Your search keyword '"laser capture microdissection"' showing total 6,749 results

1. Vascularized characteristics and functional regeneration of three-dimensional cell reconstruction of oral mucosa equivalents based on vascular homeostasis phenotypic modification.

Author

Shi, Lijuan, Xu, Yiwen, Li, Jingying, He, Li, Li, Kaiyu, Yin, Shigang, Nie, Minhai, and Liu, Xuqian

Subjects

*IMAGING systems, *CARDIOVASCULAR system, *ULTRASONIC imaging, *SCANNING electron microscopy, *HOMEOSTASIS, *ORAL mucosa

Abstract

Our prior research has effectively developed tissue-engineered vascularized oral mucosa equivalents (VOME); however, challenges such as low repeatability and stability, as well as the inability to accurately replicate the complexity of real blood vessels, were encountered. Therefore, this study aimed to screen the VOME and native oral mucosa vascular homeostasis phenotypes by tandem mass tag-tagged proteomics associated with laser capture microdissection and human angiogenesis antibody array technology. Then, lentiviruses were constructed and stably transfected with vascular endothelial-like cells (VELCs) to detect angiogenic capacity. HE, EdU Apollo tracer staining, immunofluorescence staining, scanning electron microscopy, biomechanical testing, and a small animal ultrasound imaging system were used to analyze the characteristics of vascularization homeostasis and monitor functional regeneration of the vascularized homeostatic phenotypic oral mucosal equivalents (VHPOME). The results showed that PGAM1, COL5A1, ANG, and RNH1 are potential specific angiogenesis phenotypes. High expression of PGAM1, COL5A1, and ANG and/or low expression of RNH1 can promote the angiogenesis of VOME. ANG/shRNH1 has the most significant tube-like structure-formation ability. The expression of PGAM1, COL5A1, and ANG in the VHPOME group was higher than that of the control group, and the expression of RNH1 was lower than that of the control group. COL5A1/ANG can significantly improve the mechanical properties. The blood flow signal was most significant in the ANG/shRNH1 group. PGAM1, COL5A1, ANG, shRNH1, PGAM1/ANG, COL5A1/ANG, PGAM1/shRNH1, PGAM1/shRNH1, COL5A1/shRNH1, and ANG/shRNH1 may be the targets for establishing vascularization homeostasis and functional regeneration of oral mucosal equivalent genes (groups), and ANG/shRNH1 has the most significant effect. [ABSTRACT FROM AUTHOR]

Published

2024

2. Hippocampal CA1 Pyramidal Neurons Display Sublayer and Circuitry Dependent Degenerative Expression Profiles in Aged Female Down Syndrome Mice.

Author

Alldred, Melissa J., Pidikiti, Harshitha, Ibrahim, Kryillos W., Lee, Sang Han, Heguy, Adriana, Hoffman, Gabriel E., Mufson, Elliott J., Stutzmann, Grace E., and Ginsberg, Stephen D.

Subjects

*ALZHEIMER'S disease, *INNERVATION, *TEMPORAL lobe, *DOWN syndrome, *RNA sequencing, *PYRAMIDAL neurons

Abstract

Background: Individuals with Down syndrome (DS) have intellectual disability and develop Alzheimer's disease (AD) pathology during midlife, particularly in the hippocampal component of the medial temporal lobe memory circuit. However, molecular and cellular mechanisms underlying selective vulnerability of hippocampal CA1 neurons remains a major knowledge gap during DS/AD onset. This is compounded by evidence showing spatial (e.g., deep versus superficial) localization of pyramidal neurons (PNs) has profound effects on activity and innervation within the CA1 region. Objective: We investigated whether there is a spatial profiling difference in CA1 PNs in an aged female DS/AD mouse model. We posit dysfunction may be dependent on spatial localization and innervation patterns within discrete CA1 subfields. Methods: Laser capture microdissection was performed on trisomic CA1 PNs in an established mouse model of DS/AD compared to disomic controls, isolating the entire CA1 pyramidal neuron layer and sublayer microisolations of deep and superficial PNs from the distal CA1 (CA1a) region. Results: RNA sequencing and bioinformatic inquiry revealed dysregulation of CA1 PNs based on spatial location and innervation patterns. The entire CA1 region displayed the most differentially expressed genes (DEGs) in trisomic mice reflecting innate DS vulnerability, while trisomic CA1a deep PNs exhibited fewer but more physiologically relevant DEGs, as evidenced by bioinformatic inquiry. Conclusions: CA1a deep neurons displayed numerous DEGs linked to cognitive functions whereas CA1a superficial neurons, with approximately equal numbers of DEGs, were not linked to pathways of dysregulation, suggesting the spatial location of vulnerable CA1 PNs plays an important role in circuit dissolution. [ABSTRACT FROM AUTHOR]

Published

2024

3. Analysis of microisolated frontal cortex excitatory layer III and V pyramidal neurons reveals a neurodegenerative phenotype in individuals with Down syndrome.

Author

Alldred, Melissa J., Pidikiti, Harshitha, Ibrahim, Kyrillos W., Lee, Sang Han, Heguy, Adriana, Hoffman, Gabriel E., Roussos, Panos, Wisniewski, Thomas, Wegiel, Jerzy, Stutzmann, Grace E., Mufson, Elliott J., and Ginsberg, Stephen D.

Subjects

*AMYLOID beta-protein precursor, *GENE expression, *FRONTAL lobe, *ALZHEIMER'S disease, *HUMAN chromosomes

Abstract

We elucidated the molecular fingerprint of vulnerable excitatory neurons within select cortical lamina of individuals with Down syndrome (DS) for mechanistic understanding and therapeutic potential that also informs Alzheimer's disease (AD) pathophysiology. Frontal cortex (BA9) layer III (L3) and layer V (L5) pyramidal neurons were microisolated from postmortem human DS and age- and sex-matched controls (CTR) to interrogate differentially expressed genes (DEGs) and key biological pathways relevant to neurodegenerative programs. We identified > 2300 DEGs exhibiting convergent dysregulation of gene expression in both L3 and L5 pyramidal neurons in individuals with DS versus CTR subjects. DEGs included over 100 triplicated human chromosome 21 genes in L3 and L5 neurons, demonstrating a trisomic neuronal karyotype in both laminae. In addition, thousands of other DEGs were identified, indicating gene dysregulation is not limited to trisomic genes in the aged DS brain, which we postulate is relevant to AD pathobiology. Convergent L3 and L5 DEGs highlighted pertinent biological pathways and identified key pathway-associated targets likely underlying corticocortical neurodegeneration and related cognitive decline in individuals with DS. Select key DEGs were interrogated as potential hub genes driving dysregulation, namely the triplicated DEGs amyloid precursor protein (APP) and superoxide dismutase 1 (SOD1), along with key signaling DEGs including mitogen activated protein kinase 1 and 3 (MAPK1, MAPK3) and calcium calmodulin dependent protein kinase II alpha (CAMK2A), among others. Hub DEGs determined from multiple pathway analyses identified potential therapeutic candidates for amelioration of cortical neuron dysfunction and cognitive decline in DS with translational relevance to AD. [ABSTRACT FROM AUTHOR]

Published

2024

4. Salmonella‐driven intestinal edema in mice is characterized by tensed fibronectin fibers.

Author

Rappold, Ronja, Kalogeropoulos, Konstantinos, auf dem Keller, Ulrich, Vogel, Viola, and Slack, Emma

Subjects

*EDEMA, *BLOOD coagulation, *INTESTINES, *EXTRACELLULAR fluid, *FIBRONECTINS, *FIBRIN, *FIBERS

Abstract

Intestinal edema is a common manifestation of numerous gastrointestinal diseases and is characterized by the accumulation of fluid in the interstitial space of the intestinal wall. Technical advances in laser capture microdissection and low‐biomass proteomics now allow us to specifically characterize the intestinal edema proteome. Using advanced proteomics, we identify peptides derived from antimicrobial factors with high signal intensity, but also highlight major contributions from the blood clotting system, extracellular matrix (ECM) and protease–protease inhibitor networks. The ECM is a complex fibrillar network of macromolecules that provides structural and mechanical support to the intestinal tissue. One abundant component of the ECM observed in Salmonella‐driven intestinal edema is the glycoprotein fibronectin, recognized for its structure–function interplay regulated by mechanical forces. Using mechanosensitive staining of fibronectin fibers reveals that they are tensed in the edema, despite the high abundance of proteases able to cleave fibronectin. In contrast, fibronectin fibers increasingly relax in other cecal tissue areas as the infection progresses. Co‐staining for fibrin(ogen) indicates the formation of a provisional matrix in the edema, similar to what is observed in response to skin injury, while collagen staining reveals a sparse and disrupted collagen fiber network. These observations plus the absence of low tensional fibronectin fibers and the additional finding of a high number of protease inhibitors in the edema proteome could indicate a critical role of stretched fibronectin fibers in maintaining tissue integrity in the severely inflamed cecum. Understanding these processes may also provide valuable functional diagnostic markers of intestinal disease progression in the future. [ABSTRACT FROM AUTHOR]

Published

2024

5. Effect of dynamic exclusion and the use of FAIMS, DIA and MALDI-mass spectrometry imaging with ion mobility on amyloid protein identification.

Author

Aguilan, Jennifer T., Lim, Jihyeon, Racine-Brzostek, Sabrina, Fischer, Joshua, Silvescu, Cristina, Cornett, Shannon, Nieves, Edward, Mendu, Damodara Rao, Aliste, Carlos-Madrid, Semple, Stacia, Angeletti, Ruth, Weiss, Louis M., Cole, Adam, Prystowsky, Michael, Pullman, James, and Sidoli, Simone

Subjects

*ION mobility spectroscopy, *TANDEM mass spectrometry, *PROTEOMICS, *ION mobility, *LIQUID chromatography-mass spectrometry, *AMYLOID

Abstract

Amyloidosis is a disease characterized by local and systemic extracellular deposition of amyloid protein fibrils where its excessive accumulation in tissues and resistance to degradation can lead to organ failure. Diagnosis is challenging because of approximately 36 different amyloid protein subtypes. Imaging methods like immunohistochemistry and the use of Congo red staining of amyloid proteins for laser capture microdissection combined with liquid chromatography tandem mass spectrometry (LMD/LC–MS/MS) are two diagnostic methods currently used depending on the expertise of the pathology laboratory. Here, we demonstrate a streamlined in situ amyloid peptide spatial mapping by Matrix Assisted Laser Desorption Ionization–Mass Spectrometry Imaging (MALDI-MSI) combined with Trapped Ion Mobility Spectrometry for potential transthyretin (ATTR) amyloidosis subtyping. While we utilized the standard LMD/LC–MS/MS workflow for amyloid subtyping of 31 specimens from different organs, we also evaluated the potential introduction in the MS workflow variations in data acquisition parameters like dynamic exclusion, or testing Data Dependent Acquisition combined with High-Field Asymmetric Waveform Ion Mobility Spectrometry (DDA FAIMS) versus Data Independent Acquisition (DIA) for enhanced amyloid protein identification at shorter acquisition times. We also demonstrate the use of Mascot's Error Tolerant Search and PEAKS de novo sequencing for the sequence variant analysis of amyloidosis specimens. [ABSTRACT FROM AUTHOR]

Published

2024

6. Minimal Change Disease: Pathogenetic Insights from Glomerular Proteomics.

Author

Bărar, Andrada Alina, Pralea, Ioana-Ecaterina, Maslyennikov, Yuriy, Munteanu, Raluca, Berindan-Neagoe, Ioana, Pîrlog, Radu, Rusu, Ioana, Nuțu, Andreea, Rusu, Crina Claudia, Moldovan, Diana Tania, Potra, Alina Ramona, Tirinescu, Dacian, Ticala, Maria, Elec, Florin Ioan, Iuga, Cristina Adela, and Kacso, Ina Maria

Subjects

*PROTEOMICS, *FOCAL adhesions, *EXTRACELLULAR matrix, *PRINCIPAL components analysis, *RENAL biopsy, *CYTOSKELETON

