Identificazione di un profilo molecolare di rischio nei pazienti pediatrici affetti da Linfoma di Hodgkin / Identification of a molecular risk profile in pediatric patients with Hodgkin Lymphoma

Marino, Flora <1977>

16 May 2013

Obiettivi: nonostante i miglioramenti nel trattamento, circa il 30% dei pazienti pediatrici affetti da Linfoma di Hodgkin (LH) in stadio avanzato recidiva o muore per progressione di malattia e i correnti metodi predittivi biologico-clinici non consentono di individuare tali pazienti. L’obiettivo dello studio è stato quello di definire un profilo molecolare di rischio che correli con l’outcome in questi pazienti. Materiali e metodi: studio retrospettico condotto su pazienti pediatrici affetti da LH omogeneamente trattati dal 2004 in poi. Su tali pazienti è stato intrapreso uno studio di validazione di marcatori molecolari già identificati in studi esplorativi precedenti. 27 geni sono stati analizzati in RT PCR su campioni di tessuto istologico prelevato alla diagnosi fissato in formalina e processato in paraffina relativi a una coorte di 37 pazienti, 12 ad outcome sfavorevole e 25 ad outcome favorevole. Risultati: dall’analisi univariata è emerso che solo l’espressione di CASP3 e CYCS, appartenenti al pathway apoptotico, è in grado di influenzare l’EFS in modo significativo nella nostra coorte di pazienti. Lo studio delle possibili combinazioni di questi geni ha mostrato l’esistenza di 3 gruppi di rischio che correlano con l’EFS: alto rischio (down regolazione di entrambi i geni), rischio intermedio (down regolazione di uno solo dei 2 geni), basso rischio (up regolazione di entrambi i geni). Dall’analisi multivariata è emerso che CASP3 è l’unica variabile che mantiene la sua indipendenza nell’influenzare la prognosi con un rischio di eventi di oltre il doppio di chi ha un’espressione bassa di questo gene. Conclusioni: i risultati ottenuti sulla nostra coorte di pazienti pediatrici affetti da LH confermano l’impatto sulla prognosi di due marcatori molecolari CASP3 e CYCS coinvolti nel patwhay apoptotico. La valutazione del profilo di espressione di tali geni, potrebbe pertanto essere utilizzata in corso di stadiazione, come criterio di predittività. / Purpose: despite improvement in the treatment of advanced Hodgkin lymphoma (HL), approximately 30% of pediatric patients relapse or die as result of the disease. Current methods to predict prognosis determined by clinical and biological parameters, fail to identify these patients accurately. The aim of this study was to define a molecular profile of risk correlates with outcome in these patients. Methods: retrospective study of pediatric patients with LH homogeneously treated from 2004 onwards. Of these patients was undertaken a validation study of molecular markers already identified in exploratory studies previously. 27 best predictor genes in HL was evaluated in RT PCR in formalin-fixed paraffin embedded diagnostic lymph-node samples obtained from 37 pediatric patients with HL, including 25 responders and 12 non responders to standard treatment and compared the expression profiles of patients with favorable and unfavourable clinical outcome. Results: univariate regression analysis revealed that only the expression of CASP3 and CYCS genes, involved in the apoptotic pathway, is able to significantly predict failure to treatment in our cohort of patients. The study of the possible combinations of these genes has shown the existence of 3 risk groups that correlate with EFS: high risk (down regulation of both genes), intermediate risk (down regulation of only one of the 2 genes), low risk (up regulation of both genes). Multivariate analysis showed that CASP3 is the only variable that maintains its independence in influencing the prognosis with a risk of events more than double in patients with low expression of this gene Conclusions: The results of our cohort of pediatric patients with HL confirm the impact on prognosis of two molecular markers CASP3 and CYCS involved in the apoptotic pathway. The evaluation of the expression profile of these genes, may therefore be used in the course of staging, as a criterion of predictivity.

