Prinz, Immo, Antunes, Dinler A., Cornberg, Markus, and Kraft, Anke R. M.

Subjects

T cells, VIRUS diseases, T-cell exhaustion, LYMPHOCYTIC choriomeningitis virus, T cell receptors, IMMUNE response

Abstract

A hallmark in chronic viral infections are exhausted antigen-specific CD8+ T cell responses and the inability of the immune system to eliminate the virus. Currently, there is limited information on the variability of epitope-specific T cell exhaustion within one immune response and the relevance to the T cell receptor (TCR) repertoire. The aim of this study was a comprehensive analysis and comparison of three lymphocytic choriomeningitis virus (LCMV) epitope-specific CD8+ T cell responses (NP396, GP33 and NP205) in a chronic setting with immune intervention, e.g., immune checkpoint inhibitor (ICI) therapy, in regard to the TCR repertoire. These responses, though measured within the same mice, were individual and independent from each other. The massively exhausted NP396-specific CD8+ T cells revealed a significantly reduced TCR repertoire diversity, whereas less-exhausted GP33-specific CD8+ T cell responses were rather unaffected by chronicity in regard to their TCR repertoire diversity. NP205-specific CD8+ T cell responses showed a very special TCR repertoire with a prominent public motif of TCR clonotypes that was present in all NP205-specific responses, which separated this from NP396- and GP33-specific responses. Additionally, we showed that TCR repertoire shifts induced by ICI therapy are heterogeneous on the epitope level, by revealing profound effects in NP396-, less severe and opposed effects in NP205-, and minor effects in GP33-specific responses. Overall, our data revealed individual epitope-specific responses within one viral response that are differently affected by exhaustion and ICI therapy. These individual shapings of epitope-specific T cell responses and their TCR repertoires in an LCMV mouse model indicates important implications for focusing on epitope-specific responses in future evaluations for therapeutic approaches, e.g., for chronic hepatitis virus infections in humans. [ABSTRACT FROM AUTHOR]

Published

2023

21. Differences in Cerebral Oxygenation in Cardiogenic and Respiratory Cardiac Arrest Before, During, and After Cardiopulmonary Resuscitation.

Author

Koyama, Yasuaki, Ouchi, Akira, Shimojo, Nobutake, and Inoue, Yoshiaki

Subjects

CARDIAC arrest, CARDIOPULMONARY resuscitation, RETURN of spontaneous circulation, OXYGEN in the blood, VENTRICULAR fibrillation

Abstract

We compared the changes in cerebral oxygen saturation (ScO2) levels during cardiac arrest (CA) events using porcine models of ventricular fibrillation CA (VF-CA) and asphyxial CA (A-CA). Twenty female pigs were randomly divided into VF-CA and A-CA groups. We initiated cardiopulmonary resuscitation (CPR) 4 min after CA and measured the cerebral tissue oxygenation index (TOI) using near-infrared spectroscopy (NIRS) before, during, and after CPR. In both groups, the TOI was the lowest at 3–4 min after pre-CPR phase initiation (VF-CA group: 3.4 min [2.8–3.9]; A-CA group: 3.2 min [2.9–4.6]; p = 0.386). The increase in TOI differed between the groups in the CPR phase (p < 0.001); it increased more rapidly in the VF-CA group (16.6 [5.5–32.6] vs. 1.1 [0.6–3.3] %/min; p < 0.001). Seven pigs surviving for 60 min after the return of spontaneous circulation in the VF-CA group recovered limb movement, whereas only one in the A-CA group (p = 0.023) achieved movement recovery. The increase in the TOI did not differ significantly between the groups in the post-CPR phase (p = 0.341). Therefore, it is better to monitor ScO2 concomitantly with CPR initiation using NIRS to assess the responsiveness to CPR in clinical settings. [ABSTRACT FROM AUTHOR]

Published

2023

22. Effect of Ketamine on Sleep in Treatment-Resistant Depression: A Systematic Review.

Author

Kwaśny, Aleksander, Włodarczyk, Adam, Ogonowski, Damian, and Cubała, Wiesław Jerzy

Subjects

WAKEFULNESS, SLEEP interruptions, KETAMINE, SLEEP quality, SLEEP, INTRANASAL administration, MENTAL depression

Abstract

Background: Depression is a debilitating disease with a high socioeconomic burden. Regular antidepressants usually require several weeks to ameliorate symptoms; however, numerous patients do not achieve remission. What is more, sleep disturbances are one of the most common residual symptoms. Ketamine is a novel antidepressant with rapid onset of action with a proven antisuicidal effect. Little is known about its impact on sleep–wake and circadian rhythm alterations. The aim of this systematic review is to research the impact ketamine has on sleep disturbances in depression. Methods: PubMed, Web of Science, and APA PsycINFO were searched for relevant studies on ketamine's impact on sleep disturbances in depression. Preferred Reporting Items for Systematic Reviews and Meta-Analyses PRISMA2020 methodology was applied. The systematic review protocol was registered in the PROSPERO Registry (CRD42023387897). Results: Five studies were included in this review. Two studies reported significant improvement in sleep measured by MADRS (Montgomery–Åsberg Depression Rating Scale) and QIDS-SR16 (Quick Inventory of Depressive Symptomatology Self-Report (16-item)) scales after intravenous ketamine and intranasal esketamine administration. One case report showed mitigation of symptoms in PSQI (Pittsburgh Sleep Quality Index) and ISI (Insomnia Severity Index) during 3-month treatment with esketamine. In two studies, sleep was objectively measured by nocturnal EEG (electroencephalography) and showed a decrease in nocturnal wakefulness accompanied by an increase in slow wave (SWS) and rapid eye movement (REM) sleep. Conclusion: Ketamine reduces the severity of sleep insomnia in depression. Robust data are lacking. More research is needed. [ABSTRACT FROM AUTHOR]

Published

2023

23. Status and developments of target production for research on heavy and superheavy nuclei and elements.

Author

Lommel, Bettina, Düllmann, Christoph E., Kindler, Birgit, and Renisch, Dennis

Abstract

We give an overview of the special challenges regarding target development and production for accelerator-based heavy and superheavy-nuclei experiments in the past and perspectives for the future. Production of ever heavier elements, studies of heavy-element production in fusion or transfer reactions, spectroscopic investigations on their nuclear structure and decay and on the fission processes with fragment analyses, laser spectroscopic studies of their atomic structure, high-precision mass measurements as well as chemical studies are lively fields of current science. The ever-increasing beam intensities, feasible with new accelerator development, are crucial for the synthesis of superheavy elements because of the low cross sections for many of the reactions. Therefore, the development of target and backing materials with higher durability and experiment lifetime is increasingly important. Here we concentrate on the techniques necessary for the production of targets that are needed for experiments in this special field of interest. For the future, also development on target monitoring, target cooling, and beam intensity profile shaping techniques will play an important role, but are not in the focus of this article. [ABSTRACT FROM AUTHOR]