Abstract

The mechanism underlying podocyte dysfunction in minimal change disease (MCD) remains unknown. This study aimed to shed light on the potential pathophysiology of MCD using glomerular proteomic analysis. Shotgun proteomics using label-free quantitative mass spectrometry was performed on formalin-fixed, paraffin-embedded (FFPE) renal biopsies from two groups of samples: control (CTR) and MCD. Glomeruli were excised from FFPE renal biopsies using laser capture microdissection (LCM), and a single-pot solid-phase-enhanced sample preparation (SP3) digestion method was used to improve yield and protein identifications. Principal component analysis (PCA) revealed a distinct separation between the CTR and MCD groups. Forty-eight proteins with different abundance between the two groups (p-value ≤ 0.05 and |FC| ≥ 1.5) were identified. These may represent differences in podocyte structure, as well as changes in endothelial or mesangial cells and extracellular matrix, and some were indeed found in several of these structures. However, most differentially expressed proteins were linked to the podocyte cytoskeleton and its dynamics. Some of these proteins are known to be involved in focal adhesion (NID1 and ITGA3) or slit diaphragm signaling (ANXA2, TJP1 and MYO1C), while others are structural components of the actin and microtubule cytoskeleton of podocytes (ACTR3 and NES). This study suggests the potential of mass spectrometry-based shotgun proteomic analysis with LCM glomeruli to yield valuable insights into the pathogenesis of podocytopathies like MCD. The most significantly dysregulated proteins in MCD could be attributable to cytoskeleton dysfunction or may be a compensatory response to cytoskeleton malfunction caused by various triggers. [ABSTRACT FROM AUTHOR]

Published

2024

7. Cell‐type‐specific transcriptomics uncovers spatial regulatory networks in bioenergy sorghum stems.

Author

Fu, Jie, McKinley, Brian, James, Brandon, Chrisler, William, Markillie, Lye Meng, Gaffrey, Matthew J., Mitchell, Hugh D., Riaz, Muhammad Rizwan, Marcial, Brenda, Orr, Galya, Swaminathan, Kankshita, Mullet, John, and Marshall‐Colon, Amy

Subjects

*SORGHUM, *GENE regulatory networks, *GENETIC regulation, *TRANSCRIPTOMES, *SORGO, *SUSTAINABILITY, *ENERGY crops

Abstract

SUMMARY: Bioenergy sorghum is a low‐input, drought‐resilient, deep‐rooting annual crop that has high biomass yield potential enabling the sustainable production of biofuels, biopower, and bioproducts. Bioenergy sorghum's 4–5 m stems account for ~80% of the harvested biomass. Stems accumulate high levels of sucrose that could be used to synthesize bioethanol and useful biopolymers if information about cell‐type gene expression and regulation in stems was available to enable engineering. To obtain this information, laser capture microdissection was used to isolate and collect transcriptome profiles from five major cell types that are present in stems of the sweet sorghum Wray. Transcriptome analysis identified genes with cell‐type‐specific and cell‐preferred expression patterns that reflect the distinct metabolic, transport, and regulatory functions of each cell type. Analysis of cell‐type‐specific gene regulatory networks (GRNs) revealed that unique transcription factor families contribute to distinct regulatory landscapes, where regulation is organized through various modes and identifiable network motifs. Cell‐specific transcriptome data was combined with known secondary cell wall (SCW) networks to identify the GRNs that differentially activate SCW formation in vascular sclerenchyma and epidermal cells. The spatial transcriptomic dataset provides a valuable source of information about the function of different sorghum cell types and GRNs that will enable the engineering of bioenergy sorghum stems, and an interactive web application developed during this project will allow easy access and exploration of the data (https://mc‐lab.shinyapps.io/lcm‐dataset/). [ABSTRACT FROM AUTHOR]

Published

2024

8. The isolation strategy and chemical analysis of oil cells from Asari Radix et Rhizoma.

Author

Hu, Haibo, Liu, Guangxue, and Li, Yaoli

Subjects

*ANALYTICAL chemistry, *CELL analysis, *HERBAL medicine, *METHYL ether, *PLANT cells & tissues

Abstract

Background: Single-cell analysis, a rapidly evolving field, encounters significant challenges in detecting individual cells within complex plant tissues, particularly oil cells (OCs). The intricate process of single-cell isolation, coupled with the inherent chemical volatility of oil cells, necessitates a comprehensive methodology. Results: This study presents a method for obtaining intact OC from Asari Radix et Rhizoma (ARR), a traditional herbal medicine. The developed approach facilitates both qualitative and quantitative analysis of diverse OCs. To determine the most reliable approach, four practical methods—laser capture microdissection, micromanipulation capturing, micromanipulation piping, and cell picking—were systematically compared and evaluated, unequivocally establishing cell picking as the most effective method for OC isolation and chemical analysis. Microscopic observations showed that OCs predominantly distribute in the cortex of adventitious and fibrous roots, as well as the pith and cortex of the rhizome, with distinct morphologies—oblong in roots and circular in rhizomes. Sixty-three volatile constituents were identified in OCs, with eighteen compounds exhibiting significant differences. Safrole, methyleugenol, and asaricin emerged as the most abundant constituents in OCs. Notably, cis-4-thujanol and tetramethylpyrazine were exclusive to rhizome OCs, while isoeugenol methyl ether was specific to fibrous root OCs based on the detections. ARR roots and rhizomes displayed marked disparities in OC distribution, morphology, and constituents. Conclusion: The study highlights the efficacy of cell picking coupled with HS–SPME–GC–MS as a flexible, reliable, and sensitive method for OC isolation and chemical analysis, providing a robust methodology for future endeavors in single-cell analyses. [ABSTRACT FROM AUTHOR]

Published

2024

9. Spatial MS multiomics on clinical prostate cancer tissues.

Author

Truong, Jacob X. M., Rao, Sushma R., Ryan, Feargal J., Lynn, David J., Snel, Marten F., Butler, Lisa M., and Trim, Paul J.

Subjects

*MULTIOMICS, *PROSTATE cancer, *RADICAL prostatectomy, *LIPIDOMICS, *BENIGN tumors, *MASS spectrometers

Abstract

Mass spectrometry (MS) and MS imaging (MSI) are used extensively for both the spatial and bulk characterization of samples in lipidomics and proteomics workflows. These datasets are typically generated independently due to different requirements for sample preparation. However, modern omics technologies now provide higher sample throughput and deeper molecular coverage, which, in combination with more sophisticated bioinformatic and statistical pipelines, make generating multiomics data from a single sample a reality. In this workflow, we use spatial lipidomics data generated by matrix-assisted laser desorption/ionization MSI (MALDI-MSI) on prostate cancer (PCa) radical prostatectomy cores to guide the definition of tumor and benign tissue regions for laser capture microdissection (LCM) and bottom-up proteomics all on the same sample and using the same mass spectrometer. Accurate region of interest (ROI) mapping was facilitated by the SCiLS region mapper software and dissected regions were analyzed using a dia-PASEF workflow. A total of 5525 unique protein groups were identified from all dissected regions. Lysophosphatidylcholine acyltransferase 1 (LPCAT1), a lipid remodelling enzyme, was significantly enriched in the dissected regions of cancerous epithelium (CE) compared to benign epithelium (BE). The increased abundance of this protein was reflected in the lipidomics data with an increased ion intensity ratio for pairs of phosphatidylcholines (PC) and lysophosphatidylcholines (LPC) in CE compared to BE. [ABSTRACT FROM AUTHOR]

Published

2024

10. Laser Capture Microdissection Transcriptome Reveals Spatiotemporal Tissue Gene Expression Patterns of Medicago truncatula Roots Responding to Rhizobia

Author

Elise Schnabel, Jacklyn Thomas, Rabia El-Hawaz, Yueyao Gao, William L. Poehlman, Suchitra Chavan, Asher Pasha, Eddi Esteban, Nicholas Provart, F. Alex Feltus, and Julia Frugoli

Subjects

laser capture microdissection, M. truncatula, nodulation, RNA-Seq, Microbiology, QR1-502, Botany, QK1-989

Abstract

We report a public resource for examining the spatiotemporal RNA expression of 54,893 Medicago truncatula genes during the first 72 h of response to rhizobial inoculation. Using a methodology that allows synchronous inoculation and growth of more than 100 plants in a single media container, we harvested the same segment of each root responding to rhizobia in the initial inoculation over a time course, collected individual tissues from these segments with laser capture microdissection, and created and sequenced RNA libraries generated from these tissues. We demonstrate the utility of the resource by examining the expression patterns of a set of genes induced very early in nodule signaling, as well as two gene families (CLE peptides and nodule specific PLAT-domain proteins) and show that despite similar whole-root expression patterns, there are tissue differences in expression between the genes. Using a rhizobial response dataset generated from transcriptomics on intact root segments, we also examined differential temporal expression patterns and determined that, after nodule tissue, the epidermis and cortical cells contained the most temporally patterned genes. We circumscribed gene lists for each time and tissue examined and developed an expression pattern visualization tool. Finally, we explored transcriptomic differences between the inner cortical cells that become nodules and those that do not, confirming that the expression of 1-aminocyclopropane-1-carboxylate synthases distinguishes inner cortical cells that become nodules and provide and describe potential downstream genes involved in early nodule cell division. [Graphic: see text] Copyright © 2023 The Author(s). This is an open access article distributed under the CC BY-NC-ND 4.0 International license.

Published

2023

11. Substance P, NPY, CCK and their receptors in five brain regions in major depressive disorder with transcriptomic analysis of locus coeruleus neurons.

Author

Barde, Swapnali, Aguila, Julio, Zhong, Wen, Solarz, Anna, Mei, Irene, Prud'homme, Josee, Palkovits, Miklos, Turecki, Gustavo, Mulder, Jan, Uhlén, Mathias, Nagy, Corina, Mechawar, Naguib, Hedlund, Eva, and Hökfelt, Tomas

Subjects

*LOCUS coeruleus, *MENTAL depression, *SUBSTANCE P, *SUICIDE, *NORADRENERGIC neurons, *GENE expression, *NEURONS, *POSTMORTEM changes

Abstract

Major depressive disorder (MDD) is a serious disease and a burden to patients, families and society. Rodent experiments and human studies suggest that several neuropeptide systems are involved in mood regulation. The aim of this study is two-fold: (i) to monitor, with qPCR, transcript levels of the substance P/tachykinin (TAC), NPY and CCK systems in bulk samples from control and suicide subjects, targeting five postmortem brain regions including locus coeruleus (LC); and (ii) to analyse expression of neuropeptide family transcripts in LC neurons of 'normal' postmortem brains by using laser capture microdissection with Smart-Seq2 RNA sequencing. qPCR revealed distinct regional expression patterns in male and female controls with higher levels for the TAC system in the dorsal raphe nucleus and LC, versus higher transcripts levels of the NPY and CCK systems in prefrontal cortex. In suicide patients, TAC, TAC receptors and a few NPY family transcript levels were increased mainly in prefrontal cortex and LC. The second study on 'normal' noradrenergic LC neurons revealed expression of transcripts for GAL, NPY, TAC1, CCK , and TACR1 and many other peptides (e.g. Cerebellin4 and CARTPT) and receptors (e.g. Adcyap1R1 and GPR173). These data and our previous results on suicide brains indicates that the tachykinin and galanin systems may be valid targets for developing antidepressant medicines. Moreover, the perturbation of neuropeptide systems in MDD patients, and the detection of further neuropeptide and receptor transcripts in LC, shed new light on signalling in noradrenergic LC neurons and on mechanisms possibly associated with mood disorders. [ABSTRACT FROM AUTHOR]

Published

2024

12. Laser capture microdissection provides a novel molecular profile of human primary cutaneous melanoma.

Author

Navrazhina, Kristina, Garcet, Sandra, Williams, Samuel C., Gulati, Nicholas, Kiecker, Felix, Frew, John W., Mitsui, Hiroshi, and Krueger, James G.

