Multivariate analysis of leaf tissue morphogenesis

Samuel Belteton (3322188)

10 May 2020

Leaf size and shape are strongly influenced by the growth patterns of the epidermal tissue. Pavement cells are the prevalent cell type in the epidermis and during cell expansion they undergo a drastic shape change from a simple polyhedral cells to puzzled-shaped cell. The role of these cell protrusions, more commonly referred to as lobes, remains unknown but their formation has been proposed to help increase the structural integrity of the epidermal tissue. How the symmetry breaking event that initiates a lobe is controlled remains unknown, however pharmacological and genetic disruption of the microtubule system has been shown to interfere not only with lobe initiation but also with lobe expansion. Additionally, the role of microtubules in the pattering of microfibril deposition, the load-bearing structure of the cell wall, makes the microtubule system a good candidate to evaluate its dynamics as a function of shape change. Two main mechanical models for lobe initiation are evaluated here, one where microtubules serve as stable features suppressing local expansion and one where microtubules, similarly to the anisotropic expansion patterning in hypocotyl cells, pro-mote the local anisotropic expansion of the cell resulting in lobe formation. The main method to evaluate these models was through the use of long-term time-lapse image analysis using a plasma-membrane marker for accurate shape change quantification and a microtubule marker to quantify their location, persistence, and density as a function of cell shape change. Using the junctions where three cells come together,cells were sub-divided into segments and the shape of these segments were tracked using a new coordinate system that allowed the detection of new lobes as which can arise from ∼300 deflections. By mapping sub-cellular processes, such as microtubule persistence, to this coordinate system, correlations of microtubule organization and shape change was possible. Additionally, a subset of microtubules bundles that splay across the anticlinal and periclinal walls, perpendicular and parallel to the leaf surface respectively, were identified as marking the location and direction of lobe formation.Disrupting the cell boundary by partially digesting pectin, a main component in the middle lamella, revealed the cell-autonomous morphogenesis mechanism in pavementcells. Under pectinase treatment, cell invaginations were produced and similarly to lobes their initiation was microtubule and cellulose dependent. Lastly, stress prediction using finite-element models, based from live-cell images, co-localized regions of high cell wall stress with both microtubule persistence and shape shape locations in both lobing and invaginated segments. Together, a model of cellular shape change is presented where microtubules translate cell wall stresses to tissue morphogenesis.

Botany

Leaf tissue morphogenesis

Effects of Peripheral Nerve Injury on the Cells of the Dorsal Root Ganglion: a Role for Primary Cilia

Smith, Sarah K.

12 1900

Primary cilia are ubiquitous sensory organelles found on most cell types including cells of the dorsal root ganglia (DRG). The DRG are groups of peripheral neurons that relay sensory information from the periphery to the CNS. Other cell types in the DRG include a type of glial cell, the satellite glial cells (SGCs). The SGCs surround the DRG neurons and, with the neurons, form functional sensory units. Currently are no reports describing the numbers of DRG cells that have cilia. We found that 26% of the SGCs had primary cilia. The incidence of cilia on neurons varied with neuron size, a property that roughly correlates with physiological characteristics. We found that 29% of the small, 16% of the medium and 5% of the large neurons had primary cilia. Primary cilia have been shown to have a role in cell proliferation in a variety of cell types. In some of the cells the cilia mediate the proliferative effects of Sonic hedgehog (Shh). In the CNS, Shh signaling through primary cilia affects proliferation during development as well as following injury, but no studies have looked at this function in the PNS. The SGCs and neurons of the DRG undergo complex changes following peripheral nerve injury such as axotomy. One marked change seen after axotomy is SGC proliferation and at later stages, neuronal death. We found that following axotomy there is a significant increase in the percentage of SGCs with primary cilia. We also found a significant increase in the percentage of medium-sized neurons with primary cilia. In other experiments we tested the idea that Shh plays a role in SGC proliferation. When Shh signaling was blocked following axotomy we found decreased proliferation of SGCs. This is the first report of a change in the percentage of cells with cilia following injury in the PNS, and the first report of a role for Shh in SGC proliferation following axotomy.