MED/06 Oncologia medica

The effect of osmolytes on protein fold stability at the single-molecule level

Aioanei, Daniel <1980>

22 April 2013

By pulling and releasing the tension on protein homomers with the Atomic Force Miscroscope (AFM) at different pulling speeds, dwell times and dwell distances, the observed force-response of the protein can be fitted with suitable theoretical models. In this respect we developed mathematical procedures and open-source computer codes for driving such experiments and fitting Bell’s model to experimental protein unfolding forces and protein folding frequencies. We applied the above techniques to the study of proteins GB1 (the B1 IgG-binding domain of protein G from Streptococcus) and I27 (a module of human cardiac titin) in aqueous solutions of protecting osmolytes such as dimethyl sulfoxide (DMSO), glycerol and trimethylamine N-oxide (TMAO). In order to get a molecular understanding of the experimental results we developed an Ising-like model for proteins that incorporates the osmophobic nature of their backbone. The model benefits from analytical thermodynamics and kinetics amenable to Monte-Carlo simulation. The prevailing view used to be that small protecting osmolytes bridge the separating beta-strands of proteins with mechanical resistance, presumably shifting the transition state to significantly higher distances that correlate with the molecular size of the osmolyte molecules. Our experiments showed instead that protecting osmolytes slow down protein unfolding and speed-up protein folding at physiological pH without shifting the protein transition state on the mechanical reaction coordinate. Together with the theoretical results of the Ising-model, our results lend support to the osmophobic theory according to which osmolyte stabilisation is a result of the preferential exclusion of the osmolyte molecules from the protein backbone. The results obtained during this thesis work have markedly improved our understanding of the strategy selected by Nature to strengthen protein stability in hostile environments, shifting the focus from hypothetical protein-osmolyte interactions to the more general mechanism based on the osmophobicity of the protein backbone.

CHIM/06 Chimica organica

Sintesi di molecole biologicamente attive con tecniche chemoenzimatiche:beta-lattami, profeni e alfa-amminoacidi non naturali / Synthesis of biologically active molecules by using chemoenzymatic techniques:beta-lactams, profens and unnatural alfa-amino acids

Pori, Matteo <1983>

22 April 2013

Il progetto di ricerca di questa tesi è stato focalizzato sulla sintesi di tre classi di molecole: β-lattami, Profeni e α-amminonitrili, utilizzando moderne tecniche di sintesi organica, metodologie ecosostenibili e strategie biocatalitiche. I profeni sono una categoria di antiinfiammatori molto diffusa e in particolare abbiamo sviluppato e ottimizzato una procedura in due step per ottenere (S)-Profeni da 2-arilpropanali raceme. Il primo step consiste in una bioriduzione delle aldeidi per dare i relativi (S)-2-Aril Propanoli tramite un processo DKR mediato dall’enzima Horse Liver Alcohol Dehydrogenase. Il secondo, l’ossidazione a (S)-Profeni, è promossa da NaClO2 e TEMPO come catalizzatore. Con lo scopo di migliorare il processo, in collaborazione con il gruppo di ricerca di Francesca Paradisi all’University College Dublino abbiamo immobilizzato l’enzima HLADH, ottenendo buone rese e una migliore enantioselettività. Abbiamo inoltre proposto un interessante approccio enzimatico per l’ossidazione degli (S)-2-Aril Propanoli utilizzando una laccasi da Trametes Versicolor. L’anello β-lattamico è un eterociclo molto importante, noto per essere un interessante farmacoforo. Abbiamo sintetizzato nuovi N-metiltio beta-lattami, che hanno mostrato un’attività antibatterica molto interessante contro ceppi resistenti di Staphilococcus Aureus prelevati da pazienti affetti da fibrosis cistica. Abbiamo poi coniugato gruppi polifenolici a questi nuovi β-lattami ottenendo molecule antiossidanti e antibatteriche, cioè con attività duale. Abbiamo poi sintetizzato un nuovo ibrido retinoide-betalattame che ha indotto differenziazione si cellule di neuroblastoma. Abbiamo poi sfruttato la reazione di aperture dell’anello monobattamico tramite enzimi idrolitici, con lo scopo di ottenere β-amminoacidi chirali desimmetrizzati come il monoestere dell’acido β–amminoglutammico. Per quando riguarda gli α-amminonitrili, è stato sviluppato un protocollo di Strecker. Le reazioni sono state molto efficienti utilizzando come fonte di cianuro l’acetone cianidrina in acqua, utilizzando differenti aldeidi e chetoni, ammine primarie e secondarie. Per mettere a punto una versione asimmetrica del protocollo, abbiamo usato ammine chirali con lo scopo di ottenere nuovi α-amminonitrili chirali. / The research project of this thesis has been focused on the synthesis of three class of molecules: β-lactams, Profens and α-aminonitriles by using modern techniques of organic synthesis, favouring sustainable and green methodologies, especially biocatalytic strategies. Profens are a very important and widespread category of pain killer and in particular we developed and optimized a two steps procedure to obtain (S)-Profens from racemic 2-aryl propanals. The first step was a bioreduction of the aldehydes to (S)-2-Aryl Propanols with a DKR process mediated by Horse Liver Alcohol Dehydrogenase (HLADH); the second one was a “green oxidation” to (S)-Profens promoted by NaClO2 and TEMPO/NaClO as catalyst. To improve the whole two-step process, in a collaboration with the research group of Francesca Paradisi at the University College of Dublin we immobilized a modified HLADH, with good yields and better enantioselectivity. We also proposed an interesting enzymatic approach for the oxidation of (S)-2-Aryl Propanols by using Laccase from Trametes Versicolor. β-lactam ring is a very important heterocycle, known to be an interesting pharmacophore. We synthesized new N-methylthio monobactams which showed an interesting antibacterial activity against resistant strains of Staphilococcus Aureus collected from patients of cystic fibrosis. We then conjugated polyphenolic groups to the new monobactams obtaining molecules with antioxidant and antibacterial with dual-activity. A new hybrid retinoid-β-lactam was developed which induced differentiation on neuroblastoma cells. The ring opening of monobactams by hydrolytic enzymes was investigated to access desymmetrizated chiral β-aminoacids such as beta-aminoglutamic acid monoesters. For what concerns the third class of molecules reported, the α-aminonitriles, a new Strecker protocol was developed. Reactions worked very well in water by using acetone cyanohydrin as cyanide source with different aldehydes and ketones and primary or secondary amines; to provide an asymmetric version of our protocol we used chiral amines from chiral pool obtaining new chiral α-aminonitriles.