Subjects

*GENE expression profiling, *MELANOMA, *MICRODISSECTION, *TISSUE analysis, *CANCER-related mortality, *LASERS

Abstract

Melanoma accounts for the majority of skin cancer‐related mortality, highlighting the need to better understand melanoma initiation and progression. In‐depth molecular analysis of neoplastic melanocytes in whole tissue biopsies may be diluted by inflammatory infiltration, which may obscure gene signatures specific to neoplastic cells. Thus, a method is needed to precisely uncover molecular changes specific to tumor cells from a limited sample of primary melanomas. Here, we performed laser capture microdissection (LCM) and gene expression profiling of patient‐derived frozen sections of pigmented lesions and primary cutaneous melanoma. Compared to bulk tissue analysis, analysis of LCM‐derived samples identified 9528 additional differentially expressed genes (DEGs) including melanocyte‐specific genes like PMEL and TYR, with enriched of pathways related to cell proliferation. LCM methodology also identified potentially targetable kinases specific to melanoma cells that were not detected by bulk tissue analysis. Taken together, our data demonstrate that there are marked differences in gene expression profiles depending on the method of sample isolation. We found that LCM captured higher expression of melanoma‐related genes while whole tissue biopsy identified a wider range of inflammatory markers. Taken together, our data demonstrate that LCM is a valid approach to identify melanoma‐specific changes using a relatively small amount of primary patient‐derived melanoma sample. [ABSTRACT FROM AUTHOR]

Published

2024

13. Distinct transcriptomic responses to Aβ plaques, neurofibrillary tangles, and APOE in Alzheimer's disease.

Author

Das, Sudeshna, Li, Zhaozhi, Wachter, Astrid, Alla, Srinija, Noori, Ayush, Abdourahman, Aicha, Tamm, Joseph A., Woodbury, Maya E., Talanian, Robert V., Biber, Knut, Karran, Eric H., Hyman, Bradley T., and Serrano‐Pozo, Alberto

Abstract

INTRODUCTION: Omics studies have revealed that various brain cell types undergo profound molecular changes in Alzheimer's disease (AD) but the spatial relationships with plaques and tangles and APOE‐linked differences remain unclear. METHODS: We performed laser capture microdissection of amyloid beta (Aβ) plaques, the 50 μm halo around them, tangles with the 50 μm halo around them, and areas distant (> 50 μm) from plaques and tangles in the temporal cortex of AD and control donors, followed by RNA‐sequencing. RESULTS: Aβ plaques exhibited upregulated microglial (neuroinflammation/phagocytosis) and downregulated neuronal (neurotransmission/energy metabolism) genes, whereas tangles had mostly downregulated neuronal genes. Aβ plaques had more differentially expressed genes than tangles. We identified a gradient Aβ plaque > peri‐plaque > tangle > distant for these changes. AD APOE ε4 homozygotes had greater changes than APOE ε3 across locations, especially within Aβ plaques. DISCUSSION: Transcriptomic changes in AD consist primarily of neuroinflammation and neuronal dysfunction, are spatially associated mainly with Aβ plaques, and are exacerbated by the APOE ε4 allele. [ABSTRACT FROM AUTHOR]

Published

2024

14. Gene Expression Analysis of Laser-Captured Purkinje Cells in the Essential Tremor Cerebellum.

Author

Martuscello, Regina T., Sivaprakasam, Karthigayini, Hartstone, Whitney, Kuo, Sheng-Han, Konopka, Genevieve, Louis, Elan D., and Faust, Phyllis L.

Subjects

*ESSENTIAL tremor, *PURKINJE cells, *GENE expression, *CEREBELLAR cortex, *ION transport (Biology), *CEREBELLUM

Abstract

Essential tremor (ET) is a common, progressive neurological disease characterized by an 8–12-Hz kinetic tremor. Despite its high prevalence, the patho-mechanisms of tremor in ET are not fully known. Through comprehensive studies in postmortem brains, we identified major morphological changes in the ET cerebellum that reflect cellular damage in Purkinje cells (PCs), suggesting that PC damage is central to ET pathogenesis. We previously performed a transcriptome analysis in ET cerebellar cortex, identifying candidate genes and several dysregulated pathways. To directly target PCs, we purified RNA from PCs isolated by laser capture microdissection and performed the first ever PC-specific RNA-sequencing analysis in ET versus controls. Frozen postmortem cerebellar cortex from 24 ETs and 16 controls underwent laser capture microdissection, obtaining ≥2000 PCs per sample. RNA transcriptome was analyzed via differential gene expression, principal component analysis (PCA), and gene set enrichment analyses (GSEA). We identified 36 differentially expressed genes, encompassing multiple cellular processes. Some ET (13/24) had greater dysregulation of these genes and segregated from most controls and remaining ETs in PCA. Characterization of genes/pathways enriched in this PCA and GSEA identified multiple pathway dysregulations in ET, including RNA processing/splicing, synapse organization/ion transport, and oxidative stress/inflammation. Furthermore, a different set of pathways characterized marked heterogeneity among ET patients. Our data indicate a range of possible mechanisms for the pathogenesis of ET. Significant heterogeneity among ET combined with dysregulation of multiple cellular processes supports the notion that ET is a family of disorders rather than one disease entity. [ABSTRACT FROM AUTHOR]

Published

2023

15. Proteomic patterns in glomerular research, a laser capture microdissection and liquid chromatography-tandem mass spectrometry approach

Author

Bărar Andrada A., Pralea Ioana E., Berindan-Neagoe Ioana, Pirlog Radu, Nutu Andreea, Maslyennikov Yuriy, Potra Alina R., Iuga Cristina A., and Kacso Ina M.

Subjects

proteomics, minimal change disease, focal segmental glomerulosclerosis, laser capture microdissection, tandem mass spectrometry, Medicine

Abstract

Introduction: Molecular techniques have the potential to shed light on glomerular diseases that conventional renal pathology may be unable to reveal. The aim of this study was to investigate whether proteomic patterns of glomeruli obtained from kidney biopsies can differentiate between minimal change disease (MCD), focal segmental glomerulosclerosis (FSGS) and control groups (CTR).

Published

2023

16. Plasma and Kidney Proteome Profiling Combined with Laser Capture Microdissection Reveal Large Increases in Immunoglobulins with Age

Author

Leanne J. G. Chan, Niclas Olsson, Magdalena Preciado López, Kayley Hake, Haruna Tomono, Matthew A. Veras, and Fiona E. McAllister

Subjects

proteomics, laser capture microdissection, aging, kidney, immunoglobulins, complement, Microbiology, QR1-502

Abstract

One of the main hallmarks of aging is aging-associated inflammation, also known as inflammaging. In this study, by comparing plasma and kidney proteome profiling of young and old mice using LC–MS profiling, we discovered that immunoglobulins are the proteins that exhibit the highest increase with age. This observation seems to have been disregarded because conventional proteome profiling experiments typically overlook the expression of high-abundance proteins or employ depletion methods to remove them before LC–MS analysis. We show that proteome profiling of immunoglobulins will likely be a useful biomarker of aging. Spatial profiling using immunofluorescence staining of kidney sections indicates that the main increases in immunoglobulins with age are localized in the glomeruli of the kidney. Using laser capture microdissection coupled with LC–MS, we show an increase in multiple immune-related proteins in glomeruli from aged mice. Increased deposition of immunoglobulins, immune complexes, and complement proteins in the kidney glomeruli may be a factor leading to reduced filtering capacity of the kidney with age. Therapeutic strategies to reduce the deposition of immunoglobulins in the kidney may be an attractive strategy for healthy aging.

Published

2024

17. Proteomics by Mass Spectrometry in the Typing of Amyloidosis

Author

Castelli, Jussara Bianchi, Carvalho, Valdemir Melechco, Xavier de Ávila, Diane, editor, and Villacorta Junior, Humberto, editor

Published

2023

18. Rapid assessment of 3-dimensional intra-tumor heterogeneity through cycling temperature capillary electrophoresis

Author

Anna Połeć, Per Olaf Ekstrøm, Christian Fougner, Therese Sørlie, and Jens Henrik Norum

Subjects

Laser capture microdissection, Cycling temperature capillary electrophoresis, Intra-tumor heterogeneity, 3D modeling, Medicine, Biology (General), QH301-705.5, Science (General), Q1-390

Abstract

Abstract Objective Tumors are heterogeneous three-dimensional masses populated by numerous cell types, including distinct sub-clones of cancerous cells. Various sub-clones within the same tumor mass may respond differently to cancer treatment, and intra-tumor heterogeneity contributes to acquired therapeutic resistance. Thus, one tissue biopsy will in most cases not be representative of the entire genetic landscape of a tumor mass. In this study, we aimed to establish an easily accessible, low cost method to address intra-tumor heterogeneity in three dimensions, for a limited number of DNA alterations. Results This study includes analyses of the three-dimensional (3D) distribution of DNA mutations in human colon cancer and mouse mammary gland tumor tissue samples. We used laser capture microdissection for the unbiased collection of tissue in several XY-planes throughout the tumor masses. Cycling temperature capillary electrophoresis was used to determine mutant allele frequency. High-resolution distribution maps of KRAS and Trp53 mutations were generated for each XY-plane in human and mouse tumor samples, respectively. To provide a holistic interpretation of the mutation distribution, we generated interactive 3D heatmaps giving an easily interpretable understanding of the spatial distribution of the analyzed mutations. The method described herein provides an accessible way of describing intra-tumor heterogeneity for a limited number of mutations.

Published

2023

19. The transcriptome reveals the molecular regulatory network of primordial follicle depletion in obese mice.

Author

Zhou, Jiaqi, Lin, Lin, Liu, Longping, Wang, Jianbin, Xia, Guoliang, and Wang, Chao

Subjects

*VASCULAR endothelial growth factors, *RNA sequencing, *OVARIAN follicle, *GRANULOSA cells, *OBESITY

Abstract

To explore the dynamic transcriptional regulatory network of primordial follicle fate in obese mice to elucidate the potential mechanism of primordial follicle depletion. Experimental study and transcriptomic analysis. Healthy (n=15) and obese (n=15) female mice. Six-week-old CD-1 mice were divided into healthy and high-fat diet groups and fed continuously for 12 weeks. The diet of healthy mice contained 10% fat. The diet of high-fat mice contained 60% fat. Primordial to primary follicle transition rate, gene expression changes, enriched Kyoto Encyclopedia of Genes and Genomes pathways, and ferroptosis. Primordial follicle depletion was increased in the ovaries of obese mice. We found that deposited fat around primordial and primary follicles of obese mice was higher than that for healthy mice. The proliferation of granulosa cells around primary follicles was increased in obese mice. In addition, we uncovered specific gene signatures associated with the primordial to primary follicle transition (PPT) in obese mice using laser capture microdissection RNA sequencing analysis. Gene set enrichment analysis indicated that ferroptosis, cell oxidation, vascular endothelial growth factor, and mammalian target of rapamycin signaling were increased significantly in the primordial follicles of obese mice. Notably, the ferritin, acyl CoA synthetase long-chain family member 4, and solid carrier family 7 member 11 associated proteins of the ferroptosis signaling pathway were significantly increased in the PPT phase of obese mice. Our work suggests that ferroptosis is a key pathway activated within immature ovarian follicles in the context of obesity and that the process may be involved in the physiological regulation of the PPT as well. [ABSTRACT FROM AUTHOR]

Published

2023

20. Proteomics and transcriptomics of the Betz cell in the human brain

Author

Scott, Connor, Ansorge, Olaf, and Fischer, Roman

Subjects

Motor neurons, Neuropathology, RNA sequencing, Molecular Biology, Laser Capture Microdissection, Neurobiology, Nervous system--Degeneration, Mass spectrometry, Neurons, Amyotrophic lateral sclerosis, Molecular Neuroscience

Abstract

Very little is known about the enigmatic gigantopyramidal neuron in the Primary Motor Cortex. These Betz cells are the largest neurons in the human brain, display unique morphology, play a fundamental role in voluntary movement, and are selectively vulnerable to a range of neurodegenerative diseases, including Amyotrophic Lateral Sclerosis (ALS). Yet, there has been no targeted studies to investigate the molecular profile of these neurons and how that may be affected in disease. Here, for the first time, laser microdissected human Betz cells were subjected to extensive proteomic analysis via a workflow that has been optimised to produce leading proteomic performance from individually pooled neurons. The proteome of the Betz cell has been comparatively analysed to similar neurons to reveal key insights into their physiology. This thesis molecularly confirms previous assumptions about their biology and discovers cellular mechanisms that are enriched within these neurons. To complement proteomic findings, laser microdissected Betz cells were also subjected to RNA-sequencing to investigate their gene expression patterns, to validate recently generated proteomic observations, and for the first time, to reveal the transcriptome of the Betz cell. To ease and improve future Betz cell research, the proteomic/transcriptomic data were screened to search for Betz cells biomarkers - for which there are currently none that immunochemically target Betz cells without also binding to surrounding neurons. Several proteins were identified that could selectively target Betz cells, potentially acting Betz cell biomarkers. Finally, proteomic/transcriptomic analysis was also applied to microdissected Betz cells from ALS patients to determine how/why these neurons degenerate in ALS. The findings herein, align with the excitotoxicity hypothesis of ALS, i.e. that upper motor neurons become over-activated by excess glutamate activity. These data also provide clues to other pathways that may cause the degeneration of Betz cells in ALS e.g. DNA damage, oxidative stress, dysregulated energy production, and impaired axonal guidance.