Published

2023

24. Toward Establishing an Ideal Adjuvant for Non-Inflammatory Immune Enhancement.

Author

Seya, Tsukasa, Tatematsu, Megumi, and Matsumoto, Misako

Subjects

IMMUNOLOGICAL adjuvants, AMINO acid sequence, DRUG discovery, DOUBLE-stranded RNA, NUCLEIC acids, TOLL-like receptors

Abstract

The vertebrate immune system functions to eliminate invading foreign nucleic acids and foreign proteins from infectious diseases and malignant tumors. Because pathogens and cancer cells have unique amino acid sequences and motifs (e.g., microbe-associated molecular patterns, MAMPs) that are recognized as "non-self" to the host, immune enhancement is one strategy to eliminate invading cells. MAMPs contain nucleic acids specific or characteristic of the microbe and are potential candidates for immunostimulants or adjuvants. Adjuvants are included in many vaccines and are a way to boost immunity by deliberately administering them along with antigens. Although adjuvants are an important component of vaccines, it is difficult to evaluate their efficacy ex vivo and in vivo on their own (without antigens). In addition, inflammation induced by currently candidate adjuvants may cause adverse events, which is a hurdle to their approval as drugs. In addition, the lack of guidelines for evaluating the safety and efficacy of adjuvants in drug discovery research also makes regulatory approval difficult. Viral double-stranded (ds) RNA mimics have been reported as potent adjuvants, but the safety barrier remains unresolved. Here we present ARNAX, a noninflammatory nucleic acid adjuvant that selectively targets Toll-like receptor 3 (TLR3) in antigen-presenting dendritic cells (APCs) to safely induce antigen cross-presentation and subsequently induce an acquired immune response independent of inflammation. This review discusses the challenges faced in the clinical development of novel adjuvants. [ABSTRACT FROM AUTHOR]

Published

2022

25. Validation of the Longitudinal Interval Follow-Up Evaluation for the Long-Term Measurement of Mood Symptoms in Bipolar Disorder.

Author

Porter, Richard J., Moot, Will, Inder, Maree L., Crowe, Marie T., Douglas, Katie M., Carter, Janet D., and Frampton, Christopher

Subjects

BIPOLAR disorder, RECEIVER operating characteristic curves, SYMPTOMS, PSYCHOTHERAPY patients, MANIA

Abstract

The long-term burden of symptoms is an important outcome in bipolar disorder (BD). A method which has minimal burden of assessment uses a retrospective interview, the Longitudinal Interval Follow-up Examination (LIFE), although this may be subject to problems with recall. This study examines the relationship between the retrospective LIFE scale and concurrently-rated mood rating scales in two clinical trials of 18 months of psychotherapy for patients with BD. The Montgomery-Asberg Depression Rating Scale (MADRS) and Young Mania Rating Scale (YMRS) were administered every eight to nine weeks and the LIFE was carried out every 6 months. Correlations between scores on mood rating scales and at equivalent times on the LIFE were examined, as well as of potential clinical moderators. There were significant correlations between LIFE depression ratings and concurrent MADRS score (r = 0.57) and between LIFE mania ratings and YMRS score (r = 0.40). In determining "mild depression" on the MADRS, a receiver operating characteristics (ROC) analysis showed an AUC of 0.78 for LIFE scores. Correlations, particularly for depression scores, were high even when the LIFE rating was several months before the interview, suggesting that the LIFE has validity in examining the burden of mood symptoms over time, with relatively little burden of assessment. Future research should examine the relationship between symptom burden and quality of life measured in this way. [ABSTRACT FROM AUTHOR]

Published

2022

26. Audiological Evidence of Frequent Hereditary Mild, Moderate and Moderate-to-Severe Hearing Loss.

Author

Markova, Tatiana, Alekseeva, Natalia, Lalayants, Maria, Ryzhkova, Oxana, Shatokhina, Olga, Galeeva, Nailya, Bliznetz, Elena, Belov, Oleg, Chibisova, Svetlana, Polyakov, Alexander, and Tavartkiladze, George

Abstract

Congenital and early onset bilateral sensorineural hearing loss (SNHL) is mainly caused by mutations in numerous genes. The introduction of universal newborn hearing screening (UNHS) has increased the number of infants with mild, moderate, and moderate-to-severe sensorineural hearing loss (SNHL) detected in the first year of life. We aimed to evaluate the audiological features in patients with mild, moderate, and moderate-to-severe SNHL according to genotype. Audiological and genetic data were analyzed for 251 patients and their relatives with congenital bilateral mild, moderate, and moderate-to-severe SNHL. Hearing loss severity, audiogram profile, interaural symmetry, and dynamics of hearing thresholds were analyzed. In this case, 165 patients had GJB2 gene mutations, 30 patients were identified with STRC mutations, and 16 patients had pathogenic or likely pathogenic USH2A mutations. The presence of at least one GJB2 non-truncating variant in genotype led to less severe hearing impairment. The flat and gently sloping audiogram profiles were mostly revealed in all groups. The follow-up revealed the stability of hearing thresholds. GJB2, STRC, and USH2A pathogenic variants were detected in most patients in our cohort and were congenital in most cases. [ABSTRACT FROM AUTHOR]

Published

2022

27. High Dose of Acute Normobaric Hypoxia Does Not Adversely Affect Sprint Interval Training, Cognitive Performance and Heart Rate Variability in Males and Females.

Author

Karayigit, Raci, Ramirez-Campillo, Rodrigo, Yasli, Burak Caglar, Gabrys, Tomasz, Benesova, Daniela, and Esen, Ozcan

Subjects

HIGH-intensity interval training, HEART beat, COGNITIVE ability, REACTION time, HYPOXEMIA, EXECUTIVE function

