Your search keyword '"Montine KS"' showing total 133 results

1. Single-cell peripheral immunoprofiling of lewy body and Parkinson's disease in a multi-site cohort.

Author

Phongpreecha T, Mathi K, Cholerton B, Fox EJ, Sigal N, Espinosa C, Reincke M, Chung P, Hwang LJ, Gajera CR, Berson E, Perna A, Xie F, Shu CH, Hazra D, Channappa D, Dunn JE, Kipp LB, Poston KL, Montine KS, Maecker HT, Aghaeepour N, and Montine TJ

Subjects

Humans, Male, Female, Aged, Case-Control Studies, Biomarkers metabolism, Middle Aged, Cohort Studies, Aged, 80 and over, Lewy Bodies pathology, Lewy Bodies metabolism, Single-Cell Analysis methods, Parkinson Disease immunology, Parkinson Disease metabolism, Lewy Body Disease immunology, Leukocytes, Mononuclear metabolism, Leukocytes, Mononuclear immunology

Abstract

Background: Multiple lines of evidence support peripheral organs in the initiation or progression of Lewy body disease (LBD), a spectrum of neurodegenerative diagnoses that include Parkinson's Disease (PD) without or with dementia (PDD) and dementia with Lewy bodies (DLB). However, the potential contribution of the peripheral immune response to LBD remains unclear. This study aims to characterize peripheral immune responses unique to participants with LBD at single-cell resolution to highlight potential biomarkers and increase mechanistic understanding of LBD pathogenesis in humans., Methods: In a case-control study, peripheral mononuclear cell (PBMC) samples from research participants were randomly sampled from multiple sites across the United States. The diagnosis groups comprise healthy controls (HC, n = 159), LBD (n = 110), Alzheimer's disease dementia (ADD, n = 97), other neurodegenerative disease controls (NDC, n = 19), and immune disease controls (IDC, n = 14). PBMCs were activated with three stimulants (LPS, IL-6, and IFNa) or remained at basal state, stained by 13 surface markers and 7 intracellular signal markers, and analyzed by flow cytometry, which generated 1,184 immune features after gating., Results: The model classified LBD from HC with an AUROC of 0.87 ± 0.06 and AUPRC of 0.80 ± 0.06. Without retraining, the same model was able to distinguish LBD from ADD, NDC, and IDC. Model predictions were driven by pPLCγ2, p38, and pSTAT5 signals from specific cell populations under specific activation. The immune responses characteristic for LBD were not associated with other common medical conditions related to the risk of LBD or dementia, such as sleep disorders, hypertension, or diabetes., Conclusions and Relevance: Quantification of PBMC immune response from multisite research participants yielded a unique pattern for LBD compared to HC, multiple related neurodegenerative diseases, and autoimmune diseases thereby highlighting potential biomarkers and mechanisms of disease., (© 2024. The Author(s).)

Published

2024

2. A pathologist-AI collaboration framework for enhancing diagnostic accuracies and efficiencies.

Author

Huang Z, Yang E, Shen J, Gratzinger D, Eyerer F, Liang B, Nirschl J, Bingham D, Dussaq AM, Kunder C, Rojansky R, Gilbert A, Chang-Graham AL, Howitt BE, Liu Y, Ryan EE, Tenney TB, Zhang X, Folkins A, Fox EJ, Montine KS, Montine TJ, and Zou J

Abstract

In pathology, the deployment of artificial intelligence (AI) in clinical settings is constrained by limitations in data collection and in model transparency and interpretability. Here we describe a digital pathology framework, nuclei.io, that incorporates active learning and human-in-the-loop real-time feedback for the rapid creation of diverse datasets and models. We validate the effectiveness of the framework via two crossover user studies that leveraged collaboration between the AI and the pathologist, including the identification of plasma cells in endometrial biopsies and the detection of colorectal cancer metastasis in lymph nodes. In both studies, nuclei.io yielded considerable diagnostic performance improvements. Collaboration between clinicians and AI will aid digital pathology by enhancing accuracies and efficiencies., (© 2024. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2024

3. Navigating the Landscape of Plasma Biomarkers in Alzheimer's Disease: Focus on Past, Present, and Future Clinical Applications.

Author

Ankeny, Sarrah E., Bacci, Julia R., Decourt, Boris, Sabbagh, Marwan N., and Mielke, Michelle M.

Subjects

ALZHEIMER'S disease, TECHNOLOGICAL innovations, MEDICAL personnel, CEREBROVASCULAR disease, INDIVIDUALIZED medicine

Abstract

As the prevalence of Alzheimer's disease (AD) and its impact on healthcare systems increase, developing tools for accurate diagnosis and monitoring of disease progression is a priority. Recent technological advancements have allowed for the development of blood-based biomarkers (BBMs) to aid in the diagnosis of AD, but many questions remain regarding the clinical implementation of these BBMs. This review outlines the historical timeline of AD BBM development. It highlights key breakthroughs that have transformed the perspective of AD BBMs from theoretically ideal but unattainable markers, to clinically valid and reliable BBMs with potential for implementation in healthcare settings. Technological advancements like single-molecule detection and mass spectrometry methods have significantly improved assay sensitivity and accuracy. High-throughput, fully automated platforms have potential for clinical use. Despite these advancements, however, significant work is needed before AD BBMs can be implemented in widespread clinical practice. Cutpoints must be established, the influence of chronic conditions and medications on BBM levels must be better understood, and guidelines must be created for healthcare providers related to interpreting and communicating information obtained from AD BBMs. Additionally, the development of BBMs for synaptic dysfunction, inflammation, and cerebrovascular disease may provide better precision medicine approaches to treating AD and related dementia. Future research and collaboration between scientists and physicians are essential to addressing these challenges and further advancing AD BBMs, with the goal of integration in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2024

4. Transcriptional landscape of the interaction of human Mesenchymal Stem Cells with Glioblastoma in bioprinted co-cultures.

Author

Oliver, Lisa, Landais, Yuna, Gratas, Catherine, Cartron, Pierre-François, Paris, François, Heymann, Dominique, Vallette, François M., and Serandour, Aurelien

Subjects

LINCRNA, MESENCHYMAL stem cells, HUMAN stem cells, STEM cell treatment, BIOPRINTING, CANCER cell culture

Abstract

Background: The interaction between mesenchymal stem cells (MSC) and Glioblastoma (GBM), although potentially of the highest importance, is ill-understood. This is due, in part, to the lack of relevant experimental models. The similarity between the in vitro situations and the in vivo situation can be improved by 3D co-culture as it reproduces key cell–cell interactions between the tumor microenvironment (TME) and cancer cells. Methods: MSC Can acquired characteristics of cancer associated fibroblasts (CAF) by being cultured with conditioned medium from GBM cultures and thus are called MSCCAF. We co Cultured MSCCAF with patient derived GBM in a scaffold 3D bioprinted model. We studied the response to current GBM therapy (e.g. Temozolomide + /Radiation) on the co cultures by bulk transcriptomic (RNA Seq) and epigenetic (ATAC Seq) analyses Results: The transcriptomic modifications induced by standard GBM treatment in bioprinted scaffolds of mono- or co-cultures of GBM ± MSC can be analyzed. We found that mitochondrial encoded OXPHOS genes are overexpressed under these conditions and are modified by both co-culture and treatment (chemotherapy ± radiation). We have identified two new markers of MSC/GBM interactions, one epigenetically regulated (i.e. TREM-1) associated with an increased overall survival in GBM patients and another implicated in post-transcriptional regulation (i.e. the long non-coding RNA, miR3681HG), which is associated with a reduced overall survival in GBM patients. [ABSTRACT FROM AUTHOR]

Published

2024

5. Perturbations in eIF3 subunit stoichiometry alter expression of ribosomal proteins and key components of the MAPK signaling pathways.

Author

Herrmannová, Anna, Jelínek, Jan, Pospíšilová, Klára, Kerényi, Farkas, Vomastek, Tomáš, Watt, Kathleen, Brábek, Jan, Mohammad, Mahabub Pasha, Wagner, Susan, Topisirovic, Ivan, and Valášek, Leoš Shivaya

Published

2024

6. Robust estimation of cancer and immune cell-type proportions from bulk tumor ATAC-Seq data.

Author

Gabriel, Aurélie Anne-Gaëlle, Racle, Julien, Falquet, Maryline, Jandus, Camilla, and Gfeller, David

Published

2024

7. Systematic perturbations of SETD2, NSD1, NSD2, NSD3, and ASH1L reveal their distinct contributions to H3K36 methylation.

Author

Shipman, Gerry A., Padilla, Reinnier, Horth, Cynthia, Hu, Bo, Bareke, Eric, Vitorino, Francisca N., Gongora, Joanna M., Garcia, Benjamin A., Lu, Chao, and Majewski, Jacek

Published

2024

8. Endogenous glucocorticoids are required for normal macrophage activation and gastric Helicobacter pylori immunity.

Author

Khadka, Stuti, Dziadowicz, Sebastian A., Xu, Xiaojiang, Wang, Lei, Hu, Gangqing, Carrero, Javier A., DiPaolo, Richard J., and Busada, Jonathan T.