CHIM/06 Chimica organica

De Novo Design of Foldamers for Preparation of Nanostructured Materials / De Novo Design di foldameri per la preparazione di materiali nanostrutturati

Castellucci, Nicola <1984>

22 April 2013

This thesis deals with the synthesis and the conformation analysis of hybrid foldamers containing the 4-carboxyoxazolidin-2-one unit or related molecules, in which an imido-type function is obtained by coupling the nitrogen of the heterocycle with the carboxylic acid moiety of the next unit. The imide group is characterized by a nitrogen atom connected to an endocyclic and an exocyclic carbonyl, which tend always to adopt the trans conformation. As a consequence of this locally constrained disposition effect, these imide-type oligomers are forced to fold in ordered conformations. The synthetic approach is highly tuneable with endless variations, so, simply by changing the design and the synthesis, a wide variety of foldamers with the required properties may be prepared “on demand”. Thus a wide variety of unusual secondary structures and interesting supramolecular materials may be obtained with hybrid foldamers. The behaviour in the solid state of some of these compounds has been analyzed in detail, thus showing the formation of different kinds of supramolecular materials that may be used for several applications. A winning example is the production of a bolaamphiphilic gelators that may also be doped with small amounts of dansyl containing compounds, needed to show the cellular uptake into IGROV-1 cells, by confocal laser scanning microscopy. These gels are readily internalized by cells and are biologically inactive, making them very good candidates in the promising field of drug delivery. In the last part of the thesis, a particular attention was directed to the search of new scaffolds that behave as constrained amino acid mimetics, showing that tetramic acids derivatives could be good candidates for the synthesis and applications of molecules having an ordered secondary structure. / Il lavoro di ricerca svolto nel triennio di frequenza della Scuola di Dottorato in Scienze Chimiche ha avuto come obiettivo la sintesi e l’analisi conformazionale di molecole sintetiche, appartenenti alla classe dei foldameri pseudopeptidici. La maggior parte delle molecole sintetizzate hanno come nucleo centrale un’unità eterociclica derivante dalla treonina detta ossazolidinone. Gli acil-derivati di questo scaffold sintetico hanno la particolarità di assumere strutture secondarie stabili e ben definite. In questo ambito è stata messa a punto la sintesi di etero‐oligomeri (contenenti due o più diversi amminoacidi naturali o sintetici), sia lineari sia ciclici per mimare strutture secondarie come eliche, turns o sheets. Alcune classi di oligomeri tendono ad assumere una struttura ordinata in fase solida, presentandosi sotto forma di fibrille osservabili al microscopio ottico. Alcuni composti hanno mostrato interessanti proprietà come gelator, cioè composi in grado di formare gel sia con acqua che con solventi organici. Tali gel si sono dimostrati anche buoni complessanti per sali metallici. Sia i monomeri che gli oligomeri sono stati sintetizzati utilizzando metodi di coupling in soluzione. Una particolare attenzione è stata riposta nella purificazione delle varie molecole. Oltre ai composti di natura ossazolidinonica, è stata valutata la sintesi di altri scaffold sintetici che, una volta inseriti in strutture molecolari più complesse, danno origine a molecole in grado di essere classificate come foldameri. Una parte consistente dell’attività di laboratorio è stata volta alla sintesi di acidi tetrammici, eterocicli ricorrenti in natura. Un’analisi conformazionale delle molecole sintetizzate ha dimostrato come anche questo tipo di molecole sia in grado di auto assemblarsi in strutture secondarie ordinate.