Abstract

Simple Summary: Sprint interval training (SIT) is a feasible and time-efficient alternative to classical endurance training that has gained popularity among athletes because of its ability to elicit physiological and cardiorespiratory adaptations in a shorter amount of time than traditional endurance training. Further, popular altitude/hypoxic training techniques include intermittent hypoxic training, in which athletes exercise at submaximal levels under simulated hypoxia while living at sea level (normoxia). Hypoxic exercise is likely a more potent stimulant to upregulate muscle factors (e.g., mitochondrial biogenesis, oxidative, and glycolytic enzymes) than similar normoxic exercise. However, SIT in hypoxia may disturb acute performance indices during sprint intervals. Hypoxia may also impair cognitive function. Acute hypoxia may decrease cognitive performance in areas such as memory and executive functioning. Moreover, males and females may have distinct athletic performance responses to SIT and hypoxia. However, to date, there is no study that has investigated the effects of different doses of acute normobaric hypoxia on SIT and cognitive performance, nor has there been research investigating potential sex-based differences. Although preliminary studies suggested sex-related differences in physiological responses to hypoxia, the effects of sex on sprint interval training (SIT) performance in different degrees of hypoxia are largely lacking. The aim of this study was to examine the acute effect of different doses of normobaric hypoxia on SIT performance as well as heart rate variability (HRV) and cognitive performance (CP) in amateur-trained team sport players by comparing potential sex differences. In a randomized, double-blind, crossover design, 26 (13 females) amateur team-sport (football, basketball, handball, rugby) players completed acute SIT (6 × 15 s all-out sprints, separated with 2 min active recovery, against a load equivalent to 9% of body weight) on a cycle ergometer, in one of four conditions: (I) normoxia without a mask (FiO2: 20.9%) (CON); (II) normoxia with a mask (FiO2: 20.9%) (NOR); (III) moderate hypoxia (FiO2: 15.4%) with mask (MHYP); and (IV) high hypoxia (FiO2: 13.4%) with mask (HHYP). Peak (PPO) and mean power output (MPO), HRV, heart rate (HR), CP, capillary lactate (BLa), and ratings of perceived exertion (RPE) pre- and post-SIT were compared between CON, NOR, MHYP and HHYP. There were no significant differences found between trials for PPO (p = 0.55), MPO (p = 0.44), RPE (p = 0.39), HR (p = 0.49), HRV (p > 0.05) and CP (response accuracy: p = 0.92; reaction time: p = 0.24). The changes in MP, PP, RPE, HR, CP and HRV were similar between men and women (all p > 0.05). While BLa was similar (p = 0.10) between MHYP and HHYP trials, it was greater compared to CON (p = 0.01) and NOR (p = 0.01), without a sex-effect. In conclusion, compared to normoxia, hypoxia, and wearing a mask, have no effect on SIT acute responses (other than lactate), including PP, MP, RPE, CP, HR, and cardiac autonomic modulation either in men or women. [ABSTRACT FROM AUTHOR]

Published

2022

28. Predicting Remission among Perinatal Women with Depression in Rural Pakistan: A Prognostic Model for Task-Shared Interventions in Primary Care Settings.

Author

Waqas, Ahmed, Sikander, Siham, Malik, Abid, Atif, Najia, Karyotaki, Eirini, and Rahman, Atif

Subjects

DEPRESSION in women, RURAL women, PROGNOSTIC models, PRIMARY care, MENTAL depression, SELF-efficacy

Abstract

Perinatal depression is highly prevalent in low- and middle-income countries (LMICs) and is associated with adverse maternal and child health consequences. Task-shared psychological and psychosocial interventions for perinatal depression have demonstrated clinical and cost-effectiveness when delivered on a large scale. However, task-sharing approaches, especially in LMICs, require an effective mechanism, whereby clients who are not likely to benefit from such interventions are identified from the outset so that they can benefit from higher intensity treatments. Such a stratified approach can ensure that limited resources are utilized appropriately and effectively. The use of standardized and easy-to-implement algorithmic devices (e.g., nomograms) could help with such targeted dissemination of interventions. The present investigation posits a prognostic model and a nomogram to predict the prognosis of perinatal depression among women in rural Pakistan. The nomogram was developed to deliver stratified model of care in primary care settings by identifying those women who respond well to a non-specialist delivered intervention and those requiring specialist care. This secondary analysis utilized data from 903 pregnant women with depression who participated in a cluster randomized, controlled trial that tested the effectiveness of the Thinking Healthy Program in rural Rawalpindi, Pakistan. The participants were recruited from 40 union councils in two sub-districts of Rawalpindi and randomly assigned to intervention and enhanced usual care. Sixteen sessions of the THP intervention were delivered by trained community health workers to women with depression over pregnancy and the postnatal period. A trained assessment team used the Structured Clinical Interview for DSM-IV current major depressive episode module to diagnose major depressive disorder at baseline and post-intervention. The intervention received by the participants emerged as the most significant predictor in the prognostic model. Among clinical factors, baseline severity of core-emotional symptoms emerged as an essential predictor, followed by atypical symptoms and insomnia. Higher severity of these symptoms was associated with a poorer prognosis. Other important predictors of a favorable prognosis included support from one's mother or mother-in-law, financial empowerment, higher socioeconomic class, and living in a joint family system. This prognostic model yielded acceptable discrimination (c-statistic = 0.75) and calibration to aid in personalized delivery of the intervention. [ABSTRACT FROM AUTHOR]

Published

2022

29. Simultaneous Bilateral Frontal and Bilateral Cerebellar Transcranial Direct Current Stimulation in Treatment-Resistant Depression—Clinical Effects and Electrical Field Modelling of a Novel Electrodes Montage.

Author

D'Urso, Giordano, Dini, Michelangelo, Bonato, Marta, Gallucci, Silvia, Parazzini, Marta, Maiorana, Natale, Bortolomasi, Marco, Priori, Alberto, and Ferrucci, Roberta

Subjects

TRANSCRANIAL direct current stimulation, HAMILTON Depression Inventory, INDUCTIVE effect, ELECTRODES, BRAIN stimulation

Abstract

Depressive disorders are one of the leading causes of disability worldwide. Transcranial direct current stimulation (tDCS) is a safe, simple, non-invasive brain stimulation technique showing considerable effectiveness in improving depressive symptoms. Most studies to date have applied anodal tDCS to the left dorsolateral prefrontal cortex (DLPFC), in line with the hypothesis that depressed patients exhibit relative hypoactivity in the left DLPFC compared to the right. Considering the emerging role of the cerebellum in emotional processes, we aimed to study the effect of combining bilateral cerebellar tDCS with the commonly used bifrontal stimulation in patients with severe depression. This open-label pilot study entailed the simultaneous administration of bilateral cerebellar (anode over the left cerebellum, cathode over the right cerebellum) and bilateral frontal (anode over the left DLPFC, cathode over the right DLPFC) tDCS to patients (N = 12) with treatment-resistant depression. The 21-item Hamilton Depression Rating Scale (HDRS) and Beck's Depression Inventory-II (BDI-II) were selected as outcome measures. Electric fields distribution originating from this novel electrode montage was obtained by a computational method applied to a realistic human head model. We observed a 30% reduction of both clinician-rated and self-reported severity of depressive symptoms after only five days (10 sessions) of treatment. Younger age was associated with greater clinical improvement. Adverse events were similar to those of the conventional electrodes montage. The modelling studies demonstrated that the electric fields generated by each pair of electrodes are primarily distributed in the cortical areas under the electrodes. In conclusion, the cerebellum could represent a promising adjunctive target for tDCS interventions in patients with TRD, particularly for younger patients. [ABSTRACT FROM AUTHOR]