Subjects

BACTERIAL colonies, GLUCOCORTICOID receptors, ATROPHIC gastritis, MACROPHAGE activation, GENE expression profiling, HELICOBACTER pylori infections

Abstract

Glucocorticoids are steroid hormones well known for their potent anti-inflammatory effects. However, their immunomodulatory properties are multifaceted. Increasing evidence suggests that glucocorticoid signaling promotes effective immunity and that disruption of glucocorticoid signaling impairs immune function. In this study, we conditionally deleted the glucocorticoid receptor (GR) in the myeloid lineage using the LysM-Cre driver (myGRKO). We examined the impact on macrophage activation and gastric immune responses to Helicobacter pylori, the best-known risk factor of gastric cancer. Our results indicate that, compared with wild type (WT), glucocorticoid receptor knockout (GRKO) macrophages exhibited higher expression of proinflammatory genes in steroid-free conditions. However, when challenged in vivo, GRKO macrophages exhibited aberrant chromatin landscapes and impaired proinflammatory gene expression profiles. Moreover, gastric colonization with H. pylori revealed impaired gastric immune responses and reduced T cell recruitment in myGRKO mice. As a result, myGRKO mice were protected from atrophic gastritis and pyloric metaplasia development. These results demonstrate a dual role for glucocorticoid signaling in preparing macrophages to respond to bacterial infection but limiting their pathogenic activation. In addition, our results support that macrophages are critical for gastric H. pylori immunity. NEW & NOTEWORTHY: Signaling by endogenous glucocorticoids primes macrophages toward more robust responses to pathogens. Disruption of glucocorticoid signaling caused dysregulation of the chromatin landscape, blunted proinflammatory gene activation upon bacterial challenge, and impaired the gastric inflammatory response to Helicobacter pylori infection. [ABSTRACT FROM AUTHOR]

Published

2024

9. Histone variant H2AZ1 drives lung cancer progression through the RELA-HIF1A-EGFR signaling pathway.

Author

Zhao, Huijie, Wu, Xing, Wang, Yinghan, Li, Xiuling, Du, Yuhui, Zhou, Zhiqing, Li, Yu, Liu, Yue, Zeng, Xiaofei, and Chen, Guoan

Subjects

LUNG cancer, CANCER invasiveness, OVERALL survival, CELLULAR signal transduction, WESTERN immunoblotting

Abstract

Background: A growing body of evidence indicates that histone variants play an oncogenic role in cancer progression. However, the role and mechanism of histone variant H2AZ1 in lung cancer remain poorly understood. In this study, we aim to identify novel functions and molecular mechanisms of H2AZ1 in lung cancer. Methods: We analyzed H2AZ1 expression in lung adenocarcinoma using several RNA-seq and microarray datasets. Immunohistochemistry staining for H2AZ1 was performed on two sets of lung cancer tissue microarrays. To study the function of H2AZ1, we conducted assays for cell proliferation, colony formation, invasion, and migration. We employed CUT&Tag-seq, ATAC-seq, RNA-seq, and Western blotting to explore the regulatory patterns and potential mechanisms of H2AZ1 in lung adenocarcinoma. Results: Our findings reveal that H2AZ1 is highly expressed in lung cancer and high levels of H2AZ1 mRNA are associated with poor patient survival. Silencing H2AZ1 impaired cell proliferation, colony formation, migration, and invasion. Mechanistically, our CUT&Tag-seq, ATAC-seq, and RNA-seq results showed that H2AZ1 is primarily deposited around TSS and affects multiple oncogenic signaling pathways. Importantly, we uncovered that H2AZ1 may drive lung cancer progression through the RELA-HIF1A-EGFR signaling pathway. Conclusion: H2AZ1 plays an oncogenic role via several cancer-related pathways, including the RELA-HIF1A-EGFR axis in lung cancer. Intervention targeting H2AZ1 and its related signaling genes may have translational potential for precision therapy. [ABSTRACT FROM AUTHOR]

Published

2024

10. Beyond the usual suspects: multi-factorial computational models in the search for neurodegenerative disease mechanisms.

Author

Khan, Ahmed Faraz and Iturria-Medina, Yasser

Published

2024

11. Spatial regulation of NMN supplementation on brain lipid metabolism upon subacute and sub-chronic PM exposure in C57BL/6 mice.

Author

Jiang, Yue, Li, Fang, Ye, Lizhu, Zhang, Rui, Chen, Shen, Peng, Hui, Zhang, Haiyan, Li, Daochuan, Chen, Liping, Zeng, Xiaowen, Dong, Guanghui, Xu, Wei, Liao, Chunyang, Zhang, Rong, Luo, Qian, and Chen, Wen

Subjects

BRAIN metabolism, LIPID metabolism, METABOLIC regulation, PARTICULATE matter, NERVOUS system

Abstract

Background: Atmospheric particulate matter (PM) exposure-induced neuroinflammation is critical in mediating nervous system impairment. However, effective intervention is yet to be developed. Results: In this study, we examine the effect of β-nicotinamide mononucleotide (NMN) supplementation on nervous system damage upon PM exposure and the mechanism of spatial regulation of lipid metabolism. 120 C57BL/6 male mice were exposed to real ambient PM for 11 days (subacute) or 16 weeks (sub-chronic). NMN supplementation boosted the level of nicotinamide adenine dinucleotide (NAD+) in the mouse brain by 2.04 times. This augmentation effectively reduced neuroinflammation, as evidenced by a marked decrease in activated microglia levels across various brain regions, ranging from 29.29 to 85.96%. Whole brain lipidomics analysis revealed that NMN intervention resulted in an less increased levels of ceramide (Cer) and lysophospholipid in the brain following subacute PM exposure, and reversed triglyceride (TG) and glycerophospholipids (GP) following sub-chronic PM exposure, which conferred mice with anti-neuroinflammation response, improved immune function, and enhanced membrane stability. In addition, we demonstrated that the hippocampus and hypothalamus might be the most sensitive brain regions in response to PM exposure and NMN supplementation. Particularly, the alteration of TG (60:10, 56:2, 60:7), diacylglycerol (DG, 42:6), and lysophosphatidylcholine (LPC, 18:3) are the most profound, which correlated with the changes in functional annotation and perturbation of pathways including oxidative stress, inflammation, and membrane instability unveiled by spatial transcriptomic analysis. Conclusions: This study demonstrates that NMN intervention effectively reduces neuroinflammation in the hippocampus and hypothalamus after PM exposure by modulating spatial lipid metabolism. Strategies targeting the improvement of lipid homeostasis may provide significant protection against brain injury associated with air pollutant exposure. [ABSTRACT FROM AUTHOR]

Published

2024

12. Neuron collinearity differentiates human hippocampal subregions: a validated deep learning approach.

Author

Oltmer, Jan, Williams, Emily M, Groha, Stefan, Rosenblum, Emma W, Roy, Jessica, Llamas-Rodriguez, Josue, Perosa, Valentina, Champion, Samantha N, Frosch, Matthew P, and Augustinack, Jean C

Published

2024

13. Pilot PET study of vaginally administered bioadhesive nanoparticles in cynomolgus monkeys: Kinetics and safety evaluation.

Author

Grun, Molly K., Honhar, Praveen, Wang, Yazhe, Rossano, Samantha, Khang, Minsoo, Suh, Hee Won, Fowles, Krista, Kliman, Harvey J., Cavaliere, Alessandra, Carson, Richard E., Marquez‐Nostra, Bernadette, and Saltzman, W. Mark

Subjects

DELIVERY (Obstetrics), KRA, VAGINA, NANOPARTICLES, TREATMENT effectiveness

Abstract

Long‐lasting vaginal dosage forms could improve the therapeutic efficacy of vaginal microbicides, but achieving long‐term delivery to the vaginal canal has been a significant challenge. To advance understanding of vaginal dosage retention and biodistribution, we describe a method of noninvasive imaging with 89Zr‐labeled bioadhesive nanoparticles (BNPs) in non‐human primates. We additionally examined the safety of repeated BNP application. BNPs administered vaginally to cynomolgus monkeys were still detected after 24 h (1.7% retention) and 120 h (0.1% retention). BNPs did not translocate to the uterus or into systemic circulation. Analysis of inflammatory biomarkers in the vaginal fluid and plasma suggest that BNPs are safe and biocompatible, even after multiple doses. BNPs are a promising delivery vehicle for vaginally administered therapeutics. Further studies using the non‐human primate imaging materials and methods developed here could help advance clinical translation of BNPs and other long‐lasting vaginal dosage forms. [ABSTRACT FROM AUTHOR]

Published

2024

14. Emerging role of galectin 3 in neuroinflammation and neurodegeneration.

Author

Lozinski, Brian M., Khanh Ta, and Yifei Dong

Published

2024

15. Autoimmune hypothesis of Alzheimer's disease: unanswered question.

Author

Arshavsky, Yuri I.