CHIM/06 Chimica organica

Valutazione del ruolo dell'espressione di IRS-1 nel differenziamento osteoblastico di cellule di osteosarcoma ed MSCs / Evaluation of IRS-1 role in osteoblastic differentiation of osteosarcoma cells and MSCs

Contaldo, Clara <1984>

08 May 2013

L’osteosarcoma (OS) è il tumore primitivo dell’osso più comune in età pediatrica e adolescenziale. L’OS è stato recentemente riconsiderato come una patologia da de-differenziamento, legata all’interruzione del processo cui vanno incontro i precursori osteoblastici, quali le cellule staminali mesenchimali (MSCs), per trasformarsi in osteoblasti maturi. Il sistema IGF è coinvolto nella regolazione della proliferazione e del differenziamento di cellule di OS. IRS-1 è un mediatore critico di tale via di segnalazione e il suo livello di espressione modula il differenziamento di cellule ematopoietiche. Lo scopo di questa tesi è stato quello di definire il ruolo di IRS-1 nel differenziamento osteoblastico di MSCs e cellule di OS. Il potenziale differenziativo di cellule di OS umano e murino e di MSCs derivate da midollo osseo è stato valutato tramite Alizarin Red staining e Real Time-PCR. Dai dati ottenuti è emerso come i livelli di espressione di IRS-1 diminuiscano durante il differenziamento osteoblastico. Conseguentemente, i livelli di espressione di IRS-1 sono stati manipolati utilizzando shRNA per down-regolare l’espressione della proteina o un plasmide per sovra-esprimerla. Sia la down-regolazione sia la sovra-espressione di IRS-1 hanno inibito il differenziamento osteoblastico delle linee cellulari considerate. Allo scopo di valutare il contributo di IRS-1 nella via di segnalazione di IGF-1R è stato utilizzato l’inibitore di tale recettore, αIR-3. Anche in questo caso è stata osservata una riduzione della capacità differenziativa. L’inibitore del proteasoma MG-132 ha portato ad un aumento dei livelli di IRS-1, portando nuovamente all’inibizione del differenziamento osteoblastico e suggerendo che l’ubiquitinazione di questa proteina potrebbe avere un ruolo importante nel mantenimento di appropriati livelli di espressione di IRS-1. I risultati ottenuti indicano la criticità dei livelli di espressione di IRS-1 nella determinazione della capacità differenziativa sia di cellule di OS umano e murino, sia delle MSCs. / Osteosarcoma (OS) is the most common primary malignant bone tumor affecting children and adolescents. OS has recently been re-considered as a differentiation disease, caused by genetic and epigenetic alterations which may impair normal bone development by blocking multipotent mesenchymal stem cell (MSCs) differentiation into osteoblasts. The IGF-system is involved in regulating OS cell proliferation and differentiation. IRS-1 is a critical mediator of IGF-1R signaling and its expression level modulates hematopoietic cell differentiation. The aim of this study is to define the role of IRS-1 in the osteoblastic differentiation of MSCs and OS cells. Differentiating potential of human and murine OS cell lines and bone marrow-derived mouse MSCs was evaluated by Alizarin Red staining and real-time PCR. We found that IRS-1 expression level decreased during differentiation. Consequently, IRS-1 expression levels were manipulated using shRNAs to knock-down, or a plasmid to over-express the protein. Both down-regulation and over-expression of IRS-1 inhibited osteoblastic differentiation. To understand the contribution of IRS-1 in the IGF-1R pathway we used the αIR-3 IGF-1R blocking antibody, which inhibited the differentiation process. The proteasome inhibitor MG-132 led to an increase in IRS-1 protein level that again inhibited osteoblastic differentiation, suggesting ubiquitination may play a role in maintaining the appropriate expression level of IRS-1. Taken together, these results indicate that IRS-1 expression level is critical for determining the differentiating capacity of MSCs as well as human and mouse OS cells and that precise regulation of IRS-1 expression by cells is required for this commitment to osteoblastic differentiation.

