Brainstem tau pathology in Alzheimer’s disease is characterized by increase of three repeat tau and independent of amyloid β / 脳幹におけるアルツハイマー病のタウ病変は、3リピート型タウの増加を特徴とし、アミロイドβ蓄積から独立して存在する

Uematsu, Miho

26 March 2018

京都大学 / 0048 / 新制・課程博士 / 博士(医学) / 甲第21010号 / 医博第4356号 / 新制||医||1028(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 井上 治久, 教授 村井 俊哉, 教授 林 康紀 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

Alzheimer's disease pathology

Tau isoform

Human brain

Virtual slide imaging

Brainstem

490

Sodium Pumps Keep Us Running: Distinct Roles For Na,K-ATPase Isozymes In Regulation of Skeletal Muscle Excitability

Hakimjavadi, Hesamedin

10 June 2019

No description available.

Physiological Psychology

Na,K-ATPase

Isoform

Skeletal Muscle

Adrenergic stimulation

Na pump

Fatigue

The Role of Fibroblast Growth Factor-2 Isoforms in Ischemia-reperfusion Injury and Cardioprotection

Liao, Siyun

23 April 2008

No description available.

Pharmacology

Fibroblast growth factor 2

isoform

LMW

HMW

FGFR

ischemia reperfusion injury

cardioprotection

JNK

apoptosis

MOLECULAR AND PHYSIOLOGICAL STUDIES OF ELECTROLYTE AND FLUID TRANSPORT PERTURBATIONS IN NKCC1 AND NHE3 DEFICIENT MICE

Flagella, Michael

11 October 2001

No description available.

MICROARRAY

SODIUM/PROTON EXCHANGER 3

SODIUM POTASSIUM CHLORIDE ISOFORM 1

BLOOD PRESSURE

SECRETION

PDK2 leads to cisplatin resistance through suppression of mitochondrial function in ovarian clear cell carcinoma / 卵巣明細胞癌においてPDK2はミトコンドリア機能を抑制しシスプラチン耐性をもたらす

Kitamura, Sachiko

23 March 2022

京都大学 / 新制・課程博士 / 博士(医学) / 甲第23763号 / 医博第4809号 / 新制||医||1056(附属図書館) / 京都大学大学院医学研究科医学専攻 / (主査)教授 中島 貴子, 教授 戸井 雅和, 教授 伊藤 貴浩 / 学位規則第4条第1項該当 / Doctor of Medical Science / Kyoto University / DFAM

pyruvate dehydrogenase kinase isoform 2

mitochondria

clear cell carcinoma

ovarian cancer

chemoresistance

490

OCT1-mediated cellular drug uptake and interactions between drug transport and drug metabolism / OCT1-mediated cellular drug uptake and interactions between drug transport and drug metabolism

Saadatmand, Ali Reza

25 October 2012

No description available.

610 Medizin, Gesundheit

Medicine

Biology (incl. Psychology)

medikament-Aufnahme

Metabolisierung

drug uptake

drug metabolism

44.38 Pharmakologie

Identification of the Pla2 Responsible For Prostanoid Synthesis in Response to Inflammatory Cytokines

Fernando, Chaminda

01 January 2005

Preliminary studies from our laboratory showed that cPLA2α may be responsible for approximately 50-60% of the PGE2 production in response to inflammatory cytokines. Thus, we hypothesized that a closely-related PLA2 is responsible for 40-50% of the PGE2 produced in response to inflammatory cytokines. To this end, we utilized RNAi technology, extensively optimized, to down regulate the expression of closely-related isoforms of phospholipase A2 in A549 cells and used an enzyme linked immuno sorbent assay (ELISA) to quantitate the PGE2 produced. These studies found that cytosolic phospholipase A2α (cPLA2α) regulated 97.7% of the prostaglandin E2 (PGE2) produced in response to inflammatory cytokines (e.g. IL-1β or TNFα), as well as regulating the basal levels of this prostanoid. Furthermore, cPLA2γ, cPLA2δ, and iPLA2 were found to also to regulate the basal levels of PGE2 production. On the other hand, cPLA2β was not involved in prostanoid synthesis in A549 cells either in the presence or absence of inflammatory cytokines. Thus, our studies show that cPLA2α plays the pivotal role in the production of PGE2 in response to inflammatory cytokines, and suggests that cPLA2α may be a possible drug target in diseases such as asthma, inflammation, and cancer.

cytokines

RNAi

prostanoid

adenacarcinoma

immunoblotting

protein

phospholipases

protaglandin

eicosanoid

biosynthesis

isoform

Life Sciences

Software for Estimation of Human Transcriptome Isoform Expression Using RNA-Seq Data

Johnson, Kristen

18 May 2012

The goal of this thesis research was to develop software to be used with RNA-Seq data for transcriptome quantification that was capable of handling multireads and quantifying isoforms on a more global level. Current software available for these purposes uses various forms of parameter alteration in order to work with multireads. Many still analyze isoforms per gene or per researcher determined clusters as well. By doing so, the effects of multireads are diminished or possibly wrongly represented. To address this issue, two programs, GWIE and ChromIE, were developed based on a simple iterative EM-like algorithm with no parameter manipulation. These programs are used to produce accurate isoform expression levels.