Published

2022

30. Novel Functions of Integrins as Receptors of CD154: Their Role in Inflammation and Apoptosis.

Author

Hassan, Ghada S., Salti, Suzanne, and Mourad, Walid

Subjects

INFLAMMATORY mediators, CANCER cells, MYELOID cells, APOPTOSIS, INTEGRINS, T cells

Abstract

CD154, an inflammatory mediator also known as CD40 ligand, has been identified as a novel binding partner for some members of the integrin family. The αIIbβ3, specifically expressed on platelets, was the first integrin to be described as a receptor for CD154 after CD40. Its interaction with soluble CD154 (sCD154) highly contributes to thrombus formation and stability. Identifying αIIbβ3 opened the door for investigating other integrins as partners of CD154. The αMβ2 expressed on myeloid cells was shown capable of binding CD154 and contributing as such to cell activation, adhesion, and release of proinflammatory mediators. In parallel, α5β1 communicates with sCD154, inducing pro-inflammatory responses. Additional pathogenic effects involving apoptosis-preventing functions were exhibited by the CD154–α5β1 dyad in T cells, conferring a role for such interaction in the survival of malignant cells, as well as the persistence of autoreactive T cells. More recently, CD154 receptors integrated two new integrin members, αvβ3 and α4β1, with little known as to their biological significance in this context. This article provides an overview of the novel role of integrins as receptors of CD154 and as critical players in pro-inflammatory and apoptotic responses. [ABSTRACT FROM AUTHOR]

Published

2022

31. Cautionary Observations Concerning the Introduction of Psychophysiological Biomarkers into Neuropsychiatric Practice.

Author

Rapp, Paul E., Cellucci, Christopher, Darmon, David, and Keyser, David

Published

2022

32. High Temperature Superconducting Flux Pumps for Contactless Energization.

Author

Wen, Zezhao, Zhang, Hongye, and Mueller, Markus

Subjects

HIGH temperature superconductors, SUPERCONDUCTING magnets, SUPERCONDUCTING coils, POWER electronics, ELECTRICAL energy, ELECTRIC machines, FLUX pinning, MAGNETS

Abstract

The development of superconducting technology has seen continuously increasing interest, especially in the area of clean power systems and electrification of transport with low CO2 emission. Electric machines, as the major producer and consumer of the global electrical energy, have played a critical role in achieving zero carbon emission. The superior current carrying capacity of superconductors with zero DC loss opens the way to the next-generation electric machines characterized by much higher efficiency and power density compared to conventional machines. The persistent current mode is the optimal working condition for a superconducting magnet, and thus the energization of superconducting field windings has become a crucial challenge to be tackled, to which high temperature superconducting (HTS) flux pumps have been proposed as a promising solution. An HTS flux pump enables current injection into a closed superconducting coil wirelessly and provides continuous compensation to offset current decay, avoiding excessive cryogenic losses and sophisticated power electronics facilities. Despite many publications regarding the design and analyses of various types of HTS flux pumps, the practical application of HTS flux pumps in a high-performance superconducting machine has been rarely reported. Therefore, it is of significance to specify the main challenges for building and implementing a reliable HTS flux pump. In addition, the physical mechanisms of distinct HTS flux pumps have caused some confusion, which should be clarified. Above all, a systematic review of the recent development and progress of HTS flux pumps remains lacking. Given the above-mentioned issues, this paper summarized the most up-to-date advances of this emerging technology, clarified the working mechanisms and commonly adopted modeling approaches, presented objective analyses of the applicability of various HTS flux pumps, specified the primary challenges for implementing HTS flux pumps, and proposed useful suggestions to improve this wireless excitation technology. The overall aim of this work is to bring a deep insight into the understanding of HTS flux pumps and provide comprehensive guidance for their future research and applications. [ABSTRACT FROM AUTHOR]

Published

2022

33. Host phenology can drive the evolution of intermediate virulence strategies in some obligate‐killer parasites.

Author

MacDonald, Hannelore, Akçay, Erol, and Brisson, Dustin

Subjects

PHENOLOGY, PARASITES, ECOLOGICAL impact, PLANT phenology, SEASONS

Abstract

Traditional mechanistic trade‐offs between transmission and virulence are the foundation of nearly all theory on parasite virulence evolution. For obligate‐host killer parasites, evolution toward intermediate virulence depends on a trade‐off between virulence (time to death) and transmission (the number of progeny released upon death). Although several ecological factors impact optimal virulence strategies constrained by trade‐offs, these factors have been insufficient to explain the intermediate virulence levels observed in nature. The timing of seasonal activity, or phenology, is a factor that commonly influences ecological interactions but is difficult to incorporate into virulence evolution studies. We present a mathematical model of a seasonal obligate‐killer parasite to study the impact of host phenology on virulence evolution. The model demonstrates that host phenology can select for intermediate parasite virulence even when a traditional mechanistic trade‐off between transmission and virulence is omitted. The optimal virulence strategy is impacted by both the host activity period duration and the host emergence timing variation. Parasites with lower virulence strategies are favored in environments with longer host activity periods and when hosts emerge synchronously. The results demonstrate that host phenology can be sufficient to select for intermediate virulence strategies, providing an alternative driver of virulence evolution in some natural systems. [ABSTRACT FROM AUTHOR]

Published

2022

34. Recent Advancements in Enhancing Antimicrobial Activity of Plant-Derived Polyphenols by Biochemical Means.

Author

Panda, Likun and Duarte-Sierra, Arturo

Subjects

PLANT polyphenols, HORSERADISH peroxidase, POLYPHENOLS, ANTI-infective agents, VITAMIN C, MAILLARD reaction

Abstract

Plants are a reservoir of phytochemicals, which are known to possess several beneficial health properties. Along with all the secondary metabolites, polyphenols have emerged as potential replacements for synthetic additives due to their lower toxicity and fewer side effects. However, controlling microbial growth using these preservatives requires very high doses of plant-derived compounds, which limits their use to only specific conditions. Their use at high concentrations leads to unavoidable changes in the organoleptic properties of foods. Therefore, the biochemical modification of natural preservatives can be a promising alternative to enhance the antimicrobial efficacy of plant-derived compounds/polyphenols. Amongst these modifications, low concentration of ascorbic acid (AA)–Cu (II), degradation products of ascorbic acid (DPAA), Maillard reaction products (MRPs), laccase–mediator (Lac–Med) and horse radish peroxidase (HRP)–H2O2 systems standout. This review reveals the importance of plant polyphenols, their role as antimicrobial agents, the mechanism of the biochemical methods and the ways these methods may be used in enhancing the antimicrobial potency of the plant polyphenols. Ultimately, this study may act as a base for the development of potent antimicrobial agents that may find their use in food applications. [ABSTRACT FROM AUTHOR]

Published

2022

35. Understanding the Bioactivity and Prognostic Implication of Commonly Used Surface Antigens in Multiple Myeloma.

Author

Lebel, Eyal, Nachmias, Boaz, Pick, Marjorie, Gross Even-Zohar, Noa, and Gatt, Moshe E.