Subjects

EXPLICIT memory, ALZHEIMER'S disease, MEMORY disorders, AUTOIMMUNE diseases, BLOOD-brain barrier, MEMORY trace (Psychology)

Abstract

Alzheimer's disease (AD) was described more than a century ago. However, there are still no effective approaches to its treatment, which may suggest that the search for the cure is not being conducted in the most productive direction. AD begins as selective impairments of declarative memory with no deficits in other cognitive functions. Therefore, understanding of the AD pathogenesis has to include the understanding of this selectivity. Currently, the main efforts aimed at prevention and treatment of AD are based on the dominating hypothesis for the AD pathogenesis: the amyloid hypothesis. But this hypothesis does not explain selective memory impairments since β-amyloid accumulates extracellularly and should be toxic to all types of cerebral neurons, not only to "memory engram neurons." To explain selective memory impairment, I propose the autoimmune hypothesis of AD, based on the analysis of risk factors for AD and molecular mechanisms of memory formation. Memory formation is associated with epigenetic modifications of chromatin in memory engram neurons and, therefore, might be accompanied by the expression of memory-specific proteins recognized by the adaptive immune system as "non-self" antigens. Normally, the brain is protected by the blood-brain barrier (BBB). All risk factors for AD provoke BBB disruptions, possibly leading to an autoimmune reaction against memory engram neurons. This reaction would make them selectively sensitive to tauopathy. If this hypothesis is confirmed, the strategies for AD prevention and treatment would be radically changed. [ABSTRACT FROM AUTHOR]

Published

2024

16. Advanced MRI-based evaluation of gray and white matter changes in Parkinson's disease.

Author

Mohsen, Mohamed, Mohamed, Nehal Aboubakr Elsayed, Bedir, Abdelhalim El-Tantawy Mohamed, Razek, Ahmed Abdel Khalek Abdel, and Saied, Ahmed Effat Abbas Mohamed

Published

2024

17. Intestinal retinol saturase is implicated in the development of obesity and epithelial homeostasis upon injury.

Author

Kiefer, Marie F., Meng, Yueming, Yang, Na, Vahrenbrink, Madita, Wulff, Sascha, Li, Chen, Wowro, Sylvia J., Petricek, Konstantin M., Sommerfeld, Manuela, Flores, Roberto E., Obermayer, Benedikt, Piepelow, Karolin, Klaus, Susanne, Hartl, Kimberly, Guillot, Adrien, Tacke, Frank, Sigal, Michael, and Schupp, Michael

Subjects

HIGH-fat diet, WEIGHT loss, INFLAMMATORY bowel diseases, HOMEOSTASIS, WEIGHT gain, VITAMIN A, INTESTINES, FAT

Abstract

Retinol saturase (RetSat) is an oxidoreductase involved in lipid metabolism and the cellular sensitivity to peroxides. RetSat is highly expressed in metabolic organs like the liver and adipose tissue and its global loss in mice increases body weight and adiposity. The regulation of RetSat expression and its function in the intestine are unexplored. Here, we show that RetSat is present in different segments of the digestive system, localizes to intestinal epithelial cells, and is upregulated by feeding mice high-fat diet (HFD). Intestine-specific RetSat deletion in adult mice did not affect nutrient absorption and energy homeostasis basally, but lowered body weight gain and fat mass of HFD-fed mice, potentially via increasing locomotor activity. Moreover, jejunal expression of genes related to β-oxidation and cholesterol efflux was decreased, and colonic cholesterol content was reduced upon RetSat deletion. In colitis, which we show to downregulate intestinal RetSat expression in humans and mice, RetSat ablation improved epithelial architecture of the murine colon. Thus, intestinal RetSat expression is regulated by dietary interventions and inflammation, and its loss reduces weight gain upon HFD feeding and alleviates epithelial damage upon injury. NEW & NOTEWORTHY: Retinol saturase (RetSat) is an oxidoreductase with unknown function in the intestine. We found that RetSat localizes in intestinal epithelial cells and that its deletion reduced weight gain and fat mass in obese mice. In colitis, which decreased intestinal RetSat expression in humans and mice, RetSat ablation improved the epithelial architecture of the murine colon, presumably by decreasing ROS production, thus rendering RetSat a novel target for metabolic and inflammatory bowel disease. [ABSTRACT FROM AUTHOR]

Published

2024

18. mRNA and circRNA mislocalization to synapses are key features of Alzheimer's disease.

Author

Smukowski, Samuel N., Danyko, Cassidy, Somberg, Jenna, Kaufman, Eli J., Course, Meredith M., Postupna, Nadia, Barker-Haliski, Melissa, Keene, C. Dirk, and Valdmanis, Paul N.

Subjects

CIRCULAR RNA, ALZHEIMER'S disease, IMMOBILIZED proteins, NEUROFIBRILLARY tangles, AMPA receptors, NEUROPLASTICITY, MESSENGER RNA, SYNAPSES

Abstract

Proper transport of RNAs to synapses is essential for localized translation of proteins in response to synaptic signals and synaptic plasticity. Alzheimer's disease (AD) is a neurodegenerative disease characterized by accumulation of amyloid aggregates and hyperphosphorylated tau neurofibrillary tangles followed by widespread synapse loss. To understand whether RNA synaptic localization is impacted in AD, we performed RNA sequencing on synaptosomes and brain homogenates from AD patients and cognitively healthy controls. This resulted in the discovery of hundreds of mislocalized mRNAs in AD among frontal and temporal brain regions. Similar observations were found in an APPswe/PSEN1dE9 mouse model. Furthermore, major differences were observed among circular RNAs (circRNAs) localized to synapses in AD including two overlapping isoforms of circGSK3β, one upregulated, and one downregulated. Expression of these distinct isoforms affected tau phosphorylation in neuronal cells substantiating the importance of circRNAs in the brain and pointing to a new class of therapeutic targets. Author summary: Synaptic plasticity is the foundation for cognition and describes the process by which synaptic connections between neurons are formed, strengthened, or weakened based on signals transmitted by neighboring neurons. Essential to this process is the ability of synapses to respond rapidly to signals and restructure their morphology by translating proteins from a pool of localized mRNAs which is orchestrated by a complex cytoskeletal trafficking system. Given that synapse loss is a cardinal feature of Alzheimer's disease (AD), we RNA sequenced fractionated synaptic particles from brain samples from AD patients and healthy controls to determine whether RNA localization to synapses is impacted in AD. We discovered hundreds of mislocalized mRNAs as well as circular RNAs (circRNAs) which are non-coding isoforms shown to play critical regulatory roles in the brain. Among our data, we discovered two isoforms of circGSK3β, one upregulated, and one downregulated in AD. Expression of these isoforms in neuronal culture was shown to affect tau phosphorylation, dysregulation of which is a hallmark of AD. These findings point to RNA localization and circRNAs as key components to understanding AD pathology and implicate new targets for AD therapies. [ABSTRACT FROM AUTHOR]

Published

2024

19. Expression of FAM159B in Humans, Rats, and Mice: A Cross-species Examination.

Author

Beyer, Anna-Sophia Liselott, Kaemmerer, Daniel, Sänger, Jörg, and Lupp, Amelie

Subjects

LABORATORY rats, ISLANDS of Langerhans, ADAPTOR proteins, BLOOD sugar, SOMATOSTATIN

Abstract

Little is known about the adaptor protein FAM159B. To determine whether FAM159B expression findings in rats or mice can be extrapolated to humans, we compared FAM159B expression in healthy tissue samples from all three species using immunohistochemistry. Despite variations in expression intensity, similar FAM159B expression patterns were observed in most organs across species. The most prominent species difference was noted in pancreatic islets; while FAM159B expression was limited to single cells on the outer edges in mice and rats, it was detectable across entire islets in humans. Double-labeling immunohistochemistry revealed partial overlap of FAM159B expression with that of insulin, glucagon, and somatostatin in human islets. By contrast, FAM159B showed complete colocalization with only somatostatin in rats and mice. An additional analysis of FAM159B expression in lean and obese Zucker rats revealed larger islet areas due to increased β-cell mass in obese rats, which was accompanied by a smaller percentage of FAM159B-positive δ-cells per islet area. Beyond the known differences in islet architecture across species, our results point to larger dissimilarities in blood glucose regulation between rodents and humans than generally assumed. Moreover, findings regarding FAM159B expression (and function) cannot be directly transferred between rodents and humans. [ABSTRACT FROM AUTHOR]

Published

2024

20. Eye Adult Changes in Thought (Eye ACT) Study: Design and Report on the Inaugural Cohort.

Author

Lee, Cecilia S., Ferguson, Alina N., Gibbons, Laura E., Walker, Rod, Su, Yu-Ru, Krakauer, Chloe, Brush, Michael, Kam, Jason, Larson, Eric B., Arterburn, David E., Crane, Paul K., Takahashi, Missy, Zhang, Yi, Jiang, Yu, Wu, Yue, Cooper, Julie, Pope, Beth, Blazes, Marian, Lee, Aaron Y., and Lee, Michael L.