Peripheral nervous system

primary cilia

satellite glial cells

proliferation

Identifikation av proteinmarkörer för cellulär proliferation / Identification of protein markers for cellular proliferation using a cell model for malignant transformation

Åkesson, Lovisa

January 2015

No description available.

biomarker

microscopy

antibodies

proliferation

immunofluorescence

Engineering and Technology

Teknik och teknologier

Komparace postupu americké administrativy vůči Íránu v otázce proliferace jaderných zbraní za vlád prezidentů Bushe a Obamy / US Foreign Policy towards Iran: A Comparison of presidents Bush and Obama

Čermák, Michal

January 2013

The topic of the diploma thesis is a comparison of the American activities during the presidencies of George W. Bush and Barack Obama towards Iran, in regard to the threat of nuclear weapons proliferation. It observes the diplomatic actions in relation to Iran and other actors, who play an important role in this issue, and also some other methods, used by the world's leading superpower to prevent Iran from the development of nuclear weapons. The mentioned topic is situated into the broader context of continuity and change in the US security and foreign policy. The objective of the diploma thesis is to assess what where the differences in the US actions under Obama's administration, compared with the actions during the presidency of his predecessor, as well as how the Obama's administration followed them, and to assess how effective these actions were.

HSPA12B: A Novel Facilitator of Lung Tumor Growth

Ma, He, Lu, Ting, Zhang, Xiaojin, Li, Chuanfu, Xiong, Jingwei, Huang, Lei, Liu, Ping, Li, Yuehua, Liu, Li, Ding, Zhengnian

01 January 2015

Lung tumor progression is regulated by proangiogenic factors. Heat shock protein A12B (HSPA12B) is a recently identified regulator of expression of proangiogenic factors. However, whether HSPA12B plays a role in lung tumor growth is unknown. To address this question, transgenic mice overexpressing HSPA12B (Tg) and wildtype littermates (WT) were implanted with Lewis lung cancer cells to induce lung tumorigenesis. Tg mice showed significantly higher number and bigger size of tumors than WT mice. Tg tumors exhibited increased angiogenesis and proliferation while reduced apoptosis compared with WT tumors. Interestingly, a significantly enhanced upregulation of Cox-2 was detected in Tg tumors than in WT tumors. Also, Tg tumors demonstrated upregulation of VEGF and angiopoietin-1, downregulation of AKAP12, and increased eNOS phosphorylation compared with WT tumors. Celecoxib, a selective Cox-2 inhibitor, suppressed the HSPA12B-induced increase in lung tumor burden. Moreover, celecoxib decreased angiogenesis and proliferation whereas increased apoptosis in Tg tumors. Additionally, celecoxib reduced angiopoietin-1 expression and eNOS phosphorylation but increased AKAP12 levels in Tg tumors. Our results indicate that HSPA12B stimulates lung tumor growth via a Cox-2-dependent mechanism. The present study identified HSPA12B as a novel facilitator of lung tumor growth and a potential therapeutic target for the treatment of lung cancer.

angiogenesis

apoptosis

heat shock protein A12B

lung cancer

proliferation

Surgery

Effects of Phytohemagglutinin-P (PHA-P) on Bone of the Growing Rat

Wang, T. M., Jee, W. S.S., Woodbury, L. A., Matthews, J. L.