Subjects

CELL surface antigens, MULTIPLE myeloma, PROGNOSIS, MESENCHYMAL stem cells, PLASMA cells

Abstract

Multiple myeloma (MM) progression is dependent on its interaction with the bone marrow microenvironment and the immune system and is mediated by key surface antigens. Some antigens promote adhesion to the bone marrow matrix and stromal cells, while others are involved in intercellular interactions that result in differentiation of B-cells to plasma cells (PC). These interactions are also involved in malignant transformation of the normal PC to MM PC as well as disease progression. Here, we review selected surface antigens that are commonly used in the flow cytometry analysis of MM for identification of plasma cells (PC) and the discrimination between normal and malignant PC as well as prognostication. These include the markers: CD38, CD138, CD45, CD19, CD117, CD56, CD81, CD27, and CD28. Furthermore, we will discuss the novel marker CD24 and its involvement in MM. The bioactivity of each antigen is reviewed, as well as its expression on normal vs. malignant PC, prognostic implications, and therapeutic utility. Understanding the role of these specific surface antigens, as well as complex co-expressions of combinations of antigens, may allow for a more personalized prognostic monitoring and treatment of MM patients. [ABSTRACT FROM AUTHOR]

Published

2022

36. Upregulated Proteasome Subunits in COVID-19 Patients: A Link with Hypoxemia, Lymphopenia and Inflammation.

Author

Alfaro, Enrique, Díaz-García, Elena, García-Tovar, Sara, Zamarrón, Ester, Mangas, Alberto, Galera, Raúl, López-Collazo, Eduardo, García-Rio, Francisco, and Cubillos-Zapata, Carolina

Subjects

COVID-19, PROTEOLYSIS, LYMPHOPENIA, HYPOXEMIA, IMMUNOREGULATION, LYMPHOCYTE count, GENETIC overexpression

Abstract

Severe COVID-19 disease leads to hypoxemia, inflammation and lymphopenia. Viral infection induces cellular stress and causes the activation of the innate immune response. The ubiquitin-proteasome system (UPS) is highly implicated in viral immune response regulation. The main function of the proteasome is protein degradation in its active form, which recognises and binds to ubiquitylated proteins. Some proteasome subunits have been reported to be upregulated under hypoxic and hyperinflammatory conditions. Here, we conducted a prospective cohort study of COVID-19 patients (n = 44) and age-and sex-matched controls (n = 20). In this study, we suggested that hypoxia could induce the overexpression of certain genes encoding for subunits from the α and β core of the 20S proteasome and from regulatory particles (19S and 11S) in COVID-19 patients. Furthermore, the gene expression of proteasome subunits was associated with lymphocyte count reduction and positively correlated with inflammatory molecular and clinical markers. Given the importance of the proteasome in maintaining cellular homeostasis, including the regulation of the apoptotic and pyroptotic pathways, these results provide a potential link between COVID-19 complications and proteasome gene expression. [ABSTRACT FROM AUTHOR]

Published

2022

37. Wohlfahrtsstaat und Interessenorganisationen im Wandel

Author

Schroeder, Wolfgang, Schulze, Michaela, Schroeder, Wolfgang, and Schulze, Michaela

Subjects

Welfare state--Germany, Pressure groups--Germany

Abstract

Interest groups within the context of changing welfare states have gained widespread attention within the social sciences. Welfare states and interest groups are being faced with new challenges (e.g. in the context of several changes, such as new social risks). Schwache Interessen (weak interests) (such as poorly qualified ones) are also gaining more attention. This book discusses several different fields of interest representation in the welfare state. It analyses in what way constellations of interest representation have changed in modified welfare state environments. Several different organisations are analysed, including labour unions, the employers'association and political parties. Moreover, the book also takes umbrella organisations of municipalities, social courts and educational policymakers into account. Until now, they have gained little attention from scholars. With contributions by: Lena Brüsewitz, Imke Friedrich, Sascha Kristin Futh, Tanja Klenk, Ulrike A.C. Müller, Frank Nullmeier, Sabine Ruß-Sattar, Friedbert Rüb, Wolfgang Schroeder, Benedikt Schreiter, Michaela Schulze, Florian Steinmüller, Christoph Strünck, Felix Welti

Published

2019

38. Breakup reactions and their ambiguities.

Author

Gómez-Ramos, M., Obertelli, A., and Sun, Y. L.

Subjects

AMBIGUITY, BIG data

Abstract

We review the ambiguities in the nuclear information extracted from breakup reactions, focusing on those originating from the description of the reaction mechanism and the overall ambiguity inherent to their interpretation in terms of shell occupancies. We present the current discussion about nucleon knockout reactions and how the understanding of the reaction mechanism would help reducing uncertainties. For the former, we consider the case of 11 Li, due to the existing large data set. For the latter, we recall the paradigmatic example of the electro-dissociation of the deuteron to address the question of the scale and scheme dependence from the theoretical framework used for the interpretation. [ABSTRACT FROM AUTHOR]

Published

2021

39. Polarization Radiometric Calibration in Laboratory for a Channeled Spectropolarimeter.

Author

Xing, Wenhe, Ju, Xueping, Bo, Jian, Yan, Changxiang, Yang, Bin, Xu, Shuyan, and Zhang, Junqiang

Subjects

STOKES parameters, OPTICAL polarization, CALIBRATION, ACCURACY of information, OPTICAL properties, MULTISPECTRAL imaging

Abstract

The process of radiometric calibration would be coupled with the polarization properties of an optical system for spectropolarimetry, which would have significant influences on reconstructed Stokes parameters. In this paper, we propose a novel polarization radiometric calibration model that decouples the radiometric calibration coefficient and polarization properties of an optical system. The alignment errors of the polarization module and the variation of the retardations at different fields of view are considered and calibrated independently. According to these calibration results, the input Stokes parameters at different fields of view can be reconstructed accurately through the proposed model. Simulations are performed for the presented calibration and reconstruction methods, which indicate that the measurement accuracy of polarization information is improved compared with the traditional undecoupled calibration method. [ABSTRACT FROM AUTHOR]

Published

2020

40. Ihog proteins contribute to integrin-mediated focal adhesions.

Author

Qi Y, Liu H, Zhang K, Wu Y, Shen C, and Lin X

Subjects

Animals, Cell Adhesion, Drosophila metabolism, Drosophila melanogaster genetics, Drosophila melanogaster metabolism, Mammals, Membrane Glycoproteins, Receptors, Cell Surface, Drosophila Proteins genetics, Focal Adhesions metabolism, Hedgehog Proteins genetics, Integrins genetics

Abstract

Integrin expression forms focal adhesions, but how this process is physiologically regulated is unclear. Ihog proteins are evolutionarily conserved, playing roles in Hedgehog signaling and serving as trans-homophilic adhesion molecules to mediate cell-cell interactions. Whether these proteins are also engaged in other cell adhesion processes remains unknown. Here, we report that Drosophila Ihog proteins function in the integrin-mediated adhesions. Removal of Ihog proteins causes blister and spheroidal muscle in wings and embryos, respectively. We demonstrate that Ihog proteins interact with integrin via the extracellular portion and that their removal perturbs integrin distribution. Finally, we show that Boc, a mammalian Ihog protein, rescues the embryonic defects caused by removing its Drosophila homologs. We thus propose that Ihog proteins contribute to integrin-mediated focal adhesions., (© 2022. Science China Press and Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2023

41. Screening key lncRNAs with diagnostic and prognostic value for head and neck squamous cell carcinoma based on machine learning and mRNA-lncRNA co-expression network analysis.