Subjects

VISION, CONTRAST sensitivity (Vision), ALZHEIMER'S disease, VISUAL acuity, ADULTS

Abstract

Background: Conflicting research on retinal biomarkers of Alzheimer's disease and related dementias (AD/ADRD) is likely related to limited sample sizes, study design, and protocol differences. Objective: The prospective Eye Adult Changes in Thought (Eye ACT) seeks to address these gaps. Methods: Eye ACT participants are recruited from ACT, an ongoing cohort of dementia-free, older adults followed biennially until AD/ADRD, and undergo visual function and retinal imaging assessment either in clinic or at home. Results: 330 participants were recruited as of 03/2023. Compared to ACT participants not in Eye ACT (N = 1868), Eye ACT participants (N = 330) are younger (mean age: 70.3 versus 71.2, p = 0.014), newer to ACT (median ACT visits since baseline: 3 versus 4, p < 0.001), have more years of education (17.7 versus 16.2, p < 0.001) and had lower rates of visual impairment (12% versus 22%, p < 0.001). Compared to those seen in clinic (N = 300), Eye ACT participants seen at home (N = 30) are older (77.2 versus 74.9, p = 0.015), more frequently female (60% versus 49%, p = 0.026), and have significantly worse visual acuity (71.1 versus 78.9 Early Treatment Diabetic Retinopathy Study letters, p < 0.001) and contrast sensitivity (–1.9 versus –2.1 mean log units at 3 cycles per degree, p = 0.002). Cognitive scores and retinal imaging measurements are similar between the two groups. Conclusions: Participants assessed at home had significantly worse visual function than those seen in clinic. By including these participants, Eye ACT provides a unique longitudinal cohort for evaluating potential retinal biomarkers of dementia. [ABSTRACT FROM AUTHOR]

Published

2024

21. Acceptability of virtual reality to screen for dementia in older adults.

Author

Siette, Joyce, Adam, Patrick J., and Harris, Celia B.

Subjects

OLDER people, VIRTUAL reality, DEMENTIA, DIGITAL health, MEDICAL personnel, MEDICAL screening

Abstract

Background: Early detection of dementia and cognitive decline is crucial for effective interventions and overall wellbeing. Although virtual reality (VR) tools offer potential advantages to traditional dementia screening tools, there is a lack of knowledge regarding older adults' acceptance of VR tools, as well as the predictors and features influencing their adoption. This study aims to (i) explore older adults' perceptions of the acceptability and usefulness of VR diagnostic tools for dementia, and (ii) identify demographic predictors of adoption and features of VR applications that contribute to future adoption among older adults. Methods: A cross-sectional study was conducted involving community-dwelling older adults who completed online questionnaires covering demographics, medical history, technology acceptance, previous usage, and perceived usefulness and barriers to VR adoption. Multiple linear regression was employed to assess relationships between sociodemographic factors, prior technology use, perceived ease, usefulness, and intention to adopt VR-based diagnostic tools. Results: Older adults (N = 77, Mage = 73.74, SD = 6.4) were predominantly female and born in English-speaking countries. Perceived usefulness of VR applications and educational attainment emerged as significant predictors of the likelihood to use VR applications for dementia screening. Generally, older adults showed acceptance of VR applications for healthcare and dementia screening. Fully immersive applications were preferred, and older adults were mostly willing to share electronic information from screening with their healthcare providers. Conclusions: The field of research on VR applications in healthcare is expanding. Understanding the demographic characteristics of populations that stand to benefit from healthcare innovations is critical for promoting adoption of digital health technologies and mitigating its barriers to access. [ABSTRACT FROM AUTHOR]

Published

2024

22. Alzheimer DataLENS: An Open Data Analytics Portal for Alzheimer's Disease Research.

Author

Noori, Ayush, Jayakumar, Rojashree, Moturi, Vaishnavi, Li, Zhaozhi, Liu, Rongxin, Serrano-Pozo, Alberto, Hyman, Bradley T., and Das, Sudeshna

Subjects

ALZHEIMER'S disease, GENOME-wide association studies, RNA sequencing, TRANSCRIPTOMES, PROTEIN-protein interactions

Abstract

Background: Recent Alzheimer's disease (AD) discoveries are increasingly based on studies from a variety of omics technologies on large cohorts. Currently, there is no easily accessible resource for neuroscientists to browse, query, and visualize these complex datasets in a harmonized manner. Objective: Create an online portal of public omics datasets for AD research. Methods: We developed Alzheimer DataLENS, a web-based portal, using the R Shiny platform to query and visualize publicly available transcriptomics and genetics studies of AD on human cohorts. To ensure consistent representation of AD findings, all datasets were processed through a uniform bioinformatics pipeline. Results: Alzheimer DataLENS currently houses 2 single-nucleus RNA sequencing datasets, over 30 bulk RNA sequencing datasets from 19 brain regions and 3 cohorts, and 2 genome-wide association studies (GWAS). Available visualizations for single-nucleus data include bubble plots, heatmaps, and UMAP plots; for bulk expression data include box plots and heatmaps; for pathways include protein-protein interaction network plots; and for GWAS results include Manhattan plots. Alzheimer DataLENS also links to two other knowledge resources: the AD Progression Atlas and the Astrocyte Atlas. Conclusions: Alzheimer DataLENS is a valuable resource for investigators to quickly and systematically explore omics datasets and is freely accessible at . [ABSTRACT FROM AUTHOR]

Published

2024

23. Cardiac GR Mediates the Diurnal Rhythm in Ventricular Arrhythmia Susceptibility.

Author

Tikhomirov, Roman, Oakley, Robert H., Anderson, Cali, Yirong Xiang, Al-Othman, Sami, Smith, Matthew, Yaar, Sana, Torre, Eleonora, Jianying Li, Wilson, Leslie R., Goulding, David R., Donaldson, Ian, Harno, Erika, Soattin, Luca, Shiels, Holly A., Morris, Gwilym M., Henggui Zhang, Boyett, Mark R., Cidlowski, John A., and Mesirca, Pietro

Published

2024

24. Immunoproteasomal Processing of IsoLG-Adducted Proteins Is Essential for Hypertension.

Author

de la Visitación, Néstor, Wei Chen, Krishnan, Jaya, Van Beusecum, Justin P., Amarnath, Venkataraman, Hennen, Elizabeth M., Shilin Zhao, Saleem, Mohammad, Mingfang Ao, Dikalov, Sergey I., Dikalova, Anna E., Harrison, David G., and Patrick, David M.

Published

2024

25. Genome-wide distribution of 5-hydroxymethyluracil and chromatin accessibility in the Breviolum minutum genome.

Author

Marinov, Georgi K., Chen, Xinyi, Swaffer, Matthew P., Xiang, Tingting, Grossman, Arthur R., and Greenleaf, William J.

Published

2024

26. Epigenetic Regulation of Cardiomyocyte Maturation by Arginine Methyltransferase CARM1.

Author

Garbutt, Tiffany A., Wang, Zhenhua, Wang, Haofei, Ma, Hong, Ruan, Hongmei, Dong, Yanhan, Xie, Yifang, Tan, Lianmei, Phookan, Ranan, Stouffer, Joy A., Vedantham, Vasanth, Yang, Yuchen, Qian, Li, and Liu, Jiandong

Published

2024

27. Hyperphosphorylated Tau Inflicts Intracellular Stress Responses that Are Mitigated by Apomorphine.

Author

Song, Zhenfeng, Wang, Kuang-Wei, Hagar, Hsiao-Tien Chien, Chen, Hong-Ru, Kuan, Chia-Yi, Zhang, Kezhong, and Kuo, Min-Hao

Abstract

Abnormal phosphorylation of the microtubule-binding protein tau in the brain is a key pathological marker for Alzheimer's disease and additional neurodegenerative tauopathies. However, how hyperphosphorylated tau causes cellular dysfunction or death that underlies neurodegeneration remains an unsolved question critical for the understanding of disease mechanism and the design of efficacious drugs. Using a recombinant hyperphosphorylated tau protein (p-tau) synthesized by the PIMAX approach, we examined how cells responded to the cytotoxic tau and explored means to enhance cellular resistance to tau attack. Upon p-tau uptake, the intracellular calcium levels rose promptly. Gene expression analyses revealed that p-tau potently triggered endoplasmic reticulum (ER) stress, unfolded protein response (UPR), ER stress-associated apoptosis, and pro-inflammation in cells. Proteomics studies showed that p-tau diminished heme oxygenase-1 (HO-1), an ER stress-associated anti-inflammation and anti-oxidative stress regulator, while stimulated the accumulation of MIOS and other proteins. p-Tau-induced ER stress-associated apoptosis and pro-inflammation are ameliorated by apomorphine, a brain-permeable prescription drug widely used to treat Parkinson's disease symptoms, and by overexpression of HO-1. Our results reveal probable cellular functions targeted by hyperphosphorylated tau. Some of these dysfunctions and stress responses have been linked to neurodegeneration in Alzheimer's disease. The observations that the ill effects of p-tau can be mitigated by a small compound and by overexpressing HO-1 that is otherwise diminished in the treated cells inform new directions of Alzheimer's disease drug discovery. [ABSTRACT FROM AUTHOR]

Published

2024

28. A PCR-independent approach for mtDNA enrichment and next-generation sequencing: comprehensive evaluation and clinical application.