MED/06 Oncologia medica

Electrochemical sensing strategies for the detection of interactions between biological macromolecules

Onofri, Manuele <1983>

22 April 2013

Electrochemical biosensors provide an attractive means to analyze the content of a biological sample due to the direct conversion of a biological event to an electronic signal, enabling the development of cheap, small, portable and simple devices, that allow multiplex and real-time detection. At the same time nanobiotechnology is drastically revolutionizing the biosensors development and different transduction strategies exploit concepts developed in these field to simplify the analysis operations for operators and end users, offering higher specificity, higher sensitivity, higher operational stability, integrated sample treatments and shorter analysis time. The aim of this PhD work has been the application of nanobiotechnological strategies to electrochemical biosensors for the detection of biological macromolecules. Specifically, one project was focused on the application of a DNA nanotechnology called hybridization chain reaction (HCR), to amplify the hybridization signal in an electrochemical DNA biosensor. Another project on which the research activity was focused concerns the development of an electrochemical biosensor based on a biological model membrane anchored to a solid surface (tBLM), for the recognition of interactions between the lipid membrane and different types of target molecules.

CHIM/06 Chimica organica

Design, Synthesis and Characterization of N-Containing Organic Compounds / Progettazione, sintesi e caratterizzazione di composti organici contenenti azoto

Long, Sha <1983>

22 April 2013

The needed of new intermediates/products for screening in the fields of drug discovery and material science is the driving force behind the development of new methodologies and technologies. Organic scaffolds are privileged targets for this scouting. Among them a priority place must be attributed to those including nitrogen functionalities in their scaffolds. It comes out that new methodologies, allowing the introduction of the nitrogen atom for the synthesis of an established target or for the curiosity driven researches, will always be welcome. The target of this PhD Thesis’ work is framed within this goal. Accordingly, Chapter 1 reports the preparation of new N-Heteroarylmethyl 3-carboxy-5-hydroxy piperidine scaffold, as potential and selective α-glucosidase inhibitors. The proposed reversible uncompetitive mechanism of inhibition makes them attractive as interesting candidate for drug development. Chapter 2 is more environmentally method-driven research. Eco-friendly studies on the synthesis of enantiomerically pure 1,4-dihydropyridines using “solid” ammonia (magnesium nitride) is reported via classical Hantzch method. Chapter 3 and Chapter 4 may be targeted as the core of the Thesis’s research work. Chapter 3 reports the studies addressed to the synthesis of N-containing heterocycles by using N-trialkylsilylimine/hetero-Diels–Alder (HAD) approach. New eco-friendly methodology as MAOS (Microwave Assisted Organic Synthesis) has been used as witness of our interest to a sustainable chemistry. Theoretical calculations were adopted to fully clarify the reaction mechanism. Chapter 4 is dedicated to picture the most recent studies performed on the application of N-Metallo-ketene imines (metallo= Si, Sn, Al), relatively new intermediates which are becoming very popular, in the preparation of highly functionalized N-containing derivatives, accordingly to the Thesis’ target. Derivatives obtained are designed in such a way that they could be of interest in the field of drug and new material chemistry.

CHIM/06 Chimica organica

Studio e caratterizzazione di biosensori sviluppati su dispositivi inorganici ed organici / Study and charactezization of biosensors developed on inorganic and organic device