01 January 1982

The effects of phytohemagglutinin-P, (PHA-P), a mitogen known to selectively stimulate cells of hematogenous or lymphoid monocytic origin, 25 and 50 mg/kg/day administered for 15 days on proximal tibiae of growing male Sprague-Dawley rats, were studied. The general effect of PHA-P was to decrease the amount of cartilage, hard tissue, and longtitudinal growth in the proximal tibial metaphysis. A decrease in longitudinal bone growth, in the number of chondrocytes, in the thickness of cartilage plate, in the metaphyseal mass of hard tissue, in the percentage of calcified cartilage core, and in the number of osteoblasts per mm of bone surface was observed. Additionally, PHA-P increased the number of osteoclasts, the number of labeled osteoclastic nuclei, and the average number of nuclei per osteoclast. There was a significant decrease in the time to the first appearance of labeled osteoclastic nuclei as the dose of PHA-P increased. Thus, PHA-P treatment leads to the dominance of osteoclastic over chondroblastic and osteoblastic activity and results in a hard tissue deficit in a growing skeleton. The data indicate that PHA-P administration selectively increases osteoclast numbers by elevating osteoclastic progenitor cell proliferation and enhancing their fusion and differentiation to osteoclasts.

bone

differentiation

osteoclasts

phytohemagglutinin-P (PHA-P)

proliferation

Cell Proliferation and Hepatocarcinogenesis in Rat Initiated by Diethylnitrosamine and Promoted by Phenobarbital: Potential Roles of Early DNA Damage and Liver Metallothionein Expression

Chakraborty, Tridib, Chatterjee, Amrita, Rana, Ajay, Srivastawa, Sunil, Damodaran, Suresh, Chatterjee, Malay

19 July 2007

Cell proliferation plays an important role in multistage chemical carcinogenesis. Again, several reports demonstrated that upregulation of metallothionein (MT) expression is associated with increased cell proliferation that may contribute to the pathogenesis of preneoplastic phenotype to frank malignancy. In this study, we evaluated the roles of early DNA damage, altered expressions of liver MT and Ki-67 nuclear antigen, and altered hepatic levels of zinc (Zn) and copper (Cu) on cell proliferation and the progression of hepatocarcinogenesis through premalignant, late premalignant and malignant transformation phases in male Sprague-Dawley rats. We have further studied the association between MT expression and cell proliferation in hepatocarcinogenesis. There was substantial induction of DNA single-strand breaks (SSBs) (P < 0.001) and development of hepatocellular premalignant lesions along with significant decrease in hepatic levels of Zn and increase in Cu content following a single, necrogenic, intraperitoneal (i.p.) injection (200 mg/Kg body weight) of diethylnitrosamine (DEN) at week 4 of the experimental protocol. Moreover, DEN + phenobarbital (PB)-treatment significantly elevated MT-, Ki-67-, and BrdU-immunoexpressions along with their immunolabeling indices. Furthermore, positive correlations between MT- and Ki-67- labeling (P = 0.0006) at various time intervals, as well as, between MT immunoreactivity and 5'-bromo-2'-deoxyuridine-labeling index (BrdU-LI) (P = 0.0007) indicate that, MT expression might be associated with Ki-67 expression and cell proliferation thereby. The study suggests that DEN treatment may lead to alteration of Zn and Cu levels resulting in early DNA damage along with elevation of MT expression that may ultimately lead to hepatic cell proliferation. The results thus provide evidence in support of the role of MT as a potential positive regulator of cell growth during the early stages of hepatocellular transformation in rats.

cell proliferation

diethylnitrosamine

DNA-strand breaks

hepatocarcinogenesis

Ki-67

metallothionein

Le récepteur Sigma 1 : implication dans la prolifération et la stéatose des hépatocytes / Sigma 1 Receptor : Role in Hepatocyte Proliferation and Steatosis