Author

Liang, Dong, Zhu, Lin, Zhu, Yuqing, Huang, Mingtao, Lin, Ying, Li, Hang, Hu, Ping, Zhang, Jun, Shen, Bin, and Xu, Zhengfeng

Subjects

MITOCHONDRIAL DNA, NUCLEOTIDE sequencing, CLINICAL medicine, LEBER'S hereditary optic atrophy

Abstract

Background: Sequencing the mitochondrial genome has been increasingly important for the investigation of primary mitochondrial diseases (PMD) and mitochondrial genetics. To overcome the limitations originating from PCR-based mtDNA enrichment, we set out to develop and evaluate a PCR-independent approach in this study, named Pime-Seq (PCR-independent mtDNA enrichment and next generation Sequencing). Results: By using the optimized mtDNA enrichment procedure, the mtDNA reads ratio reached 88.0 ± 7.9% in the sequencing library when applied on human PBMC samples. We found the variants called by Pime-Seq were highly consistent among technical repeats. To evaluate the accuracy and reliability of this method, we compared Pime-Seq with lrPCR based NGS by performing both methods simultaneously on 45 samples, yielding 1677 concordant variants, as well as 146 discordant variants with low-level heteroplasmic fraction, in which Pime-Seq showed higher reliability. Furthermore, we applied Pime-Seq on 4 samples of PMD patients retrospectively, and successfully detected all the pathogenic mtDNA variants. In addition, we performed a prospective study on 192 apparently healthy pregnant women during prenatal screening, in which Pime-Seq identified pathogenic mtDNA variants in 4 samples, providing extra information for better health monitoring in these cases. Conclusions: Pime-Seq can obtain highly enriched mtDNA in a PCR-independent manner for high quality and reliable mtDNA deep-sequencing, which provides us an effective and promising tool for detecting mtDNA variants for both clinical and research purposes. [ABSTRACT FROM AUTHOR]

Published

2024

29. Gene-expression profiling of individuals resilient to Alzheimer's disease reveals higher expression of genes related to metallothionein and mitochondrial processes and no changes in the unfolded protein response.

Author

de Vries, Luuk E., Jongejan, Aldo, Monteiro Fortes, Jennifer, Balesar, Rawien, Rozemuller, Annemieke J. M., Moerland, Perry D., Huitinga, Inge, Swaab, Dick F., and Verhaagen, Joost

Subjects

UNFOLDED protein response, ALZHEIMER'S disease, GENE expression, HEAT shock proteins, GENE regulatory networks, VOXEL-based morphometry

Abstract

Some individuals show a discrepancy between cognition and the amount of neuropathological changes characteristic for Alzheimer's disease (AD). This phenomenon has been referred to as 'resilience'. The molecular and cellular underpinnings of resilience remain poorly understood. To obtain an unbiased understanding of the molecular changes underlying resilience, we investigated global changes in gene expression in the superior frontal gyrus of a cohort of cognitively and pathologically well-defined AD patients, resilient individuals and age-matched controls (n = 11–12 per group). 897 genes were significantly altered between AD and control, 1121 between resilient and control and 6 between resilient and AD. Gene set enrichment analysis (GSEA) revealed that the expression of metallothionein (MT) and of genes related to mitochondrial processes was higher in the resilient donors. Weighted gene co-expression network analysis (WGCNA) identified gene modules related to the unfolded protein response, mitochondrial processes and synaptic signaling to be differentially associated with resilience or dementia. As changes in MT, mitochondria, heat shock proteins and the unfolded protein response (UPR) were the most pronounced changes in the GSEA and/or WGCNA, immunohistochemistry was used to further validate these processes. MT was significantly increased in astrocytes in resilient individuals. A higher proportion of the mitochondrial gene MT-CO1 was detected outside the cell body versus inside the cell body in the resilient compared to the control group and there were higher levels of heat shock protein 70 (HSP70) and X-box-binding protein 1 spliced (XBP1s), two proteins related to heat shock proteins and the UPR, in the AD donors. Finally, we show evidence for putative sex-specific alterations in resilience, including gene expression differences related to autophagy in females compared to males. Taken together, these results show possible mechanisms involving MTs, mitochondrial processes and the UPR by which individuals might maintain cognition despite the presence of AD pathology. [ABSTRACT FROM AUTHOR]

Published

2024

30. Convergent epigenetic evolution drives relapse in acute myeloid leukemia.

Author

Nuno, Kevin, Azizi, Armon, Koehnke, Thomas, Lareau, Caleb, Ediriwickrema, Asiri, Corces, M. Ryan, Satpathy, Ansuman T., and Majeti, Ravindra

Published

2024

31. Reciprocal negative feedback between Prrx1 and miR-140-3p regulates rapid chondrogenesis in the regenerating antler.

Author

Hu, Pengfei, Zhang, Guokun, Ba, Hengxing, Ren, Jing, Li, Jiping, Wang, Zhen, and Li, Chunyi

Abstract

During growth phase, antlers exhibit a very rapid rate of chondrogenesis. The antler is formed from its growth center reserve mesenchyme (RM) cells, which have been found to be the derivatives of paired related homeobox 1 (Prrx1)-positive periosteal cells. However, the underlying mechanism that drives rapid chondrogenesis is not known. Herein, the miRNA expression profiles and chromatin states of three tissue layers (RM, precartilage, and cartilage) at different stages of differentiation within the antler growth center were analyzed by RNA-sequencing and ATAC-sequencing. We found that miR-140-3p was the miRNA that exhibited the greatest degree of upregulation in the rapidly growing antler, increasing from the RM to the cartilage layer. We also showed that Prrx1 was a key upstream regulator of miR-140-3p, which firmly confirmed by Prrx1 CUT&Tag sequencing of RM cells. Through multiple approaches (three-dimensional chondrogenic culture and xenogeneic antler model), we demonstrated that Prrx1 and miR-140-3p functioned as reciprocal negative feedback in the antler growth center, and downregulating PRRX1/upregulating miR-140-3p promoted rapid chondrogenesis of RM cells and xenogeneic antler. Thus, we conclude that the reciprocal negative feedback between Prrx1 and miR-140-3p is essential for balancing mesenchymal proliferation and chondrogenic differentiation in the regenerating antler. We further propose that the mechanism underlying chondrogenesis in the regenerating antler would provide a reference for helping understand the regulation of human cartilage regeneration and repair. [ABSTRACT FROM AUTHOR]

Published

2024

32. Overview of the expression patterns and roles of Lipocalin 2 in the reproductive system.

Author

Krizanac, Marinela, Mass Sanchez, Paola Berenice, Weiskirchen, Ralf, and Schröder, Sarah K.

Subjects

GENITALIA, MALE reproductive organs, MALE infertility, FEMALE reproductive organs, EPITHELIAL cells, BACTERIAL growth

Abstract

The 25 kDa-sized protein Lipocalin 2 (LCN2) was originally isolated from human neutrophil granulocytes more than 30 years ago. LCN2 is an emerging player in innate immune defense, as it reduces bacterial growth due to its ability to sequester iron-containing bacterial siderophores. On the other hand, LCN2 also serves as a transporter for various hydrophobic substances due to its β-barrel shaped structure. Over the years, LCN2 has been detected in many other cell types including epithelial cells, astrocytes, and hepatocytes. Studies have clearly shown that aberrant expression of LCN2 is associated with a variety of disorders and malignancies, including several diseases of the reproductive system. Furthermore, LCN2 was proposed as a non-invasive prognostic and/or diagnostic biomarker in this context. Although several studies have shed light on the role of LCN2 in various disorders of the female and male reproductive systems, including tumorigenesis, a comprehensive understanding of the physiological function of LCN2 in the reproductive tract is still lacking. However, there is evidence that LCN2 is directly related to fertility, as global depletion of Lcn2 in mice has a negative effect on their pregnancy rate. Since LCN2 expression can be regulated by steroid hormones, it is not surprising that its expression fluctuates greatly during remodeling processes in the female reproductive tract, especially in the uterus. Well-founded details about the expression and regulation of LCN2 in a healthy reproductive state and also about possible changes during reproductive aging could contribute to a better understanding of LCN2 as a target in various diseases. Therefore, the present review summarizes current knowledge about LCN2 in the reproductive system, including studies in rodents and humans, and discusses changes in LCN2 expression during pathological events. The limited data suggest that LCN2 is expressed and regulated differently in healthy male and female reproductive organs. [ABSTRACT FROM AUTHOR]

Published

2024

33. Contactin 5 and Apolipoproteins Interplay in Alzheimer's Disease.

Author

Dauar, Marina Tedeschi, Picard, Cynthia, Labonté, Anne, Breitner, John, Rosa-Neto, Pedro, Villeneuve, Sylvia, and Poirier, Judes

Subjects

ALZHEIMER'S disease, APOLIPOPROTEINS, LIQUID chromatography-mass spectrometry, MEMBRANE proteins, ENTORHINAL cortex, IMMOBILIZATION stress