Published

2021

21. Establishing models of, and characterising the genomic context of, neutrophil hypersegmentation

Author

Fox, Eleonore and Summers, Charlotte

Subjects

neutrophil, ARDS, neutrophil hypersegmentation, microdissected neutrophils, multilobular nuclear architecture, transcriptomic analysis, HL-60, CD34+ cells, laser capture microdissection

Abstract

Neutrophils are the most prominent leukocytes in the human body and represent the first line of defence against invading pathogens. Their nuclear architecture is highly dynamic, composed of chromatin clustered into lobes that are linked together by dense heterochromatin. Both the underlying mechanism of how neutrophils alter their nuclear architecture and the purpose of their multilobed nuclear morphology remain poorly understood. Neutrophil nuclear hypersegmentation was previously reported to be associated with the maturation state of a neutrophil. More recently, it has been observed in other contexts, suggesting it may not be a marker of cell maturity, but rather one of functional status. Neutrophil hypersegmentation has been described in response to a wide array of stimuli, and clinically in the context of tumour-associated neutrophils (TANs), bacterial infection and in the lung alveolar compartment of patients with acute respiratory distress syndrome (ARDS). This thesis describes the establishment of a model of hypersegmentation in primary human neutrophils, via an investigation of the impact of the angiotensin converting enzyme inhibitor (ACEi) captopril, glucose concentration, and hypoxia. Furthermore, the current work outlines the optimisation of a laser capture microdissection (LCM) technique for the isolation of neutrophils, based on their morphologic phenotype, to permit RNA sequencing. This optimisation has led to the first description of the transcriptome of microdissected neutrophils, and has identified genes and pathways associated with nuclear hypersegmentation. Furthermore, it has demonstrated a robust method for the transcriptomic analysis of this previously reported challenging cell type, and describes the first RNA-seq analysis of aged primary human neutrophils. These insights into the early ageing mechanisms of neutrophils highlight that neutrophils are multifaceted cells with an active transcriptional program. Further, this work reveals that neutrophil hypersegmentation is not a homogenous phenomenon, but rather a phenotype that occurs in response to multiple stimuli via distinct mechanisms. The thesis also describes the differentiation of the pro-myoblastic cell line, HL-60s and CD34+ hematopoietic stem cells as potential neutrophil-like cellular models for the investigation of hypersegmentation. Morphological and functional analysis has identified that these cells acquired segmented nuclear morphologies, and the ability to produce reactive oxygen species, phagocytose bacteria and upregulated neutrophil cell surface markers, validating these cells as tools for the study and genetic manipulation of neutrophils.

Published

2021

22. Comparative analysis of embryo proper and suspensor transcriptomes in plant embryos with different morphologies

Author

Chen, Min, Lin, Jer-Young, Wu, Xiaomeng, Apuya, Nestor R, Henry, Kelli F, Le, Brandon H, Bui, Anhthu Q, Pelletier, Julie M, Cokus, Shawn, Pellegrini, Matteo, Harada, John J, and Goldberg, Robert B

Subjects

Plant Biology, Biological Sciences, Genetics, Human Genome, Biotechnology, 1.1 Normal biological development and functioning, Underpinning research, Arabidopsis, Cell Division, Gene Expression Regulation, Plant, Gibberellins, Plant Development, Plant Proteins, Seeds, Soybeans, Transcriptome, suspensor, embryo proper, transcriptome, laser capture, microdissection, ChIP-Seq, laser capture microdissection

Abstract

An important question is what genes govern the differentiation of plant embryos into suspensor and embryo proper regions following fertilization and division of the zygote. We compared embryo proper and suspensor transcriptomes of four plants that vary in embryo morphology within the suspensor region. We determined that genes encoding enzymes in several metabolic pathways leading to the formation of hormones, such as gibberellic acid, and other metabolites are up-regulated in giant scarlet runner bean and common bean suspensors. Genes involved in transport and Golgi body organization are up-regulated within the suspensors of these plants as well, strengthening the view that giant specialized suspensors serve as a hormone factory and a conduit for transferring substances to the developing embryo proper. By contrast, genes controlling transcriptional regulation, development, and cell division are up-regulated primarily within the embryo proper. Transcriptomes from less specialized soybean and Arabidopsis suspensors demonstrated that fewer genes encoding metabolic enzymes and hormones are up-regulated. Genes active in the embryo proper, however, are functionally similar to those active in scarlet runner bean and common bean embryo proper regions. We uncovered a set of suspensor- and embryo proper-specific transcription factors (TFs) that are shared by all embryos irrespective of morphology, suggesting that they are involved in early differentiation processes common to all plants. Chromatin immunoprecipitation sequencing (ChIP-Seq) experiments with scarlet runner bean and soybean WOX9, an up-regulated suspensor TF, gained entry into a regulatory network important for suspensor development irrespective of morphology.

Published

2021

23. Rapid assessment of 3-dimensional intra-tumor heterogeneity through cycling temperature capillary electrophoresis.

Author

Połeć, Anna, Ekstrøm, Per Olaf, Fougner, Christian, Sørlie, Therese, and Norum, Jens Henrik

Subjects

*MAMMARY gland cancer, *HETEROGENEITY, *CAPILLARY electrophoresis, *COLON cancer, *GENE frequency, *CIRCULATING tumor DNA, *HUMAN DNA

Abstract

Objective: Tumors are heterogeneous three-dimensional masses populated by numerous cell types, including distinct sub-clones of cancerous cells. Various sub-clones within the same tumor mass may respond differently to cancer treatment, and intra-tumor heterogeneity contributes to acquired therapeutic resistance. Thus, one tissue biopsy will in most cases not be representative of the entire genetic landscape of a tumor mass. In this study, we aimed to establish an easily accessible, low cost method to address intra-tumor heterogeneity in three dimensions, for a limited number of DNA alterations. Results: This study includes analyses of the three-dimensional (3D) distribution of DNA mutations in human colon cancer and mouse mammary gland tumor tissue samples. We used laser capture microdissection for the unbiased collection of tissue in several XY-planes throughout the tumor masses. Cycling temperature capillary electrophoresis was used to determine mutant allele frequency. High-resolution distribution maps of KRAS and Trp53 mutations were generated for each XY-plane in human and mouse tumor samples, respectively. To provide a holistic interpretation of the mutation distribution, we generated interactive 3D heatmaps giving an easily interpretable understanding of the spatial distribution of the analyzed mutations. The method described herein provides an accessible way of describing intra-tumor heterogeneity for a limited number of mutations. [ABSTRACT FROM AUTHOR]

Published

2023

24. Laser capture microdissection‐based spatiotemporal transcriptomes uncover regulatory networks during seed abortion in seedless Ponkan (Citrus reticulata).

Author

Lu, Liqing, Yang, Haijian, Xu, Yanhui, Zhang, Li, Wu, Juxun, and Yi, Hualin

Subjects

*ABORTION, *APOPTOSIS, *FUNCTIONAL genomics, *TRANSCRIPTOMES, *CITRUS fruits, *GENE regulatory networks

Abstract

SUMMARY: Seed abortion is an important process in the formation of seedless characteristics in citrus fruits. However, the molecular regulatory mechanism underlying citrus seed abortion is poorly understood. Laser capture microdissection‐based RNA‐seq combined with Pacbio‐seq was used to profile seed development in the Ponkan cultivars 'Huagan No. 4' (seedless Ponkan) (Citrus reticulata) and 'E'gan No. 1' (seeded Ponkan) (C. reticulata) in two types of seed tissue across three developmental stages. Through comparative transcriptome and dynamic phytohormone analyses, plant hormone signal, cell division and nutrient metabolism‐related processes were revealed to play critical roles in the seed abortion of 'Huagan No. 4'. Moreover, several genes may play indispensable roles in seed abortion of 'Huagan No. 4', such as CrWRKY74, CrWRKY48 and CrMYB3R4. Overexpression of CrWRKY74 in Arabidopsis resulted in severe seed abortion. By analyzing the downstream regulatory network, we further determined that CrWRKY74 participated in seed abortion regulation by inducing abnormal programmed cell death. Of particular importance is that a preliminary model was proposed to depict the regulatory networks underlying seed abortion in citrus. The results of this study provide novel insights into the molecular mechanism across citrus seed development, and reveal the master role of CrWRKY74 in seed abortion of 'Huagan No. 4'. Significance Statement: The seedless character of citrus has important economic value and is favored by consumers, but the formation process of its internal mechanism still lacks understanding. In this study, the molecular mechanism of seed abortion in seedless Ponkan caused by abnormal programmed cell death was preliminarily analyzed by functional genomics, cytological morphological observation, physiological and biochemical assays, as well as stable genetic transformation. [ABSTRACT FROM AUTHOR]

Published

2023

25. Localized proteomic differences in the choroid plexus of Alzheimer's disease and epilepsy patients.

Author

Leitner, Dominique F., Kanshin, Evgeny, Faustin, Arline, Thierry, Manon, Friedman, Daniel, Devore, Sasha, Ueberheide, Beatrix, Devinsky, Orrin, and Wisniewski, Thomas

Subjects

EPILEPSY, CHOROID plexus, ALZHEIMER'S patients, TEMPORAL lobe epilepsy, LATERAL geniculate body, ALZHEIMER'S disease

Abstract

Introduction: Alzheimer's disease (AD) and epilepsy are reciprocally related. Among sporadic AD patients, clinical seizures occur in 10-22% and subclinical epileptiform abnormalities occur in 22-54%. Cognitive deficits, especially short-term memory impairments, occur in most epilepsy patients. Common neurophysiological and molecular mechanisms occur in AD and epilepsy. The choroid plexus undergoes pathological changes in aging, AD, and epilepsy, including decreased CSF turnover, amyloid beta (Aβ), and tau accumulation due to impaired clearance and disrupted CSF amino acid homeostasis. This pathology may contribute to synaptic dysfunction in AD and epilepsy. Methods: We evaluated control (n = 8), severe AD (n = 8; A3, B3, C3 neuropathology), and epilepsy autopsy cases (n = 12) using laser capture microdissection (LCM) followed by label-free quantitative mass spectrometry on the choroid plexus adjacent to the hippocampus at the lateral geniculate nucleus level. Results: Proteomics identified 2,459 proteins in the choroid plexus. At a 5% false discovery rate (FDR), 616 proteins were differentially expressed in AD vs. control, 1 protein in epilepsy vs. control, and 438 proteins in AD vs. epilepsy. There was more variability in the epilepsy group across syndromes. The top 20 signaling pathways associated with differentially expressed proteins in AD vs. control included cell metabolism pathways; activated fatty acid beta-oxidation (p = 2.00 x 10-7, z = 3.00), and inhibited glycolysis (p = 1.00 x 10-12, z = -3.46). For AD vs. epilepsy, the altered pathways included cell metabolism pathways, activated complement system (p = 5.62 x 10-5, z = 2.00), and pathogen-induced cytokine storm (p = 2.19 x 10-2, z = 3.61). Of the 617 altered proteins in AD and epilepsy vs. controls, 497 (81%) were positively correlated (p < 0.0001, R² = 0.27). Discussion: We found altered signaling pathways in the choroid plexus of severe AD cases and many correlated changes in the protein expression of cell metabolism pathways in AD and epilepsy cases. The shared molecular mechanisms should be investigated further to distinguish primary pathogenic changes from the secondary ones. These mechanisms could inform novel therapeutic strategies to prevent disease progression or restore normal function. A focus on dual-diagnosed AD/epilepsy cases, specific epilepsy syndromes, such as temporal lobe epilepsy, and changes across different severity levels in AD and epilepsy would add to our understanding. [ABSTRACT FROM AUTHOR]

Published

2023

26. Performance of Human Papillomavirus Attribution Algorithms to Predict Causative Genotypes in Anal High-Grade Lesions.