Villemain Le Hagre, Laure

29 October 2019

Le récepteur Sigma 1 (SigR1) est une protéine transmembranaire du RE, enrichie dans les MAMs, qui agirait comme une chaperonne. Ubiquitaire, SigR1 est très exprimé dans le système nerveux central (SNC) et le foie. Dans le SNC, SigR1 est impliqué dans un grand nombre de maladies neurodégénératives mais aussi dans le mécanisme de la douleur et dans la dépression. SigR1 est aussi impliqué dans les cancers. Il est surexprimé dans de nombreuses tumeurs cancéreuses et particulièrement dans les tumeurs hormonodépendantes dans lesquelles son expression est corrélée au statut hormonal de la tumeur. Malgré sa très forte expression dans le foie, son rôle y est inconnu. Dans l’objectif de déterminer le rôle de SigR1 dans le foie nous étudions son expression dans les différents types de tumeurs hépatiques. SigR1 est significativement surexprimé dans les adénomes hépatocellulaires (HCA) et particulièrement le sous-type muté pour le gène HNF1α, les H-HCA. Les H-HCA sont des tumeurs hépatiques bénignes stéatosées majoritairement observées chez des femmes jeunes prenant des contraceptifs oraux (œstrogènes). Quelles sont les causes et les conséquences de cette surexpression dans les hépatocytes ? En utilisant des modèles cellulaires hépatocytaires (HepG2 et Huh7) et des souris KO pour le gène HNF1α nous mettons en évidence les résultats suivants. Les œstrogènes induisent l’expression de SigR1 via son récepteur nucléaire ERα. De même, l’inhibition d’HNF1α induit une surexpression de SigR1. Cette surexpression entraine une prolifération et une stéatose des hépatocytes, correspondant au phénotype des patientes atteintes de H-HCAs. / Sigma 1 receptor (SigR1) is a transmembrane protein of the RE, enriched in the MAMs, which would act like a chaperone. Although ubiquitous, SigR1 is especially expressed in the central nervous system (CNS) and the liver. In the CNS, SigR1 has been linked to neurodegenerative diseases and also pain and depression. SigR1 is also involved in cancer. SigR1 is overexpressed in many cancer tumors and especially in hormone dependent tumors where its expression is correlated to the hormonal status of the tumor. Although SigR1 is highly expressed in the liver, its role in this organ is unknown. Aiming at finding the role of this protein in the liver we analyze its expression in several liver tumors. SigR1 is significantly overexpressed in hepatocellular adenomas mutated for HNF1α gene, H-HCA. H-HCA are benign liver tumors with marked steatosis. They are mostly found in women taking oral contraceptives (estrogens). Why is SigR1 overexpressed in H-HCA ans what are the consequences of this overexpression? Using hepatocyte cellular models (HepG2 and Huh7) and mice that are KO for HNF1α gene, we found the following results. Estrogens induce the expression of SigR1 through its nuclear receptor ERα. HNF1α inhibition also induces its expression. This overexpression leads to an increase of the cell proliferation rate and steatosis. These effects resume H-HCA patients’ phenotype.

Adénome hépatocellulaire

Prolifération

Stéatose

Hepatocellular adenoma

Proliferation

Steatosis

Recherche du neutrino stérile auprès du réacteur de l’ILL : expérience Stereo / Sterile Neutrino Search at short distance from the ILL research reactor : the Stereo experiment