Abstract

Background: Apolipoproteins and contactin 5 are proteins associated with Alzheimer's disease (AD) pathophysiology. Apolipoproteins act on transport and clearance of cholesterol and phospholipids during synaptic turnover and terminal proliferation. Contactin 5 is a neuronal membrane protein involved in key processes of neurodevelopment. Objective: To investigate the interactions between contactin 5 and apolipoproteins in AD, and the role of these proteins in response to neuronal damage. Methods: Apolipoproteins (measured by Luminex), contactin 5 (measured by Olink's proximity extension assay), and cholesterol (measured by liquid chromatography mass spectrometry) were assessed in the cerebrospinal fluid (CSF) and plasma of cognitively unimpaired participants (n = 93). Gene expression was measured using polymerase chain reaction in the frontal cortex of autopsied-confirmed AD (n = 57) and control subjects (n = 31) and in the hippocampi of mice following entorhinal cortex lesions. Results: Contactin 5 positively correlated with apolipoproteins B (p = 5.4×10–8), D (p = 1.86×10–4), E (p = 2.92×10–9), J (p = 2.65×10–9), and with cholesterol (p = 0.0096) in the CSF, and with cholesterol (p = 0.02), HDL (p = 0.0143), and LDL (p = 0.0121) in the plasma. Negative correlations were seen between CNTN5, APOB (p = 0.034) and APOE (p = 0.015) mRNA levels in the brains of control subjects. In the mouse model, apoe and apoj gene expression increased during the reinnervation phase (p < 0.05), while apob (p = 0.023) and apod (p = 0.006) increased in the deafferentation stage. Conclusions: Extensive interactions were observed between contactin 5 and apolipoproteins and cholesterol, possibly due to neuronal damage. The alterations in gene expression of apolipoproteins suggest a role in axonal, terminal, and synaptic remodeling in response to entorhinal cortex damage. [ABSTRACT FROM AUTHOR]

Published

2024

34. Thrombocytopenia Independently Leads to Changes in Monocyte Immune Function.

Author

Li, Chen, Ture, Sara K., Nieves-Lopez, Benjamin, Blick-Nitko, Sara K., Maurya, Preeti, Livada, Alison C., Stahl, Tyler J., Kim, Minsoo, Pietropaoli, Anthony P., and Morrell, Craig N.

Published

2024

35. Redistribution of PU.1 partner transcription factor RUNX1 binding secures cell survival during leukemogenesis.

Author

Bender A, Boydere F, Jayavelu AK, Tibello A, König T, Aleth H, Meyer Zu Hörste G, Vogl T, and Rosenbauer F

Abstract

Transcription factors (TFs) orchestrating lineage-development often control genes required for cellular survival. However, it is not well understood how cells survive when such TFs are lost, for example in cancer. PU.1 is an essential TF for myeloid fate, and mice with downregulated PU.1 levels develop acute myeloid leukemia (AML). Combining a multi-omics approach with a functional genetic screen, we reveal that PU.1-downregulated cells fundamentally change their survival control from cytokine-driven pathways to overexpression of an autophagy-predominated stem cell gene program, for which we also find evidence in human AML. Control of this program involves redirected chromatin occupancy of the PU.1 partner TF Runx1 to a lineage-inappropriate binding site repertoire. Hence, genomic reallocation of TF binding upon loss of a partner TF can act as a pro-oncogenic failsafe mechanism by sustaining cell survival during leukemogenesis., Competing Interests: Disclosure and competing interests statement The authors declare no competing interests., (© 2024. The Author(s).)

Published

2024

36. Oxidative stress-mediated neuroinflammation in Alzheimer's disease.

Author

Firdous SM, Khan SA, and Maity A

Subjects

Humans, Animals, Reactive Oxygen Species metabolism, Inflammation metabolism, Alzheimer Disease metabolism, Oxidative Stress, Neuroinflammatory Diseases metabolism

Abstract

Reactive oxygen species (ROS) are metabolic by-products that constitute an indispensable component of physiological processes, albeit their heightened presence may proffer substantial perils to biological entities. Such a proliferation gives rise to a gradual escalation of oxidative stress within the organism, thereby compromising mitochondrial functionality and inflicting harm upon various bodily systems, with a particular predilection for the central nervous system. In its nascent stages, it is plausible that inflammation has been a facilitator in the progression of the malady. The precise role of inflammation in Alzheimer's disease (AD) remains somewhat enigmatic, although it is conceivable that activated microglia and astrocytes might be implicated in the removal of amyloid-β (Aβ) deposits. Nonetheless, prolonged microglial activation is associated with Tau phosphorylation and Aβ aggregation. Research studies have indicated that AD brains upregulate complementary molecules, inflammatory cytokines, acute phase reacting agents, and other inflammatory mediators that may cause neurodegeneration. In this review, oxidative damage products will be discussed as potential peripheral biomarkers for AD and its early stages. The disordered excretion of pro-inflammatory cytokines, chemokines, oxygen, and nitrogen-reactive species, along with the stimulation of the complement system by glial cells, has the potential to disrupt the functionality of neuronal termini. This perturbation, in turn, culminates in compromised synaptic function, a phenomenon empirically linked to the manifestation of cognitive impairments. The management of neurodegenerative conditions in the context of dementia necessitates therapeutic interventions that specifically target the excessive production of inflammatory and oxidative agents. Furthermore, we shall deliberate upon the function of microglia and oxidative injury in the etiology of AD and the ensuing neurodegenerative processes., (© 2024. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published

2024

37. Distinctive whole-brain cell types predict tissue damage patterns in thirteen neurodegenerative conditions.

Author

Pak, Veronika, Adewale, Quadri, Bzdok, Danilo, Dadar, Mahsa, Zeighami, Yashar, and Iturria-Medina, Yasser

Published

2024

38. APOE4 genotype and aging impair injury-induced microglial behavior in brain slices, including toward Aβ, through P2RY12.

Author

Sepulveda, Jordy, Kim, Jennifer Yejean, Binder, Joseph, Vicini, Stefano, and Rebeck, G. William

Abstract

Microglia are highly dynamic cells that play a critical role in tissue homeostasis through the surveillance of brain parenchyma and response to cues associated with damage. Aging and APOE4 genotype are the strongest risk factors for Alzheimer’s disease (AD), but how they affect microglial dynamics remains unclear. Using ex vivo confocal microscopy, we analyzed microglial dynamic behaviors in the entorhinal cortex (EC) and hippocampus CA1 of 6-, 12-, and 21-month-old mice APOE3 or APOE4 knock-in mice expressing GFP under the CX3CR1 promoter. To study microglia surveillance, we imaged microglia baseline motility for 20 min and measured the extension and retraction of processes. We found that APOE4 microglia exhibited significantly less brain surveillance (27%) compared to APOE3 microglia in 6-month-old mice; aging exacerbated this deficit. To measure microglia response to damage, we imaged process motility in response to ATP, an injury-associated signal, for 30 min. We found APOE4 microglia extended their processes significantly slower (0.9 µm/min, p < 0.005) than APOE3 microglia (1.1 μm/min) in 6-month-old animals. APOE-associated alterations in microglia motility were observed in 12- and 21-month-old animals, and this effect was exacerbated with aging in APOE4 microglia. We measured protein and mRNA levels of P2RY12, a core microglial receptor required for process movement in response to damage. We found that APOE4 microglia express significantly less P2RY12 receptors compared to APOE3 microglia despite no changes in P2RY12 transcripts. To examine if the effect of APOE4 on the microglial response to ATP also applied to amyloid β (Aβ), we infused locally Hi-Lyte Fluor 555-labeled Aβ in acute brain slices of 6-month-old mice and imaged microglia movement for 2 h. APOE4 microglia showed a significantly slower (p < 0.0001) process movement toward the Aβ, and less Aβ coverage at early time points after Aβ injection. To test whether P2RY12 is involved in process movement in response to Aβ, we treated acute brain slices with a P2RY12 antagonist before Aβ injection; microglial processes no longer migrated towards Aβ. These results provide mechanistic insights into the impact of APOE4 genotype and aging in dynamic microglial behaviors prior to gross Aβ pathology and could help explain how APOE4 brains are more susceptible to AD pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

39. Regulation of YAP Promotor Accessibility in Endothelial Mechanotransduction.

Author

Mannion, Aarren J., Zhao, Honglei, Zhang, Yuanyuan, von Wright, Ylva, Bergman, Otto, Roy, Joy, Saharinen, Pipsa, and Holmgren, Lars

Published

2024

40. Inferring Alzheimer's Disease Pathologic Traits from Clinical Measures in Living Adults.

Author

Yang, Jingjing, Liu, Xizhu, Oveisgharan, Shahram, Zammit, Andrea R., Nag, Sukriti, Bennett, David A., and Buchman, Aron S.