Author

Hu, Ying, Guo, Geyang, Li, Junjun, Chen, Jie, and Tan, Pingqing

Subjects

SQUAMOUS cell carcinoma, MACHINE learning, FOCAL adhesions, SUPPORT vector machines, POLYMERASE chain reaction

Abstract

BACKGROUND: Head and neck squamous cell carcinoma (HNSCC) is the seventh most common type of cancer around the world. The aim of this study was to seek the long non-coding RNAs (lncRNAs) acting as diagnostic and prognostic biomarker of HNSCC. METHODS: Base on TCGA dataset, the differentially expressed mRNAs (DEmRNAs) and lncRNAs (DElncRNAs) were identified between HNSCC and normal tissue. The machine learning and survival analysis were performed to estimate the potential diagnostic and prognostic value of lncRNAs for HNSCC. We also build the co-expression network and functional annotation. The expression of selected candidate mRNAs and lncRNAs were validated by Quantitative real time polymerase chain reaction (qRT-PCR). RESULTS: A total of 3363 DEmRNAs (1822 down-regulated and 1541 up-regulated mRNAs) and 32 DElncRNAs (13 down-regulated and 19 up-regulated lncRNAs) between HNSCC and normal tissue were obtained. A total of 13 lncRNAs (IL12A.AS1, RP11.159F24.6, RP11.863P13.3, LINC00941, FOXCUT, RNF144A.AS1, RP11.218E20.3, HCG22, HAGLROS, LINC01615, RP11.351J23.1, AC024592.9 and MIR9.3HG) were defined as optimal diagnostic lncRNAs biomarkers for HNSCC. The area under curve (AUC) of the support vector machine (SVM) model, decision tree model and random forests model and were 0.983, 0.842 and 0.983, and the specificity and sensitivity of the three model were 95.5% and 96.2%, 77.3% and 97.6% and 93.2% and 97.8%, respectively. Among them, AC024592.9, LINC00941, LINC01615 and MIR9-3HG was not only an optimal diagnostic lncRNAs biomarkers, but also related to survival time. The focal adhesion, ECM-receptor interaction, pathways in cancer and cytokine-cytokine receptor interaction were four significantly enriched pathways in DEmRNAs co-expressed with the identified optimal diagnostic lncRNAs. But for most of the selected DEmRNAs and DElncRNAs, the expression was consistent with our integrated analysis results, including LINC00941, LINC01615, FOXCUT, TGA6 and MMP13. CONCLUSION: AC024592.9, LINC00941, LINC01615 and MIR9-3HG was not only an optimal diagnostic lncRNAs biomarkers, but also were a prognostic lncRNAs biomarkers. [ABSTRACT FROM AUTHOR]

Published

2020

42. Comorbidity between pain and mental illness - Evidence of a bidirectional relationship.

Author

Bondesson, E., Larrosa Pardo, F., Stigmar, K., Ringqvist, Å., Petersson, I. F., Jöud, A., and Schelin, M. E. C.

Abstract

Background: Pain from various locations in the body and mental illness are common and the comorbidity between the two is well-known although the temporal relationship remains to be determined. Our aim was to follow patients over time to study if pain (here dorsalgia/abdominal pain) or fibromyalgia lead to an increased risk of developing mental illness (here depression/anxiety) and/or the reverse, that is whether patients with mental illness have an increased risk to develop pain or fibromyalgia, compared to the rest of the population.Methods: This prospective cohort study used the Skåne Healthcare Register, covering all care in the region of Skåne, southern Sweden (population ~1.3 million). The cohort included healthcare consultations in primary care, outpatient specialized care and inpatient care between 2007 and 2016 for all patients without prior registered diagnosis of mental illness or pain, aged 18 or older (n = 504,365).Results: The incidence rate ratio (IRR) for developing mental illness after pain was 2.18 (95% CI = 2.14-2.22) compared to without pain. IRR for developing pain after mental illness was 2.02 (95% CI = 1.98-2.06) compared to without mental illness. Corresponding IRR for developing mental illness after fibromyalgia was 4.05 (95% CI = 3.58-4.59) and for developing fibromyalgia after mental illness 5.54 (95% CI = 4.99-6.16).Conclusions: This study shows a bidirectional influence of similar magnitude of pain and mental illness, respectively. In monitoring patients with pain or mental illness, a focus on both conditions is thus important to develop appropriate, targeted interventions and may increase the likelihood of improved outcomes.Significance: We followed a population-based cohort over a period of 10 years, including incident cases of both exposure and outcome and found a bidirectional relationship between pain and mental illness. Clinicians need to pay attention on both conditions, in patients seeking care due to mental illness or pain. [ABSTRACT FROM AUTHOR]

Published

2018

43. Iatrogenic immunosuppression and risk of non-Hodgkin lymphoma in solid organ transplantation: A population-based cohort study in Australia.

Author

Na, Renhua, Laaksonen, Maarit A., Grulich, Andrew E., Meagher, Nicola S., McCaughan, Geoffrey W., Keogh, Anne M., and Vajdic, Claire M.

Subjects

IMMUNOSUPPRESSION, LYMPHOMAS, IMMUNOSUPPRESSIVE agents, AZATHIOPRINE, TRANSPLANTATION of organs, tissues, etc.