Author

Phillips, Samuel, Cornall, Alyssa M, Molano, Monica, Jin, Fengyi, Roberts, Jennifer M, Farnsworth, Annabelle, Hillman, Richard J, Templeton, David J, Poynten, I Mary, Garland, Suzanne M, Fairley, Christopher K, Murray, Gerald L, Tabrizi, Sepehr N, Grulich, Andrew E, and Machalek, Dorothy A

Subjects

*HUMAN papillomavirus, *GENITAL warts, *GENOTYPES, *MAXIMUM likelihood statistics, *HIV, *ANAL cancer

Abstract

Background Gay and bisexual men (GBM) are at increased risk of human papillomavirus (HPV)–associated anal high-grade squamous intraepithelial lesions (HSILs). Understanding the fractions of HSILs attributable to HPV genotypes is important to inform potential impacts of screening and vaccination strategies. However, multiple infections are common, making attribution of causative types difficult. Algorithms developed for predicting HSIL-causative genotype fractions have never been compared with a reference standard in GBM. Method Samples were from the Study of the Prevention of Anal Cancer. Baseline HPV genotypes detected in anal swab samples (160 participants) were compared with HPV genotypes in anal HSILs (222 lesions) determined by laser capture microdissection (LCM). Five algorithms were compared: proportional, hierarchical, maximum, minimum, and maximum likelihood estimation. Results All algorithms predicted HPV-16 as the most common HSIL-causative genotype, and proportions differed from LCM detection (37.8%) by algorithm (with differences of −6.1%, +20.9%, −20.4%, +2.9%, and +2.2% respectively). Fractions predicted using the proportional method showed a strong positive correlation with LCM, overall (R = 0.73 and P =.002), and by human immunodeficiency virus (HIV) status (HIV positive, R = 0.74 and P =.001; HIV-negative, R = 0.68 and P =.005). Conclusions Algorithms produced a range of inaccurate estimates of HSIL attribution, with the proportional algorithm performing best. The high occurrence of multiple HPV infections means that these algorithms may be of limited use in GBM. [ABSTRACT FROM AUTHOR]

Published

2023

27. Basal forebrain cholinergic neurons are vulnerable in a mouse model of Down syndrome and their molecular fingerprint is rescued by maternal choline supplementation.

Author

Alldred, Melissa J., Pidikiti, Harshitha, Heguy, Adriana, Roussos, Panos, and Ginsberg, Stephen D.

Abstract

Basal forebrain cholinergic neuron (BFCN) degeneration is a hallmark of Down syndrome (DS) and Alzheimer's disease (AD). Current therapeutics in these disorders have been unsuccessful in slowing disease progression, likely due to poorly understood complex pathological interactions and dysregulated pathways. The Ts65Dn trisomic mouse model recapitulates both cognitive and morphological deficits of DS and AD, including BFCN degeneration and has shown lifelong behavioral changes due to maternal choline supplementation (MCS). To test the impact of MCS on trisomic BFCNs, we performed laser capture microdissection to individually isolate choline acetyltransferase‐immunopositive neurons in Ts65Dn and disomic littermates, in conjunction with MCS at the onset of BFCN degeneration. We utilized single population RNA sequencing (RNA‐seq) to interrogate transcriptomic changes within medial septal nucleus (MSN) BFCNs. Leveraging multiple bioinformatic analysis programs on differentially expressed genes (DEGs) by genotype and diet, we identified key canonical pathways and altered physiological functions within Ts65Dn MSN BFCNs, which were attenuated by MCS in trisomic offspring, including the cholinergic, glutamatergic and GABAergic pathways. We linked differential gene expression bioinformatically to multiple neurological functions, including motor dysfunction/movement disorder, early onset neurological disease, ataxia and cognitive impairment via Ingenuity Pathway Analysis. DEGs within these identified pathways may underlie aberrant behavior in the DS mice, with MCS attenuating the underlying gene expression changes. We propose MCS ameliorates aberrant BFCN gene expression within the septohippocampal circuit of trisomic mice through normalization of principally the cholinergic, glutamatergic, and GABAergic signaling pathways, resulting in attenuation of underlying neurological disease functions. [ABSTRACT FROM AUTHOR]

Published

2023

28. Transcriptomics at the Single Cell Level and Human Diseases: Opportunities and Challenges in Data Processing and Analysis

Author

Maracaja-Coutinho, Vinicius, Severino, Patricia, and Passos, Geraldo A., editor

Published

2022

29. Understanding of Root Nodule Development at Level of System Biology as Obtained by High Throughput Transcriptomic Approach

Author

Bhardwaj, Akanksha, Sinharoy, Senjuti, Kole, Chittaranjan, Series Editor, Sinharoy, Senjuti, editor, Kang, Yun, editor, and Benedito, Vagner, editor

Published

2022

30. Somatic copy number variant load in neurons of healthy controls and Alzheimer’s disease patients

Author

Zeliha Gözde Turan, Vincent Richter, Jana Bochmann, Poorya Parvizi, Etka Yapar, Ulas Işıldak, Sarah-Kristin Waterholter, Sabrina Leclere-Turbant, Çağdaş Devrim Son, Charles Duyckaerts, İdil Yet, Thomas Arendt, Mehmet Somel, and Uwe Ueberham

Subjects

Single-cell whole-genome sequencing, Copy number variation, Alzheimer’s disease, Brain, Laser capture microdissection, Fluorescence-activated cell sorting, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract The possible role of somatic copy number variations (CNVs) in Alzheimer’s disease (AD) aetiology has been controversial. Although cytogenetic studies suggested increased CNV loads in AD brains, a recent single-cell whole-genome sequencing (scWGS) experiment, studying frontal cortex brain samples, found no such evidence. Here we readdressed this issue using low-coverage scWGS on pyramidal neurons dissected via both laser capture microdissection (LCM) and fluorescence activated cell sorting (FACS) across five brain regions: entorhinal cortex, temporal cortex, hippocampal CA1, hippocampal CA3, and the cerebellum. Among reliably detected somatic CNVs identified in 1301 cells obtained from the brains of 13 AD patients and 7 healthy controls, deletions were more frequent compared to duplications. Interestingly, we observed slightly higher frequencies of CNV events in cells from AD compared to similar numbers of cells from controls (4.1% vs. 1.4%, or 0.9% vs. 0.7%, using different filtering approaches), although the differences were not statistically significant. On the technical aspects, we observed that LCM-isolated cells show higher within-cell read depth variation compared to cells isolated with FACS. To reduce within-cell read depth variation, we proposed a principal component analysis-based denoising approach that significantly improves signal-to-noise ratios. Lastly, we showed that LCM-isolated neurons in AD harbour slightly more read depth variability than neurons of controls, which might be related to the reported hyperploid profiles of some AD-affected neurons.

Published

2022

31. 不同检测标志物在宫颈腺癌中的诊断和预后 预测价值评估.

Author

张倡宁, 刘潇阳, 李青, 宋益哲, 刘彬, 阴建, 杨敬红, 钟理, 孙力, 张询, and 陈汶

Abstract

Objective To study the diagnostic value of different detection markers in histological categories of endocervical adenocarcinoma (ECA), and their assessment of patient prognosis. Methods A retrospective study of 54 patients with ECA in the Cancer Hospital, Chinese Academy of Medical Sciences from 2005-2010 were performed. The cases of ECA were classified into two categories, namely human papillomavirus-associated adenocarcinoma (HPVA) and non-human papillomavirus-associated adenocarcinoma (NHPVA), based on the 2018 international endocervical adenocarcinoma criteria and classification (IECC). To detect HR-HPV DNA and HR-HPV E6/E7 mRNA in all patients, we used whole tissue section PCR (WTS-PCR) and HPV E6/E7 mRNA in situ hybridization (ISH) techniques, respectively. Additionally, we performed Laser microdissection PCR (LCM-PCR) on 15 randomly selected HR-HPV DNA-positive cases to confirm the accuracy of the above two assays in identifying ECA lesions. Receiver operating characteristic (ROC) curves were used to analyze the efficacy of markers to identify HPVA and NHPVA. Univariate and multifactorial Cox proportional risk model regression analyses were performed for factors influencing ECA patients' prognoses. Results Of the 54 patients with ECA, 30 were HPVA and 24 were NHPVA. A total of 96.7% (29/30) of HPVA patients were positive for HR-HPV DNA and 63.3% (19/30) for HR-HPV E6/E7 mRNA, and 33.3% (8/24) of NHPVA patients were positive for HR-HPV DNA and HR-HPV E6/E7 mRNA was not detected (0/24), and the differences were statistically significant (P<0.001). LCM-PCR showed that five patients were positive for HR-HPV DNA in the area of glandular epithelial lesions and others were negative, which was in good agreement with the E6/E7 mRNA ISH assay (Kappa=0.842, P=0.001). Analysis of the ROC results showed that the AUC of HR-HPV DNA, HR-HPV E6/E7 mRNA, and p16 to identify HPVA and NHPVA were 0.817, 0.817, and 0.692, respectively, with sensitivities of 96.7%, 63.3%, and 80.0% and specificities of 66.7%, 100.0%, and 58.3%, respectively. HR-HPV DNA identified HPVA and NHPVA with higher AUC than p16 (P=0.044). The difference in survival rates between HR-HPV DNA (WTS-PCR assay) positive and negative patients was not statistically significant (P=0.156), while the difference in survival rates between HR-HPV E6/E7 mRNA positive and negative patients, and p16 positive and negative patients were statistically significant (both P<0.05). Multifactorial Cox regression analysis showed that International Federation of Obstetrics and Gynecology (FIGO) staging (HR= 19.875, 95% CI: 1.526-258.833) and parametrial involvement (HR = 14.032, 95% CI: 1.281-153.761) were independent factors influencing the prognosis of patients with ECA. Conclusions HR-HPV E6/E7 mRNA is more reflective of HPV infection in ECA tissue. The efficacy of HR-HPV E6/E7 mRNA and HR-HPV DNA (WTS-PCR assay) in identifying HPVA and NHPVA is similar, with higher sensitivity of HR-HPV DNA and higher specificity of HR-HPV E6/E7 mRNA. HR-HPV DNA is more effective than p16 in identifying HPVA and NHPVA. HPV E6/E7 mRNA and p16 positive ECA patients have better survival rates than negative. [ABSTRACT FROM AUTHOR]

Published

2023

32. Microisolation of Spatially Characterized Single Populations of Neurons for RNA Sequencing from Mouse and Postmortem Human Brain Tissues.

Author

Alldred, Melissa J. and Ginsberg, Stephen D.

Subjects

*RNA sequencing, *AUTOPSY, *GENE expression profiling, *NEURONS, *GENE expression

Abstract

Single-cell and single-population RNA sequencing (RNA-seq) is a rapidly evolving new field of intense investigation. Recent studies indicate unique transcriptomic profiles are derived based on the spatial localization of neurons within circuits and regions. Individual neuronal subtypes can have vastly different transcriptomic fingerprints, well beyond the basic excitatory neuron and inhibitory neuron designations. To study single-population gene expression profiles of spatially characterized neurons, we have developed a methodology combining laser capture microdissection (LCM), RNA purification of single populations of neurons, and subsequent library preparation for downstream applications, including RNA-seq. LCM provides the benefit of isolating single neurons characterized by morphology or via transmitter-identified and/or receptor immunoreactivity and enables spatial localization within the sample. We utilize unfixed human postmortem and mouse brain tissue that is frozen to preserve RNA quality in order to isolate the desired neurons of interest. Microisolated neurons are then pooled for RNA purification utilizing as few as 250 individual neurons from a tissue section, precluding extraneous nonspecific tissue contaminants. Library preparation is performed from picogram RNA quantities extracted from LCM-captured neurons. Single-population RNA-seq analysis demonstrates that microisolated neurons from both postmortem human and mouse brain tissues are viable for transcriptomic profiling, including differential gene expression assessment and bioinformatic pathway inquiry. [ABSTRACT FROM AUTHOR]

Published

2023

33. Dissection of Developmental Programs and Regulatory Modules Directing Endosperm Transfer Cell and Aleurone Identity in the Syncytial Endosperm of Barley.