Subjects

ALZHEIMER'S disease, RECEIVER operating characteristic curves, DISEASE risk factors, ADULTS

Abstract

Background: Alzheimer's disease neuropathologic changes (AD-NC) are important to identify people with high risk for AD dementia (ADD) and subtyping ADD. Objective: Develop imputation models based on clinical measures to infer AD-NC. Methods: We used penalized generalized linear regression to train imputation models for four AD-NC traits (amyloid-β, tangles, global AD pathology, and pathologic AD) in Rush Memory and Aging Project decedents, using clinical measures at the last visit prior to death as predictors. We validated these models by inferring AD-NC traits with clinical measures at the last visit prior to death for independent Religious Orders Study (ROS) decedents. We inferred baseline AD-NC traits for all ROS participants at study entry, and then tested if inferred AD-NC traits at study entry predicted incident ADD and postmortem pathologic AD. Results: Inferred AD-NC traits at the last visit prior to death were related to postmortem measures with R2 = (0.188,0.316,0.262) respectively for amyloid-β, tangles, and global AD pathology, and prediction Area Under the receiver operating characteristic Curve (AUC) 0.765 for pathologic AD. Inferred baseline levels of all four AD-NC traits predicted ADD. The strongest prediction was obtained by the inferred baseline probabilities of pathologic AD with AUC = (0.919,0.896) for predicting the development of ADD in 3 and 5 years from baseline. The inferred baseline levels of all four AD-NC traits significantly discriminated pathologic AD profiled eight years later with p-values < 1.4×10-10. Conclusions: Inferred AD-NC traits based on clinical measures may provide effective AD biomarkers that can estimate the burden of AD-NC traits in aging adults. [ABSTRACT FROM AUTHOR]

Published

2024

41. Micro-RNA profiles of pathology and resilience in posterior cingulate cortex of cognitively intact elders.

Author

Kelley, Christy M, Maloney, Bryan, Beck, John S, Ginsberg, Stephen D, Liang, Winnie, Lahiri, Debomoy K, Mufson, Elliott J, and Counts, Scott E

Published

2024

42. The translatome of glioblastoma.

Author

Cornelissen FMG, He Z, Ciputra E, de Haas RR, Beumer-Chuwonpad A, Noske D, Vandertop WP, Piersma SR, Jiménez CR, Murre C, and Westerman BA

Abstract

Glioblastoma (GB), the most common and aggressive brain tumor, demonstrates intrinsic resistance to current therapies, resulting in poor clinical outcomes. Cancer progression can be partially attributed to the deregulation of protein translation mechanisms that drive cancer cell growth. In this study, we present the translatome landscape of GB as a valuable data resource. Eight patient-derived GB sphere cultures (GSCs) were analyzed using ribosome profiling and messenger RNA (mRNA) sequencing. We investigated inter-cell-line differences through differential expression analysis at both the translatome and transcriptome levels. Translational changes post-radiotherapy were assessed at 30 and 60 min. The translation of non-coding RNAs (ncRNAs) was validated using in-house and public mass spectrometry (MS) data, whereas RNA expression was confirmed by quantitative PCR (qPCR). Our findings demonstrate that ribosome sequencing provides more detailed information than MS or transcriptional analyses. Transcriptional similarities among GSCs correlate with translational similarities, aligning with previously defined subtypes such as proneural and mesenchymal. Additionally, we identified a broad spectrum of open reading frame types in both coding and non-coding mRNA regions, including long non-coding RNAs (lncRNAs) and pseudogenes undergoing active translation. Translation of ncRNAs into peptides was independently confirmed by in-house data and external MS data. We also observed that translational regulation of histones (downregulated) and splicing factors (upregulated) occurs in response to radiotherapy. These data offer new insights into genome-wide protein synthesis, identifying translationally regulated genes and alternative translation initiation sites in GB under normal and radiotherapeutic conditions, providing a rich resource for GB research. Further functional validation of differentially expressed genes after radiotherapy is needed. Understanding translational control in GB can reveal mechanistic insights and identify currently unknown biomarkers, ultimately enhancing the diagnosis and treatment of this aggressive brain cancer., (© 2024 The Author(s). Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.)

Published

2024

43. Cell-type-specific cis-regulatory divergence in gene expression and chromatin accessibility revealed by human-chimpanzee hybrid cells.

Author

Ban Wang, Starr, Alexander L., and Fraser, Hunter B.

Published

2024

44. The dynamic landscape of chromatin accessibility and active regulatory elements in the mediobasal hypothalamus influences the seasonal activation of the reproductive axis in the male quail under long light exposure.

Author

Chang, Jianye, Xu, Yanglong, Fu, Yuting, Liu, Jiaxin, Jiang, Danli, Pan, Jianqiu, Ouyang, Hongjia, Liu, Wenjun, Xu, Jin, Tian, Yunbo, Huang, Yunmao, Ruan, Jue, and Shen, Xu

Abstract

Background: In cold and temperate zones, seasonal reproduction plays a crucial role in the survival and reproductive success of species. The photoperiod influences reproductive processes in seasonal breeders through the hypothalamic-pituitary-gonadal (HPG) axis, in which the mediobasal hypothalamus (MBH) serves as the central region responsible for transmitting light information to the endocrine system. However, the cis-regulatory elements and the transcriptional activation mechanisms related to seasonal activation of the reproductive axis in MBH remain largely unclear. In this study, an artificial photoperiod program was used to induce the HPG axis activation in male quails, and we compared changes in chromatin accessibility changes during the seasonal activation of the HPG axis. Results: Alterations in chromatin accessibility occurred in the mediobasal hypothalamus (MBH) and stabilized at LD7 during the activation of the HPG axis. Most open chromatin regions (OCRs) are enriched mainly in introns and distal intergenic regions. The differentially accessible regions (DARs) showed enrichment of binding motifs of the RFX, NKX, and MEF family of transcription factors that gained-loss accessibility under long-day conditions, while the binding motifs of the nuclear receptor (NR) superfamily and BZIP family gained-open accessibility. Retinoic acid signaling and GTPase-mediated signal transduction are involved in adaptation to long days and maintenance of the HPG axis activation. According to our footprint analysis, three clock-output genes (TEF, DBP, and HLF) and the THRA were the first responders to long days in LD3. THRB, NR3C2, AR, and NR3C1 are the key players associated with the initiation and maintenance of the activation of the HPG axis, which appeared at LD7 and tended to be stable under long-day conditions. By integrating chromatin and the transcriptome, three genes (DIO2, SLC16A2, and PDE6H) involved in thyroid hormone signaling showed differential chromatin accessibility and expression levels during the seasonal activation of the HPG axis. TRPA1, a target of THRB identified by DAP-seq, was sensitive to photoactivation and exhibited differential expression levels between short- and long-day conditions. Conclusion: Our data suggest that trans effects were the main factors affecting gene expression during the seasonal activation of the HPG axis. This study could lead to further research on the seasonal reproductive behavior of birds, particularly the role of MBH in controlling seasonal reproductive behavior. [ABSTRACT FROM AUTHOR]

Published

2024

45. Administration of Aripiprazole Alleviates Memory Impairment and Restores Damaged Glutamatergic System in 5xFAD Mice.

Author

Lee HJ, Kim HY, Oh SJ, Son Y, Kang KJ, Nam KR, and Choi JY

Subjects

Animals, Mice, Alzheimer Disease drug therapy, Alzheimer Disease pathology, Alzheimer Disease metabolism, Disease Models, Animal, Male, Positron-Emission Tomography, Antipsychotic Agents pharmacology, Antipsychotic Agents therapeutic use, Aripiprazole pharmacology, Aripiprazole therapeutic use, Glutamic Acid metabolism, Memory Disorders drug therapy, Memory Disorders pathology, Mice, Transgenic

Abstract

Purpose: Many patients with Alzheimer's disease (AD) also have psychosis, and it has been reported that these patients have more severely impaired cognitive functions than patients without psychosis. The glutamatergic system in the brain is known to play an important role in memory and learning in the neural circuits. However, there has been limited research on how antipsychotic drugs affect the glutamatergic system of AD. Therefore, we aimed to investigate the effects of aripiprazole on the glutamatergic system in an animal model of AD using functional molecular imaging., Procedures: In this study, 5xFAD mice were used as the animal model. At the age of 5 months, the mice were divided into wild-type, vehicle control, and aripiprazole-treated groups (n = 6 per group). The aripiprazole-treated group was administered aripiprazole for 2 months at a dose of 1 mg·kg -1 ·day -1 . At 7 months of age, the animals underwent behavioral tests and glutamate positron emission tomography (PET) scans., Results: The aripiprazole-treated group exhibited alleviated memory impairment in a novel object recognition test. Moreover, this group displayed 7-8% higher binding in the glutamate PET scan than the vehicle-treated 5xFAD group. Postmortem examination confirmed the recovery of glutamatergic damage., Conclusions: The administration of aripiprazole alleviated memory impairment and restored the damaged glutamatergic system in 5xFAD mice. Although the use of aripiprazole in AD patients may be a constraint in terms of safety, we confirmed the possibility that the administration of antipsychotic drugs can be effective in AD., (© 2024. The Author(s), under exclusive licence to World Molecular Imaging Society.)