Abstract

Iatrogenic immunosuppression is a strong risk factor for non-Hodgkin lymphoma ( NHL) but the dose-related association between individual immunosuppressive agents and NHL risk is unknown. We conducted a population-based cohort study of 4131 adult Australian liver, heart and lung transplant recipients (1984-2006). We ascertained NHL incidence by probabilistic record linkage between transplant registries and the Australian Cancer Database, and abstracted risk factor data at transplantation and at regular intervals thereafter from medical records. We estimated adjusted hazard ratios ( HR) for early (<1 year after transplantation; n = 29) and late (≥1 year; n = 61) NHL using the Fine and Gray proportional subdistribution hazards model that accounted for death as a competing risk. After adjustment for immunosuppression, the risk of both early and late NHL did not significantly differ by organ type. In final models, higher mean daily doses of azathioprine were associated with increased risk of both early [ HR 2·20, 95% confidence interval ( CI): 1·21-4·01] and late NHL ( HR 1·78, 95% CI: 1·12-2·84). There was no association between any other maintenance immunosuppressive agent and NHL risk. This study provides evidence that differences in immunosuppression may explain variation in NHL incidence by organ type, and high doses of azathioprine may independently predict NHL risk. [ABSTRACT FROM AUTHOR]

Published

2016

44. SMILR Aggravates the Progression of Atherosclerosis by Sponging miR-10b-3p to Regulate KLF5 Expression.

Author

Li H, Pan Z, Chen Q, Yang Z, and Zhang D

Subjects

Animals, Atherosclerosis pathology, Cell Proliferation physiology, Gene Expression, Humans, Kruppel-Like Transcription Factors genetics, Mice, MicroRNAs genetics, Muscle, Smooth, Vascular pathology, Myocytes, Smooth Muscle pathology, RNA, Long Noncoding genetics, RNA, Long Noncoding metabolism, U937 Cells, Atherosclerosis metabolism, Disease Progression, Kruppel-Like Transcription Factors biosynthesis, MicroRNAs metabolism, Muscle, Smooth, Vascular metabolism, Myocytes, Smooth Muscle metabolism

Abstract

Over the past few decades, long noncoding RNAs (lncRNAs) have been widely accepted to be involved in various diseases, and smooth muscle enriched long noncoding RNA (SMILR) was reported to participate in the proliferation of vascular smooth muscle cells (VSMCs). Nevertheless, the molecular mechanisms of SMILR in atherosclerosis (AS) have not been fully explored. In this study, VSMCs and human mononuclear cells (U937) treated with oxidized low-density lipoprotein (ox-LDL) were used as cell models of AS. We found that the expression of SMILR was upregulated in the serum of AS patients and ox-LDL-induced AS cell models. SMILR knockdown inhibited cell proliferation while increasing cell apoptosis in the AS cell models. In addition, SMILR acted as a sponge for miR-10b-3p, and miR-10b-3p counteracted SMILR-mediated regulation of AS. Moreover, we confirmed that miR-10b-3p could bind with KLF5, and SMILR regulated KLF5 expression by competitively binding miR-10b-3p. Furthermore, miR-10b-3p modulated cell proliferation and apoptosis in AS by targeting KLF5. Finally, miR-10b-3p regulated AS progression in vivo by targeting KLF5. Overall, our study demonstrated that SMILR participated in the progression of AS by targeting the miR-10b-3p/KLF5 axis, which may provide some clues for future studies of AS.

Published

2020

45. Heat treatment enhances the antimicrobial activity of (+)-Catechin when combined with copper sulphate.

Author

Holloway, A.C., Mueller‐Harvey, I., Gould, S.W.J., Fielder, M.D., Naughton, D.P., and Kelly, A.F.

Subjects

HEAT treatment, ANTI-infective agents, STRUCTURE-activity relationships, CATECHIN, COPPER sulfate, FLAVANOLS, COMPARATIVE studies

Abstract

The aim of the study was to compare the antimicrobial activities of freshly made, heat-treated (HT) and 14 day stored (+)-Catechin solutions with (+)-catechin flavanol isomers in the presence of copper sulphate. (+)-Catechin activity was investigated when combined with different ratios of Cu2+; 100°C heat treatment; autoclaving; and 14 day storage against Staphylococcus aureus. Cu2+-(+)-Catechin complexation, isomer structure-activity relationships, and H2O2 generation were also investigated. Freshly made, HT, and 14 day stored flavanols showed no activity. While combined Cu2+-autoclaved (+)-Catechin and -HT(+)-Catechin activities were similar, HT(+)-Catechin was more active than either freshly made (+)-catechin (generating more H2O2) or (−)-Epicatechin (though it generated less H2O2) or 14 day-(+)-Catechin (which had similar activity to Cu2+ controls-although it generated more H2O2). When combined with Cu2+, in terms of rates of activity, HT(+)-Catechin was lower than (−)-Epigallocatechin gallate and greater than freshly made (+)-Catechin. Freshly made and HT(+)-Catechin formed acidic complexes with Cu2+ as indicated by pH and UV-vis measurements although pH changes did not account for antimicrobial activity. Freshly made and HT(+)-Catechin both formed Cu2+ complexes. The HT(+)-Catechin complex generated more H2O2 which could explain its higher antimicrobial activity. Significance and Impact of the Study Natural products attract considerable attention in the search for novel antimicrobials, prebiotics and antioxidants. Enhanced biological activity of natural products has been demonstrated with chemical and heat treatment. This article extends the few publications on heat treatments of plant products and combinations with adjuncts, to raise antimicrobial activity against pathogens such as Staphylococcus aureus. We demonstrated that heat treatment could increase the activity of (+)-Catechin, a weak antimicrobial flavanol found commonly in plants in the presence of copper sulphate. Heat treatment of readily available resources merits consideration in the development of more potent substances for use in clinical settings and agriculture. [ABSTRACT FROM AUTHOR]

Published

2015

46. Knowns and Unknowns about CAR-T Cell Dysfunction.

Author

Titov, Aleksei, Kaminskiy, Yaroslav, Ganeeva, Irina, Zmievskaya, Ekaterina, Valiullina, Aygul, Rakhmatullina, Aygul, Petukhov, Alexey, Miftakhova, Regina, Rizvanov, Albert, and Bulatov, Emil

Subjects

CELLULAR therapy, CELL receptors, CELLULAR aging, CELLULAR signal transduction, TUMORS, T cells, EPIGENOMICS, IMMUNOTHERAPY

Abstract

Simple Summary: The primary issue of adoptive cell therapy is the poor in vivo persistence. In this context, it is necessary to clarify the fundamental mechanisms of T cell dysfunction. Here we review common dysfunctional states, including exhaustion and senescence, and discuss the challenges associated with phenotypical characterization of these T cell subsets. We overview the heterogeneity among exhausted T cells as well as mechanisms by which T cells get reinvigorated by checkpoint inhibitors. We emphasize that some cancers not responding to such treatment may activate distinct T cell dysfunction programs. Finally, we describe the dysfunction-promoting mechanisms specific for CAR-T cells and the ways to mitigate them. Immunotherapy using chimeric antigen receptor (CAR) T cells is a promising option for cancer treatment. However, T cells and CAR-T cells frequently become dysfunctional in cancer, where numerous evasion mechanisms impair antitumor immunity. Cancer frequently exploits intrinsic T cell dysfunction mechanisms that evolved for the purpose of defending against autoimmunity. T cell exhaustion is the most studied type of T cell dysfunction. It is characterized by impaired proliferation and cytokine secretion and is often misdefined solely by the expression of the inhibitory receptors. Another type of dysfunction is T cell senescence, which occurs when T cells permanently arrest their cell cycle and proliferation while retaining cytotoxic capability. The first section of this review provides a broad overview of T cell dysfunctional states, including exhaustion and senescence; the second section is focused on the impact of T cell dysfunction on the CAR-T therapeutic potential. Finally, we discuss the recent efforts to mitigate CAR-T cell exhaustion, with an emphasis on epigenetic and transcriptional modulation. [ABSTRACT FROM AUTHOR]

Published

2022

47. Heterologous Prime-Boost Vaccination with a Peptide-Based Vaccine and Viral Vector Reshapes Dendritic Cell, CD4+ and CD8+ T Cell Phenotypes to Improve the Antitumor Therapeutic Effect.

