La costruzione moderna a Bologna 1920 - 1940

Selvatici, Chiara <1977>

07 June 2011

Il presente lavoro di ricerca si inserisce all’interno degli ambiti di interesse del settore disciplinare dell’ICAR 10 – Architettura Tecnica, rappresentato dalla Storia della costruzione. In questo quadro, lo studio sulla Costruzione Moderna a Bologna tra il 1920 e il 1940, costituisce un tassello di una ricerca più ampia ed intesa a delineare l’importanza assunta dalla vicenda bolognese nel definire il profilo teorico ed applicativo della tecnica in cemento armato nella genesi del linguaggio architettonico che connota l’esperienza del Modernismo italiano degli anni trenta. La ricaduta più diretta della ricerca è rintracciabile nella creazione di una base informativa ipertestuale strutturata secondo diversi livelli di lettura tra loro correlati: la localizzazione, i progettisti e le imprese costruttrici, l’anno di realizzazione, la tipologia, le tecniche costruttive impiegate, la storia dell’edificio, le trasformazioni, la localizzazione della documentazione e le fonti bibliografiche, con collegamenti ipertestuali che consentono di consultare il materiale documentario. Gli esiti di tale studio hanno una duplice finalità: da un lato tale lavoro restituisce una mappatura analitica del patrimonio edilizio costruito nel ventennio analizzato, consentendo una registrazione sintetica ma puntuale delle fonti archivistiche e dei relativi apparati documentali. Un lavoro di supporto indispensabile per ogni futura ricerca intesa ad indagare le singole vicende che hanno accompagnato lo sviluppo edilizio della città di Bologna. In seconda istanza questo studio consente di porre in luce l’importanza assunta dai magisteri tecnici nel definire le scelte di ordine architettonico, ovvero di evidenziare come la conoscenza della storia materiale degli edifici induca a formulare una valutazione più appropriata e stringente sugli esiti architettonici conseguiti, superando così l’astrattezza di una interpretazione votata ai soli aspetti figurativi.

ICAR/10 Architettura tecnica

I controlli esterni e il coordinamento della finanza pubblica

Papiano, Elena <1968>

13 May 2011

No description available.

IUS/10 Diritto amministrativo

L'autotutela amministrativa e le situazioni giuridiche soggettive

Boschi, Maria Elena <1982>

13 May 2011

No description available.

IUS/10 Diritto amministrativo

Stem cell pathways in the basal-like breast carcinoma: the role of beta-catenin and HIF-1alpha / Vie di segnalazione staminali nel carcinoma mammario a fenotipo basale: il ruolo di beta-catenina e di HIF-1alpha

D’Uva, Gabriele Matteo <1980>

10 May 2011

Basal-like tumor is an aggressive breast carcinoma subtype that displays an expression signature similar to that of the basal/myoepithelial cells of the breast tissue. Basal-like carcinoma are characterized by over-expression of the Epidermal Growth Factor receptor (EGFR), high frequency of p53 mutations, cytoplasmic/nuclear localization of beta-catenin, overexpression of the Hypoxia inducible factor (HIF)-1alpha target Carbonic Anhydrase isoenzime 9 (CA9) and a gene expression pattern similar to that of normal and cancer stem cells, including the over-expression of the mammary stem cell markers CD44. In this study we investigated the role of p53, EGFR, beta-catenin and HIF-1alpha in the regulation of stem cell features and genes associated with the basal-like gene expression profile. The findings reported in this investigation indicate that p53 inactivation in ductal breast carcinoma cells leads to increased EGFR mRNA and protein levels. In our experimental model, EGFR overexpression induces beta-catenin cytoplasmatic stabilization and transcriptional activity and, by that, leads to increased aggressive features including mammosphere (MS) forming and growth capacity, invasive potential and overexpression of the mammary stem cell gene CD44. Moreover we found that EGFR/beta-catenin axis promotes hypoxia survival in breast carcinoma cells via increased CA9 expression. Indeed beta-catenin positively regulates CA9 expression upon hypoxia exposure. Interestingly we found that beta-catenin inhibits HIF-1alpha transcriptional activity. Looking for the mechanism, we found that CA9 expression is promoted by HIF-1alpha and cytoplasmatic beta-catenin further increased it post-transcriptionally, via direct mRNA binding and stabilization. These data reveal a functional beta-catenin/HIF-1alpha interplay among hallmarks of basal-like tumors and unveil a new functional role for cytoplasmic beta-catenin in the phenotype of such tumors. Therefore it can be proposed that the interplay here described among EGFR/beta-catenin and HIF-1alpha may play a role in breast cancer stem cell survival and function.