Author

Hertig, Christian, Rutten, Twan, Melzer, Michael, Schippers, Jos H. M., and Thiel, Johannes

Subjects

DEVELOPMENTAL programs, ENDOSPERM, CELL differentiation, WNT signal transduction, IN situ hybridization, PROTEIN-protein interactions, PLANT hormones, BARLEY

Abstract

Endosperm development in barley starts with the formation of a multinucleate syncytium, followed by cellularization in the ventral part of the syncytium generating endosperm transfer cells (ETCs) as first differentiating subdomain, whereas aleurone (AL) cells will originate from the periphery of the enclosing syncytium. Positional signaling in the syncytial stage determines cell identity in the cereal endosperm. Here, we performed a morphological analysis and employed laser capture microdissection (LCM)-based RNA-seq of the ETC region and the peripheral syncytium at the onset of cellularization to dissect developmental and regulatory programs directing cell specification in the early endosperm. Transcriptome data revealed domain-specific characteristics and identified two-component signaling (TCS) and hormone activities (auxin, ABA, ethylene) with associated transcription factors (TFs) as the main regulatory links for ETC specification. On the contrary, differential hormone signaling (canonical auxin, gibberellins, cytokinin) and interacting TFs control the duration of the syncytial phase and timing of cellularization of AL initials. Domain-specific expression of candidate genes was validated by in situ hybridization and putative protein–protein interactions were confirmed by split-YFP assays. This is the first transcriptome analysis dissecting syncytial subdomains of cereal seeds and provides an essential framework for initial endosperm differentiation in barley, which is likely also valuable for comparative studies with other cereal crops. [ABSTRACT FROM AUTHOR]

Published

2023

34. The Transcription Factor Twist1 Has a Significant Role in Mycosis Fungoides (MF) Cell Biology: An RNA Sequencing Study of 40 MF Cases.

Author

Häyrinen, Marjaana J., Kiiskilä, Jenni, Ranki, Annamari, Väkevä, Liisa, Barton, Henry J., Kuusisto, Milla E. L., Porvari, Katja, Kuitunen, Hanne, Haapasaari, Kirsi-Maria, Teppo, Hanna-Riikka, and Kuittinen, Outi

Subjects

*DISEASE progression, *SEQUENCE analysis, *DNA, *MYCOSIS fungoides, *IMMUNOHISTOCHEMISTRY, *RNA, *GENE expression, *SKIN tumors, *LYMPHOCYTES, *DNA methylation, *RESEARCH funding, *CYTOLOGY, *TRANSCRIPTION factors, *CUTANEOUS T-cell lymphoma

Abstract

Simple Summary: Mycosis fungoides (MF) is the most common variety of cutaneous T-cell lymphoma. Our previous studies showed that the epithelial–mesenchymal transition (EMT) transcription factors (TFs) Twist1 and Zeb1 have prognostic value in MF. The main objective of the present study was to gain better knowledge about the biological mechanisms behind this phenomenon. The RNA of 40 skin tumor biopsies (from 40 patients) was sequenced and analyzed. Twist1 protein expression seemed to classify MF cases into different groups based on their global RNA expression. Additionally, high Twist1 protein expression was associated with several genes and pathways known to have roles in aggressive tumor biology. For Zeb1, similar results were not found. Our results suggest Twist1 to be a central transcription factor and pathway regulator in the disease progression of MF. Twist1 might be an interesting object for developing targeted therapies for MF. The purpose of this RNA sequencing study was to investigate the biological mechanism underlying how the transcription factors (TFs) Twist1 and Zeb1 influence the prognosis of mycosis fungoides (MF). We used laser-captured microdissection to dissect malignant T-cells obtained from 40 skin biopsies from 40 MF patients with stage I–IV disease. Immunohistochemistry (IHC) was used to determinate the protein expression levels of Twist1 and Zeb1. Based on RNA sequencing, principal component analysis (PCA), differential expression (DE) analysis, ingenuity pathway analysis (IPA), and hub gene analysis were performed between the high and low Twist1 IHC expression cases. The DNA from 28 samples was used to analyze the TWIST1 promoter methylation level. In the PCA, Twist1 IHC expression seemed to classify cases into different groups. The DE analysis yielded 321 significant genes. In the IPA, 228 significant upstream regulators and 177 significant master regulators/causal networks were identified. In the hub gene analysis, 28 hub genes were found. The methylation level of TWIST1 promoter regions did not correlate with Twist1 protein expression. Zeb1 protein expression did not show any major correlation with global RNA expression in the PCA. Many of the observed genes and pathways associated with high Twist1 expression are known to be involved in immunoregulation, lymphocyte differentiation, and aggressive tumor biology. In conclusion, Twist1 might be an important regulator in the disease progression of MF. [ABSTRACT FROM AUTHOR]

Published

2023

35. The ability of Lactobacillus helveticus -13 (Lh-13) Isolate Isolated from Lactic Acid Products to form A biofilm by Applying Modern Microscopy Methods.

Author

1., Zhanerke Amirkhanova, Akhmetova, Saule, Kozhakhmetov, Samat, Kushugulova, Almagul, Bodeeva, Rahat, Ahvlediani, Leila, and Turmukhambetova, Anara

Subjects

*LACTIC acid, *LACTIC acid bacteria, *ATOMIC force microscopy, *BIOFILMS, *MICROSCOPY, *LACTOBACILLUS

Abstract

This article presents the study of the morpho-cultural properties and biofilm formation of lactobacilli isolated from lactic acid products (irimchik, suzbe, cheese, ashygan kozhe) produced in different districts of the Karaganda region. The species of the isolated lactic acid bacillus isolates were identified by using a MALDI-TOF mass spectrometer. The evaluation of the resistance of the isolates to various stress factors, such as the ability to survive at low acidic pH values and in the presence of bile, made it possible to identify some promising isolates – Lactobacillus helveticus -13 (Lh-13) and Lactiplantibacillus plantarum – 5 (Lpl-5), for studying antimicrobial and biofilm-forming activity. The antimicrobial activity of Lh-13, Lpl-5 was closely studied. They have a certain level of antibacterial and fungicidal activities, which indicates their pronounced inhibition against indicator microorganisms. Using a laboratory robot, TecanEVolizer100 (Tecan), the optical density of Lh-13, Lpl-5 was studied in the wells of polystyrene plates, reflecting the intensity of biofilm formation along their surface. Using laser capture microdissection, the images of cell morphology in biofilm of Lh-13 isolates included in the matrix were obtained. The atomic force microscopy made it possible to study the two and three-dimensional morphological images of biofilm-forming isolates of Lh-13. [ABSTRACT FROM AUTHOR]

Published

2023

36. Localized proteomic differences in the choroid plexus of Alzheimer's disease and epilepsy patients

Author

Dominique F. Leitner, Evgeny Kanshin, Arline Faustin, Manon Thierry, Daniel Friedman, Sasha Devore, Beatrix Ueberheide, Orrin Devinsky, and Thomas Wisniewski

Subjects

Alzheimer's disease, epilepsy, choroid plexus, proteomics, laser capture microdissection, Neurology. Diseases of the nervous system, RC346-429

Abstract

IntroductionAlzheimer's disease (AD) and epilepsy are reciprocally related. Among sporadic AD patients, clinical seizures occur in 10–22% and subclinical epileptiform abnormalities occur in 22–54%. Cognitive deficits, especially short-term memory impairments, occur in most epilepsy patients. Common neurophysiological and molecular mechanisms occur in AD and epilepsy. The choroid plexus undergoes pathological changes in aging, AD, and epilepsy, including decreased CSF turnover, amyloid beta (Aβ), and tau accumulation due to impaired clearance and disrupted CSF amino acid homeostasis. This pathology may contribute to synaptic dysfunction in AD and epilepsy.MethodsWe evaluated control (n = 8), severe AD (n = 8; A3, B3, C3 neuropathology), and epilepsy autopsy cases (n = 12) using laser capture microdissection (LCM) followed by label-free quantitative mass spectrometry on the choroid plexus adjacent to the hippocampus at the lateral geniculate nucleus level.ResultsProteomics identified 2,459 proteins in the choroid plexus. At a 5% false discovery rate (FDR), 616 proteins were differentially expressed in AD vs. control, 1 protein in epilepsy vs. control, and 438 proteins in AD vs. epilepsy. There was more variability in the epilepsy group across syndromes. The top 20 signaling pathways associated with differentially expressed proteins in AD vs. control included cell metabolism pathways; activated fatty acid beta-oxidation (p = 2.00 x 10−7, z = 3.00), and inhibited glycolysis (p = 1.00 x 10−12, z = −3.46). For AD vs. epilepsy, the altered pathways included cell metabolism pathways, activated complement system (p = 5.62 x 10−5, z = 2.00), and pathogen-induced cytokine storm (p = 2.19 x 10−2, z = 3.61). Of the 617 altered proteins in AD and epilepsy vs. controls, 497 (81%) were positively correlated (p < 0.0001, R2 = 0.27).DiscussionWe found altered signaling pathways in the choroid plexus of severe AD cases and many correlated changes in the protein expression of cell metabolism pathways in AD and epilepsy cases. The shared molecular mechanisms should be investigated further to distinguish primary pathogenic changes from the secondary ones. These mechanisms could inform novel therapeutic strategies to prevent disease progression or restore normal function. A focus on dual-diagnosed AD/epilepsy cases, specific epilepsy syndromes, such as temporal lobe epilepsy, and changes across different severity levels in AD and epilepsy would add to our understanding.

Published

2023

37. Subclinical endometritis differentially affects the transcriptomic profiles of endometrial glandular, luminal, and stromal cells of postpartum dairy cows

Author

Gonçalo Pereira, Yongzhi Guo, Elisabete Silva, Marta Filipa Silva, Claudia Bevilacqua, Gilles Charpigny, Luís Lopes-da-Costa, and Patrice Humblot

Subjects

endometrium, subclinical endometritis, laser capture microdissection, transcriptome, Dairy processing. Dairy products, SF250.5-275, Dairying, SF221-250

Abstract

ABSTRACT: In postpartum dairy cows, subclinical endometritis (SCE) is characterized by persistent endometrial inflammation, which has profound detrimental effects on subsequent reproductive performance. To date, transcriptomic studies related to this condition were either based on biopsy-derived whole-endometrium tissue or endometrial swab or cytobrush samples, thus masking effects of disease on cell type–specific gene expression. This study tested the hypothesis that different endometrial health statuses are associated with distinct transcription profiles of endometrial stromal, glandular, and luminal epithelial cells. At 44 d postpartum (DPP), endometrial biopsies were taken from dairy cows (n = 24) classified as healthy, recovered from SCE, or affected by persistent SCE, according to endometrial cytology taken at 21 and 44 DPP. Stromal, glandular, and luminal epithelial cells were isolated from the whole-tissue biopsy by laser capture microdissection, and the cell-specific transcription profiles were determined by RNA sequencing. Differential gene expression was analyzed with DESeq2 (https://bioconductor.org/packages/release/bioc/html/DESeq2.html). Results demonstrated that global transcriptomic profiles and corresponding lists of differentially expressed genes between cows with different health statuses were distinct among cell types. Results also showed that although healthy and recovered cows presented similar endometrial clinically healthy phenotypes at 44 DPP, the prior presence of immune cells still affected the transcriptome of endometrial cells at this stage, delaying complete functional recovery. Recovery or persistence of inflammation was associated with gene expression patterns involved not only in immune function but also in tissue remodeling, cell adhesion, and uterine receptivity in a cell type–specific manner. Identifying these signatures may contribute to the development of novel diagnostic tools and therapeutic strategies. In addition, these results may help to define preventive measures or ways to stimulate recovery from endometrial inflammation, thus helping to restore the fertility of postpartum dairy cows.