Blanchet, Adrien

03 October 2019

La thèse de doctorat porte sur la physique des neutrinos de réacteurs. L'étude de plus en plus précise des spectres d'antineutrinos des réacteurs a mis à jour une déviation entre la prédiction et les mesures qui pourrait indiquer l'existence d'un nouveau neutrino, non couplé avec l'interaction faible (un neutrino stérile) et de masse autour de 1 ₑV/c². L'expérience STEREO vise à tester l'hypothèse du neutrino stérile auprès du réacteur ILL de Grenoble. Le principe de STEREO repose sur 6 cellules de détection identiques disposées entre 9 et 11.5 m de distance du cœur du réacteur de recherche de l'ILL. Le détecteur a commencé la prise de données en novembre 2016, et les premiers résultats ont été publiés dès 2018. Le travail effectué pendant la thèse a consisté dans un premier temps à caractériser la réponse en énergie du détecteur. Pendant la première phase de prise de données, des défaillances matérielles se sont manifestées entrainant le découplage optique d'une cellule et une augmentation progressive des fuites de lumière entre cellules. Ces deux aspects ont contraint l'analyse de données à développer un algorithme de reconstruction des dépôts d'énergie qui corrige les fuites lumières au premier ordre. Un important travail sur la mesure des paramètres de cette méthode a été entrepris afin d'assurer que l'échelle en énergie soit bien reproduite dans la simulation GEANT4. L'estimation des incertitudes systématiques sur l'échelle en énergie a été effectuée en se servant des bruits de fond cosmogéniques. Le second aspect majeur abordé pendant la thèse est l'analyse statistique et la génération des contours d'exclusion de l'hypothèse du neutrino stérile. La déduction statistique a été conduite en s'inspirant de la méthode de Feldman et Cousins (1999) sur la génération d'intervalles de confiance fréquentistes. Un formalise en X² a spécialement été développé pour mener une analyse d'oscillations indépendante des prédictions de flux et de forme des spectres antineutrinos. Les erreurs statistiques et systématiques ont été propagées à l'aide de matrices de covariance et les lois de X² ont été calculées en générant des pseudo-expériences. L'ensemble des travaux menés pendant cette thèse de doctorat a contribué à la publication de trois papiers présentant les résultats de l'expérience STEREO. / The doctoral thesis focuses on the physics of reactor neutrinos. The increasingly precise study of antineutrinos spectra from reactors has revealed a deviation between the prediction and the measurements, which could indicate the existence of a new neutrino. This new neutrino state would not couple with the weak interaction (a sterile neutrino) and its mass would be around 1 ₑV/c². The STEREO experiment aims at testing the sterile neutrino hypothesis at the ILL reactor in Grenoble-France. The principle of the STEREO experiment is based on 6 identical detector cells aligned between 9 and 11.5 m distance from the core of the ILL research reactor. The detector started taking data in November 2016, and the first results were published in 2018. The work carried out during the thesis initially consisted in characterizing the detector's energy response. During the first phase of data taking, hardware failures occurred leading to the optical decoupling of a cell and a gradual increase in light cross-talk between cells. These two aspects have compelled data analysis to develop a dedicated energy deposit reconstruction algorithm that corrects first-order light leaks using a matrix formalism. Significant work on the measurement of the parameters of this method was undertaken to ensure that the energy scale was well reproduced in the GEANT4 simulation. The estimation of systematic uncertainties on the energy scale was performed using cosmogenic background events. The second major aspect addressed during the thesis is the statistical analysis and generation of exclusion contours of the sterile neutrino hypothesis. The statistical inference was built using the Feldman and Cousins (1999) method by generating frequentist confidence intervals. A formalization in X² has been specially developed to conduct the oscillation analysis independently of any flux or shape prediction of the antineutrino spectra. Statistical and systematic errors were propagated using covariance matrices and X² laws were constructed by generating pseudo-experiments. All the work carried out during this doctoral thesis contributed to the publication of three papers presenting the results of the STEREO experiment.

Neutrino

Stérile

Réacteur

Oscillation

Non-Prolifération

Neutrino

Reactor

Sterile

Oscillation

Non-Proliferation

Studies on pathophysiological significance of intraislet ghrelin using transgenic animal model. / 遺伝子改変動物を用いた膵島由来グレリンの病態生理学的意義の検討

Bando, Mika

24 March 2014

京都大学 / 0048 / 新制・課程博士 / 博士(人間健康科学) / 甲第18197号 / 人健博第14号 / 新制||人健||2(附属図書館) / 31055 / 京都大学大学院医学研究科人間健康科学系専攻 / (主査)教授 藤井 康友, 教授 岡 昌吾, 教授 横出 正之 / 学位規則第4条第1項該当 / Doctor of Human Health Sciences / Kyoto University / DFAM

ghrelin

insulin secretion

glucose metabolism

diabetes

beta cell proliferation

498