BIO/10 Biochimica

L'attività pionieristica della Scuola bolognese nello studio e nell'utilizzo del cemento armato: 1875 - 1924. Tecniche costruttive e tipologie architettoniche

Predari, Giorgia <1978>

07 June 2011

La ricerca mira ad indagare l’origine della Scuola ingegneristica bolognese ed il ruolo che essa ha avuto durante i suoi primi 50 anni di attività nella diffusione del calcestruzzo armato in Italia, ed in particolare nella città di Bologna, sia dal punto di vista teorico che architettonico. Il processo di sviluppo del cemento armato è stato indagato secondo i percorsi tipici della scienza e della tecnica: teoria e pratica appaiono nel periodo di sperimentazione del materiale assai lontane; soltanto grazie alla comprensione delle sue potenzialità costruttive e del modo di sfruttarle al meglio, esse iniziano a convergere. L’interesse specifico per la Scuola bolognese va quindi a collocarsi all’interno di un panorama assai più ampio, con l’obiettivo di comprendere se, e fino a quando, le due discipline proseguono lungo strade parallele o se, al contrario, esse godono di reciproche influenze.

ICAR/10 Architettura tecnica

Eterogeneità delle proprietà fisico – chimiche della proteina prionica patologica e variabilità fenotipica ceppo specifica nella malattia di Creutzfeldt – Jakob

Cescatti, Maura <1980>

07 June 2011

Transmissible spongiform encephalopathies (TSEs), or prion diseases, are neurodegenerative disorders that affect humans and mammals. Creutzfeldt-Jakob disease (CJD), the most common TSE in humans, can be sporadic (sCJD), genetic (gCJD), or acquired by infection. All TSEs are characterised by the accumulation of PrPSc, a misfolded form of the cellular protein PrPC. PrPSc is insoluble in detergents, partially resistant to proteolysis and shows a highly enriched β-sheet secondary structure. Six clinico-pathological phenotypes of sCJD have been characterized which correlate at the molecular level with two types (1 or 2) of PrPSc with distinctive physicochemical properties and the genotype at the polymorphic (methionine or valine) codon 129 of the prion protein gene. According to the protein-only hypothesis, which postulates that prions are composed exclusively of PrPSc, the strains of prions that are largely responsible for the wide spectrum of TSE phenotypes are enciphered in PrPSc conformation. In support to this view, studies mainly conducted in experimental scrapie, have shown that several prion strains can be identified based on distinguishing PrPSc biochemical properties. To further contribute to the understanding of the molecular basis of strains and to develop more sensitive strain typing assays in humans we have analyzed PrPSc biochemical properties in two experimental setting. In the first we compared the size of the core after protease digestion and the glycoform pattern of PrPSc before and after transmission of human prions to non human primates or bank voles, whereas in the second we analyzed the conformational stability of PrPSc associated with sCJD, vCJD or fCJD using guanidine hydrochloride (GdnHCl) as denaturant. Combining the results of the two studies, we were able to distinguish five human strains for at least one biochemical property. The present data extend our knowledge about the extent of strain variation and its relationship with PrPSc properties in human TSEs.

BIO/10 Biochimica

Ruolo delle specie reattive dell'ossigeno e di caveole/raft lipidici nella biosegnalazione in linee cellulari umane

Caliceti, Cristiana <1981>

07 June 2011

Membrane lipid rafts are detergent-resistant microdomains containing glycosphingolipids, cholesterol and glycosylphosphatidylinositol-linked proteins; they seem to be actively involved in many cellular processes including signal transduction, apoptosis, cell adhesion and migration. Lipid rafts may represent important functional platforms where redox signals are produced and transmitted in response to various agonists or stimuli. In addition, a new concept is emerging that could be used to define the interactions or amplification of both redox signalling and lipid raft-associated signalling. This concept is characterized by redox-mediated feed forward amplification in lipid platforms. It is proposed that lipid rafts are formed in response to various stimuli; for instance, NAD(P)H oxidase (Nox) subunits are aggregated or recruited in these platforms, increasing Nox activity. Superoxide and hydrogen peroxide generation could induce various regulatory activities, such as the induction of glucose transport activity and proliferation in leukaemia cells. The aim of our study is to probe: i) the involvement of lipid rafts in the modulation of the glucose transporter Glut1 in human acute leukemia cells; ii) the involvement of plasma membrane caveolae/lipid rafts in VEGF-mediated redox signaling via Nox activation in human leukemic cells; iii) the role of p66shc, an adaptor protein, in VEGF signaling and ROS production in endothelial cells (ECs); iv) the role of Sindecan-2, a transmembrane heparan sulphate proteoglycan, in VEGF signaling and physiological response in ECs and v) the antioxidant and pro-apoptotic activities of simple dietary phenolic acids, i. e. caffeic, syringic and protocatechuic acids in leukemia cells, characterized by a very high ROS content. Our results suggest that the role played by NAD(P)H oxidase-derived ROS in the regulation of glucose uptake, proliferation and migration of leukaemia and endothelial cells could likely occur through the control of lipid raft-associated signalling.