Published

2022

38. Global-feature of autoimmune glomerulonephritis using proteomic analysis of laser capture microdissected glomeruli

Author

Jingjing Dong, Fengping Zheng, Fanna Liu, Jingquan He, Shanshan Li, Wenjun Pu, Huixuan Xu, Zhifeng Luo, Shizhen Liu, Lianghong Yin, Donge Tang, and Yong Dai

Subjects

autoimmune glomerulonephritis, proteomic, laser capture microdissection, complement components, IgA nephropathy, lupus nephritis, Immunologic diseases. Allergy, RC581-607

Abstract

BackgroundIgA nephropathy (IgAN), (LN), membranous nephropathy (MN), and minimal change nephropathy (MCN) are all belonged to autoimmune glomerulonephritis. This study aimed to identify the specific proteomic characteristics of the four GNs diseases in order to provide frameworks for developing the appropriate drug for patients diagnosed with GNs disease.MethodsLiquid chromatography−tandem mass spectrometry (LC-MS/MS) was utilized to investigate proteomic features of glomerular tissues obtained by laser capture microdissection (LCM). 8 normal control cases, 11 IgAN cases, 19 LN cases, 5 MN cases, and 3 MCN cases in this study were selected for bioinformatics analyses.ResultsThe shared overlapping proteins among the top 100 DEPs of each GNs type were mostly downregulated, in which only FLII was significantly downregulated in the four GNs diseases. A2M was significantly upregulated in MN, IgAN, and LN subgroups. The pathway of complement and coagulation cascades was notably activated with NES value ranging 2.77 to 3.39 among MCN, MN, IgAN, and LN diseases, but the pattern of protein expression level were significantly different. In LN patients, the increased activity of complement and coagulation cascades was contributed by the high expression of multiple complements (C1QB, C3, C4A, C4B, C6, C8B, C8G, C9). Meanwhile, both C1QC and C4B were remarkably upregulated in MN patients. On the contrary, complement-regulating proteins (CD59) was substantially decreased in MCN and IgAN subgroup.ConclusionsThe integrative proteomics analysis of the four GNs diseases provide insights into unique characteristics of GNs diseases and further serve as frameworks for precision medicine diagnosis and provide novel targets for drug development.

Published

2023

39. Time‐resolved transcriptomics of mouse gastric pit cells during postnatal development reveals features distinct from whole stomach development.

Author

Wei, Ying, Xu, Zeqian, Hu, Miaomiao, Wu, Zhongqin, Liu, Axian, Czajkowsky, Daniel M., Guo, Yan, and Shao, Zhifeng

Subjects

*STOMACH, *MICE, *TRANSCRIPTOMES, *MICRODISSECTION, *PHENOTYPES

Abstract

Whole‐organ transcriptomic analyses have emerged as a common method for characterizing developmental transitions in mammalian organs. However, it is unclear if all cell types in an organ follow the whole‐organ defined developmental trajectory. Recently, a postnatal two‐stage developmental process was described for the mouse stomach. Here, using laser capture microdissection to obtain in situ transcriptomic data, we show that mouse gastric pit cells exhibit four postnatal developmental stages. Interestingly, early stages are characterized by the up‐regulation of genes associated with metabolism, a functionality not typically associated with pit cells. Hence, beyond revealing that not all constituent cells develop according to the whole‐organ determined pathway, these results broaden our understanding of the pit cell phenotypic landscape during stomach development. [ABSTRACT FROM AUTHOR]

Published

2023

40. Evaluation Of Radiopacity of Nanoparticle Incorporated Root Canal Sealer with Epoxy Resin Incorporated Root Canal Sealers - An Invitro Study.

Author

Shetty, Chitharanjan, Shetty, Aditya, Kini, Sudarshan, Shetty, Veena, and Dsouza, Neevan

Subjects

*PIT & fissure sealants (Dentistry), *RADIOPACITY, *EPOXY resins, *NANOPARTICLES, *OPACITY (Optics)

Abstract

Aim: of this study was to assess and compare, the radiopacity of nanoparticle-based (NPB) root canal sealers with Epoxy Resin Based(ERB) root canal sealer using an aluminium step wedge in accordance with ISO 6876/2012 standards. Materials and methods: The specimens, which were made of each sealer material, had a 10mm diameter and a 1mm thickness. The creation of metallic matrices, which were used in the fabrication of the impressions, was done using a light-bodied silicone-based impression medium. Using an aluminium step-wedge, the radiopacity of the NPB sealer and the ERB sealer was assessed in accordance with international standards. The optical density was measured using a sample of enamel, dentin, and aluminium of the appropriate thickness, all measuring 1 mm thick. Results: The radiopacity of the ERB sealer was 2.37, with a minimum value of 179 and a maximum value of 215. The radiopacity value for the NPB sealer was 3.47, with a minimum value of 185 and a maximum value of 255. Conclusion: Within the limits of the study, the NPB root canal sealers has better radiopacity than the ERB sealers. It has radiopacity values of the sealers are within the ADA/ISO recommendations. Clinical Significance: The radiopacity of the NPB sealer can be compared with other commercially available sealers for in vivo applications. [ABSTRACT FROM AUTHOR]

Published

2023

41. Laser Capture Microdissection - A Breakthrough Technology in Head and Neck Diagnostics.

Author

Mishra, Pallavi, Panda, Abikshyeet, Bhuyan, Lipsa, Bhattacharyya, Arnab, Bajoria, Atul Anand, and Sahoo, Sanjay Kumar

Subjects

*MICRODISSECTION, *LASERS, *LASER pulses, *NECK, *CELL populations

Abstract

Laser capture microdissection (LCM) is a technique in which, from a heterogenous tissue specimen some pure cell populations are isolated. This procedure can capture and target the desired number of cells that are required. A low energy laser pulse is used in this technique. Apart from systemic applications LCM can also be applied in the field of dentistry and pathology. [ABSTRACT FROM AUTHOR]

Published

2023

42. Regulation of Prepro-NeuropeptideW/B and Its Receptor in the Heart of ZDF Rats: An Animal Model of Type II DM.

Author

Pandey, Shashank, Jarkovska, Dagmar, Tuma, Zdenek, Smrhova, Tereza, and Chottova Dvorakova, Magdalena

Subjects

*HEART, *TYPE 2 diabetes, *G protein coupled receptors, *AUTONOMIC nervous system, *ANIMAL models in research, *CORONARY arteries, *GENE expression

Abstract

Neuropeptide B (NPB) and neuropeptide W (NPW) are neuropeptides, which constitute NPB/W signaling systems together with G-protein coupled receptors NPBWR1. The location and function of NPB/W signaling systems have been predominantly detected and mapped within the CNS, including their role in the modulation of inflammatory pain, neuroendocrine functions, and autonomic nervous systems. The aim of the study is to investigate the impact of diabetes on the neuropeptide B/W signaling system in different heart compartments and neurons which innervates it. In the RT-qPCR analysis, we observed the upregulation of mRNA for preproNPB in RV, for preproNPW in LA, and for NPBWR1 in DRG in diabetic rats. On the contrary, the expression of mRNA for NPBWR1 was downregulated in LV in diabetic rats. In the WB analysis, significant downregulation of NPBWR1 in LV (0.54-fold, p = 0.046) in diabetic rats was observed at the proteomic level. The presence of NPBWR1 was also confirmed in a dissected LCM section of cardiomyocytes and coronary arteries. The positive inotropic effect of NPW described on the diabetic cardiomyocytes in vitro could point to a possible therapeutic target for compensation of the contractile dysfunction in the diabetic heart. In conclusion, the NPB/W signaling system is involved in the regulation of heart functions and long-term diabetes leads to changes in the expression of individual members of this signaling system differently in each cardiac compartment, which is related to the different morphology and function of these cardiac chambers. [ABSTRACT FROM AUTHOR]

Published

2022

43. An optimized workflow for transcriptomic analysis from archival paraformaldehyde-fixed retinal tissues collected by laser capture microdissection.

Author

Takahashi, Kei, Beltran, William A., and Sudharsan, Raghavi

Subjects

*RNA sequencing, *TRANSCRIPTOMES, *TISSUE fixation (Histology), *POLYOXYMETHYLENE, *RNA

Abstract

RNA sequencing (RNA-seq) coupled with laser capture microdissection (LCM) is a powerful tool for transcriptomic analysis in unfixed fresh-frozen tissues. Fixation of ocular tissues for immunohistochemistry commonly involves the use of paraformaldehyde (PFA) followed by embedding in Optimal Cutting Temperature (OCT) medium for long-term cryopreservation. However, the quality of RNA derived from such archival PFA-fixed/OCT-embedded samples is often compromised, limiting its suitability for transcriptomic studies. In this study, we aimed to develop a methodology to extract high-quality RNA from PFA-fixed canine eyes by utilizing LCM to isolate retinal tissue. We demonstrate the efficacy of an optimized LCM and RNA purification protocol for transcriptomic profiling of PFA-fixed retinal specimens. We compared four pairs of canine retinal tissues, where one eye was subjected to PFA-fixation prior to OCT embedding, while the contralateral eye was embedded fresh frozen (FF) in OCT without fixation. Since the RNA obtained from PFA-fixed retinas were contaminated with genomic DNA, we employed two rounds of DNase I treatment to obtain RNA suitable for RNA-seq. Notably, the quality of sequencing reads and gene sets identified from both PFA-fixed and FF tissues were nearly identical. In summary, our study introduces an optimized workflow for transcriptomic profiling from PFA-fixed archival retina. This refined methodology paves the way for improved transcriptomic analysis of preserved ocular tissue, bridging the gap between optimal sample preservation and high-quality RNA data acquisition. [ABSTRACT FROM AUTHOR]

Published

2024

44. Insight into the Molecular Characteristics of Langhans Giant Cell by Combination of Laser Capture Microdissection and RNA Sequencing

Author

Chen Y, Jiang H, Xiong J, Shang J, Chen Z, Wu A, and Wang H

Subjects

langhans giant cell, transcriptome analysis, laser capture microdissection, molecular characteristics, ccl7., Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950

Abstract

Yanqing Chen,1 Haiqin Jiang,1 Jingshu Xiong,1 Jingzhe Shang,2,3 Zhiming Chen,1 Aiping Wu,2,3 Hongsheng Wang1 1Jiangsu Key Laboratory of Molecular Biology for Skin Diseases and STIs, Institute of Dermatology, Chinese Academy of Medical Sciences and Peking Union Medical College, Nanjing, People’s Republic of China; 2Center for Systems Medicine, Institute of Basic Medical Sciences, Chinese Academy of Medical Sciences and Peking Union Medical College, Suzhou, People’s Republic of China; 3Center of Systems Medicine, Suzhou Institute of Systems Medicine, Suzhou, People’s Republic of ChinaCorrespondence: Hongsheng Wang; Haiqin JiangJiangsu Key Laboratory of Molecular Biology for Skin Diseases and STIs, Institute of Dermatology, Chinese Academy of Medical Sciences and Peking Union Medical College, No. 12, St Jiangwangmiao, Nanjing, 210042, Jiangsu, People’s Republic of China, Tel +86-25-85478953, Fax +86-25-85478944, Email whs33@vip.sina.com; hq_j1985@126.comPurpose: The presence of Langhans giant cell (LGC) is a hallmark of mycobacterium-induced granuloma. The molecular characteristics and functions of LGC remain unclear to date. The study aimed to systematically characterize the molecular characteristics of LGC and reveal the potential functions.Methods: Human LGCs were purified through laser capture microdissection (LCM) in vitro. RNA sequencing and in-depth transcriptome analysis were performed for purified LGCs and macrophages in the same system. Skin samples from mycobacterial infection patients were used to confirm some of the transcriptional expression.Results: Human LGCs have different expression pattern from macrophages in the same in vitro system. A total of 967 differentially expressed genes were found. Bioinformatics analysis showed that LGCs are is characterized by active cell shape regulation, increased cytoskeletal components, weakened energy metabolism level, and reduced immune response. CCL7 may be a specific molecular for LGC to communicate with CCR1-expression cells in granuloma.Conclusion: LGCs have unique molecular characteristics different from that of macrophages. They may play a role in maintaining the hemostasis in granuloma.Keywords: langhans giant cell, transcriptome analysis, laser capture microdissection, molecular characteristics, CCL7

Published

2022

45. Transcriptome–pathology correlation identifies interplay between TDP-43 and the expression of its kinase CK1E in sporadic ALS

Author

Krach, Florian, Batra, Ranjan, Wheeler, Emily C, Vu, Anthony Q, Wang, Ruth, Hutt, Kasey, Rabin, Stuart J, Baughn, Michael W, Libby, Ryan T, Diaz-Garcia, Sandra, Stauffer, Jennifer, Pirie, Elaine, Saberi, Shahram, Rodriguez, Maria, Madrigal, Assael A, Kohl, Zacharias, Winner, Beate, Yeo, Gene W, and Ravits, John