RNA-Seq

Transcriptome Quantification

Isoform Expression

Multireads

Expectation-Maximization (EM) Algorithm

Other Computer Sciences

MRI T2 Signal Changes Indicate Tau Pathophysiology in a Murine Alzheimer's Disease Model

Adhikari, Rajan Deep

01 August 2017

Pathogenesis, diagnosis and treatment, the essential domains in medical practice, seem helpless to address Alzheimer's disease (AD). With a huge mortality rate, it is looming and threatening the socioeconomic barrier. Despite many different studies, the pathogenesis of AD remains inconclusive. However, growing numbers of studies suggest oxidative stress to contribute to the initiation and progression of AD. We propose an iron hypothesis: iron mediated oxidative damage by reactive oxygen species (ROS), which induces protective roles of amyloid beta and hyper-phosphorylated tau (HP-tau) to sequester iron and limit the disease. We propose to study such mechanism using transgenic mice models for AD, inducing oxidative stress to elevate intracellular iron, and analyze its co-localization with proteins using Magnetic Resonance Imaging (MRI), 1H Nuclear Magnetic Resonance (NMR) spectroscopy and Western blot. We report three primary findings: 1) a significant loss in T2 signal over bilateral hippocampi of transgenic mice compared to the wild types (WT) by three months, corresponding to early disease and the ability of proteins to sequestration iron. Ability of rescue treatments to impede disease progression reflected as preserved T2 signal intensities over these areas throughout our study period of nine months. 2) Concentration of zinc and its dual role in the presence or absence of oxidative stress reflected as loss of 1H NMR T2 measurement showed that higher concentrations of zinc were neuro protective when there was an active oxidative stress inducing condition, but neurotoxic and promote oxidative damage in normal condition. And 3) Different strains of mice, according to their transgene, expressed various proteins associated with AD. However, these expressions were in accordance with our iron-hypothesis.

MRI

T2

Tau

Alzheimer's disease

oxidative stress

iron

amyloid beta

hyper phosphorylated tau

transgene

MRI

NMR

western blot

isoform

Physiology

Design and synthesis of small molecule inhibitors of zinc metalloenzymes

Patil, Vishal

28 October 2011

Histone deacetylases (HDACs) are a class of enzymes that play a crucial role in DNA expression by removing an acetyl group from the ɛ-N-acetyl lysine residue on histone proteins. Out of 18 isoforms of HDAC enzymes which are classified into 4 classes, only 11 of them are metalloenzymes that require zinc for its catalytic activity. HDACs are considered promising target for drug development in cancer and other parasitic diseases due to their role in gene expression. Histone deacetylase inhibitors (HDACi) can cause cell cycle arrest, and induce differentiation or apotosis. While HDACi shows promising antitumor effects, their mechanism of action and selectivity against cancer cells have not been adequately defined yet. In addition, low oral bioavailability, short half-life time, bone marrow toxicity, and cardiotoxicity limit their use in clinic. Therefore, there is considerable interest in developing compounds with selectivity and specificity towards individual family members of HDACs. The prototypical pharmacophore for HDAC inhibitors consist of a metal-binding moiety that coordinates to the catalytic metal ion within the HDAC active site, a capping group that interacts with the residues at the entrance of the active site and a linker that appropriately positions the metal-binding moiety and capping group for interactions in the active site. It has been shown that modification of cap, cap linking moiety, linker or zinc binding group (ZBG) shows promises of superior potency and isoform selectivity. My thesis research involves manipulating different aspects of the pharmacophoric model to yield not only more potent, selective, and effective drugs but also to help understand the biology of HDAC isoforms. In addition, I was successful in extending studies on HDAC isoforms to other zinc metalloenzymes such as leishmanolysin (gp63) and spliceosome associated zinc-metalloenzymes to understand biology of these zinc metalloenzymes by developing potent and selective small molecule inhibitors. This will aid in improvement of existing therapeutics for treatment of cancer, leishmania, malaria and other genetic disorders.

Bifunctional inhibitors

Isoform selectivity

Spliceosome assembly inhibitors

Leishmania

Malaria

Histone deacetylase inhibitors

Cancer chemotherapy

Zinc binding groups

Metalloenzymes

Enzymes

Metalloproteins