BIO/10 Biochimica

Biochemical and molecular aspects of the nutritional regulation of cholesterol biosynthesis / Aspetti biochimico-molecolari della regolazione nutrizionale della biosintesi del colesterolo

Boschetti, Elisa <1981>

07 June 2011

No description available.

BIO/10 Biochimica

ROS generate dalle NAD(P)H ossidasi nella segnalazione redox in linee cellulari leucemiche

Vieceli Dalla Sega, Francesco <1979>

07 June 2011

Discovery of the Nox family has led to the concept that ROS are “intentionally” generated and are biologically functional in various cell types. Over the last decades, ROS have been shown to be involved in several physiological and pathological processes and ROS producing enzymes have been suggested as a target for drug development. The mechanism involved in the prosurvival effect of cytokines on the human acute myeloid leukaemia cell lines M07e and B1647 is investigated. A decrease in intracellular reactive oxygen species (ROS) content, glucose transport activity and cell survival was observed in the presence of inhibitors of plasma membrane ROS sources, such as DPI and apocynin, and by small interference RNA for NOX2 in M07e cells. Furthermore, Nox generated ROS are required to sustain B1647 cell viability and proliferation; in fact, antioxidants such as EUK-134 or Nox inhibitors and siRNA direct cells to apoptotic cell death, suggesting that manipulation of cellular NOX2 and NOX4 could affect survival of leukemic cells. Moreover, hydrogen peroxide has been long thought to be freely diffusible but recent evidence suggest that specific mammalian aquaporin homologues (AQP8) possess the capacity to channel H2O2 across membrane. In this thesis is shown that inhibition of aquaporins diminishes intracellular ROS accumulation either when H2O2 is produced by Nox enzymes or when is added exogenously to the medium. These data suggest that specific inhibition of Nox enzymes and AQP8 could be an interesting novel anti-leukemic strategy.

BIO/10 Biochimica

Ruolo dei recettori degli estrogeni nella trasduzione del segnale nella neoplasia ovarica

Mangano, Chiara <1981>

10 May 2011

Oestrogen induction of cell proliferation is critical in carcinogenesis of gynaecologic tissues. The effects of oestrogens are mediated by Oestrogen receptor (ER) ERα and ERβ, which are members of the nuclear steroid receptor superfamily. The balance between the ERα/ERβ levels seems critical during carcinogenesis due to their different role in proliferation and apoptosis. SERMs are a class of drugs targeting ERs used especially in the treatment of breast cancer, that despite their usefulness, cause side effects. Therefore, it’s important to develop new active molecules without side effects. In a previous work Andreani et al.(2007) investigated the antitumor activity of a new class of indole-derivatives in 60 different human cancer cell lines. In particular they noted that compound named 3L was able to induce a strong antiproliferative effect in cell lines derived from breast, cervix, ovary ,CNS and colon. The aim of this thesis is to characterize the biological effect in ovarian carcinoma cells (IGROV-1), colon adenocarcinoma cells (HT29), cervix adenocarcinoma cells (HelaS3) and breast cancer cells (MCF7). Among the effect exerted on the other cell lines, the most interesting is the cytostatic effect on IGROV-1. In order to identify the 3L molecular target we monitored the 3L concentration in the IGROV-1 nuclear fractions. The analysis revealed that the drug localizes in the nucleus starting from 6 hrs after treatment, suggesting a nuclear target. The stimulation with oestrogen did not increase the proliferation rate in 3L treated cells, suggesting a possible involvement with oestrogen receptors. Due to the 3L fluorescent properties, we demonstrated a colocalization between the ER and the 3L compound. In particular, a chromatin binding assay revealed the presence of a 3L-ERβ complex bound to DNA, interaction that may be the cause of the observed antiproliferative effect.

BIO/10 Biochimica