Subjects

Neurodegenerative, Neurosciences, Clinical Research, Orphan Drug, Genetics, Human Genome, ALS, Brain Disorders, Biotechnology, Rare Diseases, Aetiology, 2.1 Biological and endogenous factors, Neurological, Aged, Aged, 80 and over, Amyotrophic Lateral Sclerosis, Casein Kinase I, DNA-Binding Proteins, Female, Humans, Male, Middle Aged, Motor Neurons, Phosphorylation, Spinal Cord, Transcriptome, Neurodegeneration, Laser capture microdissection, RNA-seq, RNA, Gene-expression, TDP-43, Casein kinase, Motor neuron, Sporadic disease, Clinical Sciences, Neurology & Neurosurgery

Abstract

Sporadic amyotrophic lateral sclerosis (sALS) is the most common form of ALS, however, the molecular mechanisms underlying cellular damage and motor neuron degeneration remain elusive. To identify molecular signatures of sALS we performed genome-wide expression profiling in laser capture microdissection-enriched surviving motor neurons (MNs) from lumbar spinal cords of sALS patients with rostral onset and caudal progression. After correcting for immunological background, we discover a highly specific gene expression signature for sALS that is associated with phosphorylated TDP-43 (pTDP-43) pathology. Transcriptome-pathology correlation identified casein kinase 1ε (CSNK1E) mRNA as tightly correlated to levels of pTDP-43 in sALS patients. Enhanced crosslinking and immunoprecipitation in human sALS patient- and healthy control-derived frontal cortex, revealed that TDP-43 binds directly to and regulates the expression of CSNK1E mRNA. Additionally, we were able to show that pTDP-43 itself binds RNA. CK1E, the protein product of CSNK1E, in turn interacts with TDP-43 and promotes cytoplasmic accumulation of pTDP-43 in human stem-cell-derived MNs. Pathological TDP-43 phosphorylation is therefore, reciprocally regulated by CK1E activity and TDP-43 RNA binding. Our framework of transcriptome-pathology correlations identifies candidate genes with relevance to novel mechanisms of neurodegeneration.

Published

2018

46. Combine Phage Antibody Display Library Selection on Patient Tissue Specimens with Laser Capture Microdissection to Identify Novel Human Antibodies Targeting Clinically Relevant Tumor Antigens

Author

Su, Yang, Bidlingmaier, Scott, Lee, Nam-Kyung, and Liu, Bin

Subjects

Biochemistry and Cell Biology, Biological Sciences, Cancer, Human Genome, Biotechnology, Genetics, Aetiology, 2.1 Biological and endogenous factors, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Antibodies, Neoplasm, Antigens, Neoplasm, Cloning, Molecular, Gene Library, Humans, Laser Capture Microdissection, Neoplasms, Peptide Library, Single-Chain Antibodies, Human cancer specimen, Internalizing human monoclonal antibody, Intracellular payload delivery, Laser capture microdissection, Macropinocytosis, Natural cell surface epitope, Phage antibody library, Solid tumor, Targeted therapy, Tissue microenvironment, Other Chemical Sciences, Developmental Biology, Biochemistry and cell biology, Medicinal and biomolecular chemistry

Abstract

A functional approach to generate tumor-targeting human monoclonal antibodies is through selection of phage antibody display libraries directly on tumor cells. Although technically convenient, the use of cancer cell lines for the selection has limitations as those cell lines often undergo genetic and epigenetic changes during prolonged in vitro culture and alter their cell surface antigen expression profile. The key is to develop a technology that allows selection of phage antibody display libraries on tumor cells in situ residing in their natural tissue microenvironment. Laser capture microdissection (LCM) permits the precise procurement of tumor cells from human cancer patient tissue sections. Here, we describe a LCM-based method for selecting phage antibodies against tumor cells in situ using both fresh frozen and paraffin-embedded tissues. To restrict the selection to antibodies that bind internalizing epitopes, the method utilizes a polyclonal phage population pre-enriched for internalizing phage antibodies. The ability to recognize tumor cells in situ residing in their natural tissue microenvironment and to deliver payload intracellularly makes these LCM-selected antibodies attractive candidates for the development of targeted cancer therapeutics.

Published

2018

47. Altered microbial biogeography in an innate model of colitis

Author

Antonia Boger-May, Theodore Reed, Diana LaTorre, Katelyn Ruley-Haase, Hunter Hoffman, Lauren English, Connor Roncagli, Anne-Marie Overstreet, and David Boone

Subjects

A20, laser capture microdissection, TRAG, microbiome, innate immunity, biogeography, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Changes in the spatial organization, or biogeography, of colonic microbes have been observed in human inflammatory bowel disease (IBD) and mouse models of IBD. We have developed a mouse model of IBD that occurs spontaneously and consistently in the absence of adaptive immunity. Mice expressing tumor necrosis factor-induced protein 3 (TNFAIP3) in intestinal epithelial cells (villin-TNFAIP3) develop colitis when interbred with Recombination Activating 1-deficient mice (RAG1−/−). The colitis in villin-TNFAIP3 × RAG1−/− (TRAG) mice is prevented by antibiotics, indicating a role for microbes in this innate colitis. We therefore explored the biogeography of microbes and responses to antibiotics in TRAG colitis. Laser capture microdissection and 16S rRNA sequencing revealed altered microbial populations across the transverse axis of the colon as the inner mucus layer of TRAG, but not RAG1−/−, mice was infiltrated by microbes, which included increased abundance of the classes Gammaproteobacteria and Actinobacteria. Along the longitudinal axis differences in the efficacy of antibiotics to prevent colitis were evident. Neomycin was most effective for prevention of inflammation in the cecum, while ampicillin was most effective in the proximal and distal colon. RAG1−/−, but not TRAG, mice exhibited a structured pattern of bacterial abundance with decreased Firmicutes and Proteobacteria but increased Bacteroidetes along the proximal to distal axis of the gut. TRAG mice exhibited increased relative abundance of potential pathobionts including Bifidobacterium animalis along the longitudinal axis of the gut whereas others, like Helicobacter hepaticus were increased only in the cecum. Potential beneficial organisms including Roseburia were decreased in the proximal regions of the TRAG colon, while Bifidobacterium pseudolongulum was decreased in the TRAG distal colon. Thus, the innate immune system maintains a structured, spatially organized, gut microbiome along the transverse and longitudinal axis of the gut, and disruption of this biogeography is a feature of innate immune colitis.

Published

2022

48. Somatic copy number variant load in neurons of healthy controls and Alzheimer's disease patients.

Author

Turan, Zeliha Gözde, Richter, Vincent, Bochmann, Jana, Parvizi, Poorya, Yapar, Etka, Işıldak, Ulas, Waterholter, Sarah-Kristin, Leclere-Turbant, Sabrina, Son, Çağdaş Devrim, Duyckaerts, Charles, Yet, İdil, Arendt, Thomas, Somel, Mehmet, and Ueberham, Uwe

Subjects

*ENTORHINAL cortex, *DNA copy number variations, *ALZHEIMER'S patients, *PYRAMIDAL neurons, *NEURONS, *TEMPORAL lobe

Abstract

The possible role of somatic copy number variations (CNVs) in Alzheimer's disease (AD) aetiology has been controversial. Although cytogenetic studies suggested increased CNV loads in AD brains, a recent single-cell whole-genome sequencing (scWGS) experiment, studying frontal cortex brain samples, found no such evidence. Here we readdressed this issue using low-coverage scWGS on pyramidal neurons dissected via both laser capture microdissection (LCM) and fluorescence activated cell sorting (FACS) across five brain regions: entorhinal cortex, temporal cortex, hippocampal CA1, hippocampal CA3, and the cerebellum. Among reliably detected somatic CNVs identified in 1301 cells obtained from the brains of 13 AD patients and 7 healthy controls, deletions were more frequent compared to duplications. Interestingly, we observed slightly higher frequencies of CNV events in cells from AD compared to similar numbers of cells from controls (4.1% vs. 1.4%, or 0.9% vs. 0.7%, using different filtering approaches), although the differences were not statistically significant. On the technical aspects, we observed that LCM-isolated cells show higher within-cell read depth variation compared to cells isolated with FACS. To reduce within-cell read depth variation, we proposed a principal component analysis-based denoising approach that significantly improves signal-to-noise ratios. Lastly, we showed that LCM-isolated neurons in AD harbour slightly more read depth variability than neurons of controls, which might be related to the reported hyperploid profiles of some AD-affected neurons. [ABSTRACT FROM AUTHOR]

Published

2022

49. Multiomic Analyses of Dopaminergic Neurons Isolated from Human Substantia Nigra in Parkinson's Disease: A Descriptive and Exploratory Study.

Author

Zaccaria, Affif, Antinori, Paola, Licker, Virginie, Kövari, Enikö, Lobrinus, Johannes A., and Burkhard, Pierre R.

Subjects

*PARKINSON'S disease, *SUBSTANTIA nigra, *DOPAMINERGIC neurons, *NEURON analysis, *RNA, *ALDEHYDE dehydrogenase, *CYSTATIN C

Abstract

Dopaminergic neurons (DA) of the substantia nigra pars compacta (SNpc) selectively and progressively degenerate in Parkinson's disease (PD). Until now, molecular analyses of DA in PD have been limited to genomic or transcriptomic approaches, whereas, to the best of our knowledge, no proteomic or combined multiomic study examining the protein profile of these neurons is currently available. In this exploratory study, we used laser capture microdissection to extract regions from DA in 10 human SNpc obtained at autopsy in PD patients and control subjects. Extracted RNA and proteins were identified by RNA sequencing and nanoliquid chromatography–mass spectrometry, respectively, and the differential expression between PD and control group was assessed. Qualitative analyses confirmed that the microdissection protocol preserves the integrity of our samples and offers access to specific molecular pathways. This multiomic analysis highlighted differential expression of 52 genes and 33 proteins, including molecules of interest already known to be dysregulated in PD, such as LRP2, PNMT, CXCR4, MAOA and CBLN1 genes, or the Aldehyde dehydrogenase 1 protein. On the other hand, despite the same samples were used for both analyses, correlation between RNA and protein expression was low, as exemplified by the CST3 gene encoding for the cystatin C protein. This is the first exploratory study analyzing both gene and protein expression of laser-dissected neuronal parts from SNpc in PD. Data are available via ProteomeXchange with identifier PXD024748 and via GEO with identifier GSE 169755. [ABSTRACT FROM AUTHOR]

Published

2022

50. Profiling cell-type specific gene expression in post-mortem human brain samples through laser capture microdissection.

Author

Almeida, Daniel and Turecki, Gustavo

Subjects

*GENE expression profiling, *GENE expression, *MICRODISSECTION, *LASERS, *BRAIN diseases

Abstract

• Cell-type-specific enrichment strategies are crucial for tackling the downstream effects of tissue heterogeneity in transcriptomic analyses. • Laser capture microdissection allows for the capture of specific cell types based on size, morphology and/or presence of a specific marker. • Laser capture microdissection has been combined with a wide array of molecular techniques for studying gene expression, including RNA-sequencing. The transcriptome of a cell constitutes an essential piece of cellular identity and contributes to the multifaceted complexity and heterogeneity of cell-types within the mammalian brain. Thus, while a wealth of studies have investigated transcriptomic alterations underlying the pathophysiology of diseases of the brain, their use of bulk-tissue homogenates makes it difficult to tease apart whether observed differences are explained by disease state or cellular composition. Cell-type-specific enrichment strategies are, therefore, crucial in the context of gene expression profiling. Laser capture microdissection (LCM) is one such strategy that allows for the capture of specific cell-types, or regions of interest, under microscopic visualization. In this review, we focus on using LCM for cell-type specific gene expression profiling in post-mortem human brain samples. We begin with a discussion of various LCM systems, followed by a walk-through of each step in the LCM to gene expression profiling workflow and a description of some of the limitations associated with LCM. Throughout the review, we highlight important considerations when using LCM with post-mortem human brain samples. Whenever applicable, commercially available kits that have proven successful in the context of LCM with post-mortem human brain samples are described. [ABSTRACT FROM AUTHOR]

Published

2022