Bonetti, Simone <1983>

17 April 2013

L’attività di dottorato qui descritta ha riguardato inizialmente lo sviluppo di biosensori elettrochimici semplificati per la rilevazione di DNA e successivamente lo studio di dispositivi organici ad effetto di campo per la stimolazione e il rilevamento dell’attività bioelettrica di cellule neuronali. Il lavoro di ricerca riguardante il prima parte è stato focalizzato sulla fabbricazione e sulla caratterizzazione di un biosensore a due elettrodi per la rilevazione di DNA solubile , facilmente producibile a livello industriale. Tale sensore infatti, è in grado di leggere livelli diversi di correnti faradiche sulle superfici in oro degli elettrodi, a discrezione di un eventuale ibridizzazione del DNA da analizzare su di esse. I risultati ottenuti riguardo a questo biosensore sono :la paragonabilità dello stesso con i sensori standard a tre elettrodi basati sulla medesima metodica, la possibilità di effettuare due misure in parallelo di uno stesso campione o di 2 diversi campioni su di uno stesso di dispositivo e la buona applicabilità della chimica superficiale a base di tale biosensore a superfici create con tecnologie industriali. Successivamente a tali studi, mi sono focalizzato sull’utilizzo di dispositivi organici ad effetto campo (in particolare OTFT) per lo sviluppo di un biosensore capace di stimolare e registrare l’attività bioelettrica di cellule neuronali. Inizialmente sono state identificate le caratteristiche del materiale organico utilizzato e successivamente del dispositivo fabbricato pre e post esposizione all’ambiente fisiologico. Poi, sono stati effettuati esperimenti per osservare la capacità di stimolare e di leggere i segnali elettrogenici da parte dell’OTFT. I risultati ottenuti da tali studi sono che: il materiale organico ed il dispositivo mantengo le loro caratteristiche morfologiche e funzionali dopo l’esposizione per giorni all’ambiente fisiologico. Inoltre l’OFET in grado di stimolare il cambiamento delle tensioni di membrana cellulari e contemporaneamente di registrare tali variazioni e le eventuali risposte cellulari provocate da esse. / The activity of my PhD concerns both the development of an electrochemical biosensor for the detection of soluble DNA based on a two-electrode set-up, and the study of a bidirectional organic thin film transistor (OTFT) for the stimulation and the recording of the bioelectrical activity of the primary neurons. In the first case, my research was focused mainly on the fabrication of gold ultra-flat surfaces for the electrodes, and the comparison with surfaces coming from industrial fabrication methods. I developed the DNA two-electrode sensor and I demonstrated its reliability in correlation with results obtained with standard three-electrodes configuration. In the second part, instead, I studied the fabrication of the organic device with perylene diimide as organic material, monitoring its resistance in function of the physiological environment and the functionality of the OTFT as recorder and stimulator of the electrogenic activity of the dorsal root ganglion neurons.

CHIM/06 Chimica organica

Novel Synthetic Procedures in Organocatalysis

Petruzziello, Diego <1984>

22 April 2013

The main aim of my PhD project was the design and the synthesis of new pyrrolidine organocatalysts. New effective ferrocenyl pyrrolidine catalysts, active in benchmark organocatalytic reactions, has been developed. The ferrocenyl moiety, in combination with simple ethyl chains, is capable of fixing the enamine conformation addressing the approach trajectory of the nucleophile in the reaction. The results obtained represent an interesting proof-of-concept, showing for the first time the remarkable effectiveness of the ferrocenyl moiety in providing enantioselectivity through conformational selection. This approach could be viably employed in the rational design of ligands for metal or organocatalysts. Other hindered secondary amines has been prepared from alkylation of acyclic chiral nitroderivatives with alcohols in a highly diastereoselective fashion, giving access to functionalized, useful organocatalytic chiral pyrrolidines. A family of new pyrrolidines bearing sterogenic centers and functional groups can be readily accessible by this methodology. The second purpose of the project was to study in deep the reactivity of stabilized carbocations in new metal-free and organocatalytic reactions. By taking advantage of the results from the kinetic studies described by Mayr, a simple and effective procedure for the direct formylation of aryltetrafluoroborate salts, has been development. The coupling of a range of aryl- and heteroaryl- trifluoroborate salts with 1,3-benzodithiolylium tetrafluoroborate, has been attempted in moderate to good yields. Finally, a simple and general methodology for the enamine-mediated enantioselective α-alkylation of α-substituted aldehydes with 1,3-benzodithiolylium tetrafluoroborate has been reported. The introduction of the benzodithiole moiety permit the installation of different functional groups due to its chameleonic behaviour.

CHIM/06 Chimica organica

Regiocontrolled Synthesis of Pyrazole Derivatives Through 1,3-Dipolar Cycloaddition Reaction And Synthesis of Helicene-Thiourea based and Polymer Supported Soos's Catalyst for Asymmetric Synthesis

Chandanshive, Jay Zumbar <1983>

22 April 2013

In first part we have developed a simple regiocontrolled protocol of 1,3-DC to get ring fused pyrazole derivatives. These pyrazole derivatives were synthesized using 1,3-DC between nitrile imine and various dipolarophiles such as alkynes, cyclic α,β-ketones, lactones, thiocatones and lactums. The reactions were found to be highly regiospecific. In second part we have discussed about helicene, its properties, synthesis and applications as asymmetric catalyst.Due to inherent chirality, herein we have made an attempt to synthesize the helicene-thiourea based catalyst for asymmetric catalysis. The synthesis involved formation of two key intermediates viz, bromo-phenanthrene 5 and a vinyl-naphthalene 10. The coupling of these two intermediates leads to formation of hexahelicene.

CHIM/06 Chimica organica