Author

Hofer, Tamara, Rossi, Matteo, Carboni, Susanna, Di Berardino Besson, Wilma, von Laer, Dorothee, Wollmann, Guido, Derouazi, Madiha, and Santiago-Raber, Marie-Laure

Subjects

DENDRITIC cells, BIOLOGICAL models, VIRAL antigens, IMMUNIZATION, ANIMAL experimentation, PEPTIDE vaccines, CANCER vaccines, T cells, TUMORS, TUMOR antigens, MICE, PEPTIDES, IMMUNOTHERAPY

Abstract

Simple Summary: Developing new therapeutic cancer vaccines is of paramount importance to counteract tumor escape observed after conventional therapies in certain types of cancer. We have previously shown that the combination of two different vaccine platforms, targeting tumor-specific antigens, resulted in potent immune responses in preclinical models. Here, we show that the heterologous prime-boost combination with a protein vaccine and a viral vector vesicular stomatitis virus immunologically reshapes the immune-excluded TC-1 tumor model as well as the inflamed MC-38 tumor model, leading to beneficial therapeutic efficacy. Furthermore, the treatment with a multi-epitope vaccine allowed us to appreciate the various repartition among three antigen-specific cytotoxic T-cell responses combined with the viral boost. The combination leads to improved efficacy in all animals and highlights the importance of combining tumor epitopes. Our vaccine strategy could be further extended to prophylactic cancer vaccines and beyond, for infectious diseases. Heterologous prime-boost settings with a protein vaccine and the viral vector vesicular stomatitis virus, both expressing tumor-associated antigens (KISIMA-TAA and VSV-GP-TAA), have been previously shown to generate potent antitumor immunity. In the cold TC-1 model (HPV antigen) and the immune-infiltrate MC-38 model (Adpgk, Reps1 and Rpl18 neo-antigens), we further investigated pivotal immune cells that educate CD8+ T cells. Heterologous prime-boost vaccination induced a superior antitumor response characterized by the increase in number and functionality of antigen-specific CD8+ T cells, recruitment of cross-presenting dendritic cells, and polarization of CD4+ T cells towards an antitumor Th1 phenotype within the tumor and tumor-draining lymph nodes, turning the cold TC-1 tumor into a hot, inflamed tumor. In the inflamed MC-38 tumor model, treatment combination markedly prolonged the overall survival of mice. Treatment with multi-epitope vaccines also induced high frequencies of multiple antigen specificities in the periphery and in the tumor. Prime-boost treatment reduced tumor-infiltrating regulatory CD4+ T cells whilst increasing cross-presenting dendritic cells in tumor-draining lymph nodes. In conclusion, heterologous prime-boost vaccination possesses the ability to induce a potent anti-tumor response in both immune-excluded and immune-infiltrated mouse tumor models. Additionally, this study highlights the design of a multi-epitope vaccine for cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2021

48. Current Adenosinergic Therapies: What Do Cancer Cells Stand to Gain and Lose?

Author

Kotulová, Jana, Hajdúch, Marián, and Džubák, Petr

Subjects

TUMOR microenvironment, CELL receptors, ADENOSINES, STROMAL cells, IMMUNOTHERAPY

Abstract

A key objective in immuno-oncology is to reactivate the dormant immune system and increase tumour immunogenicity. Adenosine is an omnipresent purine that is formed in response to stress stimuli in order to restore physiological balance, mainly via anti-inflammatory, tissue-protective, and anti-nociceptive mechanisms. Adenosine overproduction occurs in all stages of tumorigenesis, from the initial inflammation/local tissue damage to the precancerous niche and the developed tumour, making the adenosinergic pathway an attractive but challenging therapeutic target. Many current efforts in immuno-oncology are focused on restoring immunosurveillance, largely by blocking adenosine-producing enzymes in the tumour microenvironment (TME) and adenosine receptors on immune cells either alone or combined with chemotherapy and/or immunotherapy. However, the effects of adenosinergic immunotherapy are not restricted to immune cells; other cells in the TME including cancer and stromal cells are also affected. Here we summarise recent advancements in the understanding of the tumour adenosinergic system and highlight the impact of current and prospective immunomodulatory therapies on other cell types within the TME, focusing on adenosine receptors in tumour cells. In addition, we evaluate the structure- and context-related limitations of targeting this pathway and highlight avenues that could possibly be exploited in future adenosinergic therapies. [ABSTRACT FROM AUTHOR]

Published

2021

49. The Mechanism of CD8 + T Cells for Reducing Myofibroblasts Accumulation during Renal Fibrosis.

Author

Gao, Min, Wang, Jing, Zang, Jianghua, An, Yina, and Dong, Yanjun

Subjects

RENAL fibrosis, T cells, MYOFIBROBLASTS, CHRONIC kidney failure, FIBROBLASTS

Abstract

Renal fibrosis is a hallmark of chronic kidney disease (CKD) and a common manifestation of end-stage renal disease that is associated with multiple types of renal insults and functional loss of the kidney. Unresolved renal inflammation triggers fibrotic processes by promoting the activation and expansion of extracellular matrix-producing fibroblasts and myofibroblasts. Growing evidence now indicates that diverse T cells and macrophage subpopulations play central roles in the inflammatory microenvironment and fibrotic process. The present review aims to elucidate the role of CD8+ T cells in renal fibrosis, and identify its possible mechanisms in the inflammatory microenvironment. [ABSTRACT FROM AUTHOR]

Published

2021

50. The Effects of 15 or 30 s SIT in Normobaric Hypoxia on Aerobic, Anaerobic Performance and Critical Power.

Author

Karabiyik, Hakan, Eser, Mustafa Can, Guler, Ozkan, Yasli, Burak Caglar, Ertetik, Goktug, Sisman, Aysegul, Koz, Mitat, Gabrys, Tomasz, Pilis, Karol, and Karayigit, Raci

Published

2021