Published

2024

46. Elevated serum LDL-C increases the risk of Lewy body dementia: a two-sample mendelian randomization study.

Author

Liu, Pengdi, Liu, Jin, Zhang, Yafei, Xing, Xin, Zhou, Le, Qu, Jianqiang, and Yan, Xianxia

Subjects

LEWY body dementia, LDL cholesterol, BLOOD lipids, HDL cholesterol, GENOME-wide association studies

Abstract

Background: Lewy body dementia (LBD) ranks second among prevalent neurodegenerative dementias. Previous studies have revealed associations of serum lipid measures with several neurodegenerative diseases. Nevertheless, the potential connection between serum lipids and LBD remains undetermined. In this study, Mendelian randomization (MR) analyses were carried out to assess the causal relationships of several serum lipid measures with the risk of developing LBD. Methods: Genome-wide association study (GWAS) data for serum lipids and LBD in European descent individuals were acquired from publicly available genetic summary data. A series of filtering procedures were conducted to identify the genetic variant candidates that are related to serum lipids, including high-density lipoprotein cholesterol (HDL-C), low-density lipoprotein cholesterol (LDL-C), and triglycerides (TG). The causal effects were primarily determined through inverse-variance weighting (IVW)-based analyses. Results: Neither TG (odds ratio [OR] = 1.149; 95% confidence interval [CI], 0.887–1.489; P = 0.293) nor HDL-C (OR = 0.864; 95% CI, 0.718–1.041; P = 0.124) had causal effects on LBD. However, a causal relationship was identified between LDL-C and LBD (OR = 1.343; 95% CI, 1.094–1.649; P = 0.005), which remained significant (OR = 1.237; 95% CI, 1.015–1.508; P = 0.035) following adjustment for HDL-C and TG in multivariable MR. Conclusions: Elevated serum LDL-C increases the risk of LBD, while HDL-C and TG have no significant causal effects on LBD. [ABSTRACT FROM AUTHOR]

Published

2024

47. The Density of Regulatory Information Is a Major Determinant of Evolutionary Constraint on Noncoding DNA in Drosophila.

Author

Sabarís, Gonzalo, Ortíz, Daniela M, Laiker, Ian, Mayansky, Ignacio, Naik, Sujay, Cavalli, Giacomo, Stern, David L, Noon, Ella Preger-Ben, and Frankel, Nicolás

Subjects

NON-coding DNA, DROSOPHILA, DROSOPHILA melanogaster, REGULATOR genes, DENSITY

Abstract

Evolutionary analyses have estimated that ∼60% of nucleotides in intergenic regions of the Drosophila melanogaster genome are functionally relevant, suggesting that regulatory information may be encoded more densely in intergenic regions than has been revealed by most functional dissections of regulatory DNA. Here, we approached this issue through a functional dissection of the regulatory region of the gene shavenbaby (svb). Most of the ∼90 kb of this large regulatory region is highly conserved in the genus Drosophila , though characterized enhancers occupy a small fraction of this region. By analyzing the regulation of svb in different contexts of Drosophila development, we found that the regulatory information that drives svb expression in the abdominal pupal epidermis is organized in a different way than the elements that drive svb expression in the embryonic epidermis. While in the embryonic epidermis svb is activated by compact enhancers separated by large inactive DNA regions, svb expression in the pupal epidermis is driven by regulatory information distributed over broader regions of svb cis -regulatory DNA. In the same vein, we observed that other developmental genes also display a dense distribution of putative regulatory elements in their regulatory regions. Furthermore, we found that a large percentage of conserved noncoding DNA of the Drosophila genome is contained within regions of open chromatin. These results suggest that part of the evolutionary constraint on noncoding DNA of Drosophila is explained by the density of regulatory information, which may be greater than previously appreciated. [ABSTRACT FROM AUTHOR]

Published

2024

48. Neuropathological and sociodemographic factors associated with the cortical amyloid load in aging and Alzheimer's disease.

Author

da Silva, Sayonara P., de Castro, Carla C. M., Rabelo, Lívia N., Engelberth, Rovena C., Fernández-Calvo, Bernardino, and Fiuza, Felipe P.

Subjects

ALZHEIMER'S disease, SOCIODEMOGRAPHIC factors, TAU proteins, AMYLOID, OCTOGENARIANS

Abstract

Alzheimer's disease (AD) is the leading cause of dementia and is characterized by a progressive decline in cognitive abilities. A pathological hallmark of AD is a region-specific accumulation of the amyloid-beta protein (Aβ). Here, we explored the association between regional Aβ deposition, sociodemographic, and local biochemical factors. We quantified the Aβ burden in postmortem cortical samples from parietal (PCx) and temporal (TCx) regions of 27 cognitively unimpaired (CU) and 15 AD donors, aged 78–100 + years. Histological images of Aβ immunohistochemistry and local concentrations of pathological and inflammatory proteins were obtained at the "Aging, Dementia and TBI Study" open database. We used the area fraction fractionator stereological methodology to quantify the Aβ burden in the gray and white matter within each cortical region. We found higher Aβ burdens in the TCx of AD octogenarians compared to CU ones. We also found higher Aβ loads in the PCx of AD nonagenarians than in AD octogenarians. Moreover, AD women exhibited increased Aβ deposition compared to CU women. Interestingly, we observed a negative correlation between education years and Aβ burden in the white matter of both cortices in CU samples. In AD brains, the Aβ40, Aβ42, and pTau181 isoforms of Aβ and Tau proteins were positively correlated with the Aβ burden. Additionally, in the TCx of AD donors, the proinflammatory cytokine TNFα showed a positive correlation with the Aβ load. These novel findings contribute to understanding the interplay between sociodemographic characteristics, local inflammatory signaling, and the development of AD-related pathology in the cerebral cortex. [ABSTRACT FROM AUTHOR]

Published

2024

49. Digestibility of crude nutrients and minerals in C57Bl/6J and CD1 mice fed a pelleted lab rodent diet.

Author

Böswald, Linda F., Matzek, Dana, and Popper, Bastian

Subjects

PELLETED feed, LABORATORY mice, LABORATORY animals, DIET, NUTRITIONAL requirements, ANIMAL feeds

Abstract

In laboratory animals, there is a scarcity of digestibility data under non-experimental conditions. Such data is important as basis to generate nutrient requirements, which contributes to the refinement of husbandry conditions. Digestibility trials can also help to identify patterns of absorption and potential factors that influence the digestibility. Thus, a digestibility trial with a pelleted diet used as standard feed in laboratory mice was conducted. To identify potential differences between genetic lines, inbred C57Bl/6 J and outbred CD1 mice (n = 18 each, male, 8 weeks-old, housed in groups of three) were used. For seven days, the feed intake was recorded and the total faeces per cage collected. Energy, crude nutrient and mineral content of diet and faecal samples were analyzed to calculate the apparent digestibility (aD). Apparent dry matter and energy digestibility did not differ between both lines investigated. The C57Bl/6 J mice had significantly higher aD of magnesium and potassium and a trend towards a lower aD of sodium than the mice of the CD1 outbred stock. Lucas-tests were performed to calculate the mean true digestibility of the nutrients and revealed a uniformity of the linear regression over data from both common laboratory mouse lines. The mean true digestibility of crude nutrients was > 90%, except for fibre, that of the minerals ranged between 66 and 97%. [ABSTRACT FROM AUTHOR]

Published

2024

50. A Continuous Extension of Gene Set Enrichment Analysis Using the Likelihood Ratio Test Statistics Identifies Vascular Endothelial Growth Factor as a Candidate Pathway for Alzheimer's Disease via ITGA5.

Author

Mahzarnia, Ali, Lutz, Michael W., and Badea, Alexandra

Subjects

VASCULAR endothelial growth factors, LIKELIHOOD ratio tests, ALZHEIMER'S disease, VASCULAR endothelial growth factor receptors, NEUROFIBRILLARY tangles

Abstract

Background: Alzheimer's disease (AD) involves brain neuropathologies such as amyloid plaque and hyperphosphorylated tau tangles and is accompanied by cognitive decline. Identifying the biological mechanisms underlying disease onset and progression based on quantifiable phenotypes will help understand disease etiology and devise therapies. Objective: Our objective was to identify molecular pathways associated with hallmark AD biomarkers and cognitive status, accounting for variables such as age, sex, education, and APOE genotype. Methods: We introduce a pathway-based statistical approach, extending the gene set likelihood ratio test to continuous phenotypes. We first analyzed independently each of the three phenotypes (amyloid-β, tau, cognition) using continuous gene set likelihood ratio tests to account for covariates, including age, sex, education, and APOE genotype. The analysis involved 634 subjects with data available for all three phenotypes, allowing for the identification of common pathways. Results: We identified 14 pathways significantly associated with amyloid-β; 5 associated with tau; and 174 associated with cognition, which showed a larger number of pathways compared to biomarkers. A single pathway, vascular endothelial growth factor receptor binding (VEGF-RB), exhibited associations with all three phenotypes. Mediation analysis showed that among the VEGF-RB family genes, ITGA5 mediates the relationship between cognitive scores and pathological biomarkers. Conclusions: We presented a new statistical approach linking continuous phenotypes, gene expression across pathways, and covariates like sex, age, and education. Our results reinforced VEGF RB2's role in AD cognition and demonstrated ITGA5's significant role in mediating the AD pathology-cognition connection. [ABSTRACT FROM AUTHOR]

Published

2024