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3. Online Adaptive MR-Guided Radiotherapy (MRgRT) in UltraCentral (UC) Lung Lesions: Cumulative Delivered Dose as Assessed with Rigid Fusion (RF) Analysis Shows Significant Improvement in Clinically Relevant Parameters

Author

Bryant, J.M.M., primary, Bhandari, M., additional, Liveringhouse, C., additional, Weygand, J., additional, Cruz-Chamorro, R.J., additional, Sandoval, M.L., additional, Sim, A.J., additional, Frakes, J.M., additional, Redler, G., additional, Andreozzi, J., additional, Nardella, L., additional, Feygelman, V., additional, Latifi, K., additional, and Rosenberg, S.A., additional

Published
2022
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5. Clinical Implementation and Utility of Triggered kV Imaging During Spine Stereotactic Body Radiotherapy for Intrafraction Motion Management

Author

Koo, J., primary, Nardella, L., additional, Degnan, M., additional, Andreozzi, J., additional, Yu, H.H.M., additional, Penagaricano, J.A., additional, Johnstone, P.A.S., additional, Oliver, D.E., additional, Ahmed, K.A., additional, Rosenburg, S., additional, Wuthrick, E.J., additional, Diaz, R., additional, Feygelman, V., additional, Moros, E.G., additional, and Redler, G., additional

Published
2021
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7. The ILAILL Study: Iloprost as Adjuvant to Surgery for Acute Ischemia of Lower Limbs

Author

de Donato, Gaetano, Gussoni, Gualberto, de Donato, Gianmarco, Andreozzi, Giuseppe Maria, Bonizzoni, Erminio, Mazzone, Antonino, Odero, Attilio, Paroni, Giovanni, Setacci, Carlo, Settembrini, Piergiorgio, Veglia, Fabrizio, Martini, Romeo, Setacci, Francesco, Palombo, Domenico, de Laurentiis, R., Bianco, G., Baldi, I., Pratesi, C., Pulli, R., Romano, E., Martino, A., la Marca, G., Ebner, H., Sbraga, P., Zaraca, F., Spinelli, F., Mandolfino, T., Benedetto, F., Baccellieri, D., Ferrari, M., Adami, D., del Corso, A., Ruggieri, M., Novali, C., Mangiacotti, B., Ponzio, F., Capaldi, G., Cao, P., Parente, B., Parlani, G., Maltempi, P., Ferrero, S., Colotto, P., Nardella, L., Pastorino, S., Rauti, G., Chiesa, R., Marone, E. M., Bertoglio, C., Cristiani, A. M., Carissimi, T., Deriu, G., Antonello, Michele, Nessi, F., Cumbo, P., Ferrero, E., Mattassi, R., Callini, E., Ippoliti, A., Ascoli Marchetti, A., di Giulio, L., Spartera, C., Petrassi, C., Saracino, G., Biasi, G., Mingazzini, P., Thsomba, Y., Regina, G., Impedovo, G., Lillo, A., Angiletta, D., Marotta, V., De Donato, G, Gussoni, G, Andreozzi, Gm, Bonizzoni, E, Mazzone, A, Odero, A, Paroni, G, Setacci, C, Settembrini, P, Veglia, F, Martini, R, Setacci, F, Palombo, D, The Members of the ILAILL Study, Group, Chiesa, Roberto, Tshomba, Yamume, and Ferrari, Maurizio

Subjects
Male, Vasodilator Agents, medicine.medical_treatment, Fasciotomy, Placebos, lower limbs ischemia: surgery, Ischemia, Risk Factors, Cause of Death, Amputation, Infusions, Intravenous, Adjuvant, Treatment Outcome, Injections, Intra-Arterial, Lower Extremity, Chemotherapy, Adjuvant, Randomized, Controlled Trials, Anesthesia, Platelet aggregation inhibitor, Female, Hypotension, Intravenous, medicine.drug, Infusions, medicine.medical_specialty, Aged, Anticoagulants, Double-Blind Method, Follow-Up Studies, Heparin, Humans, Iloprost, Platelet Aggregation Inhibitors, Postoperative Hemorrhage, Surgery, Revascularization, Amputation, Surgical, Injections, medicine, Chemotherapy, acute ischemia of lower limbs, Intra-Arterial, business.industry, Perioperative, Vascular surgery, medicine.disease, business
Abstract

Acute limb ischemia (ALI) is a serious medical emergency leading to high rate of complications, being not only limb- but even life-threatening, often despite early successful revascularization.1 Improvements in surgical techniques and perioperative patient care may have reduced the incidence of major complications in ALI patients over the years, but the results of trials published recently seem to document a persistent high risk, with reported 30-day amputation rate of 5% to 12%, mortality risk at 10% to 38%, combined incidence of amputation and death of 25% to 37.5%, at 1- to 6-month follow-up.2–7 Concomitant underlying diseases, the metabolic derangement that seems as a result of the acute insult, and a possible reperfusion injury following revascularization may account for this severe prognosis.8 Only anticoagulation, fasciotomy (when indicated), and perioperative supportive treatment are established strategies in ALI patients.1,8,9 Possible benefit from cardiovascular active therapies has recently been suggested in patients undergoing peripheral revascularization or noncardiac major surgical intervention.10,11 Moreover, several categories of compounds, potentially acting on pathobiological mechanisms of ischemia-reperfusion syndrome, have been tested in experimental models, but none of them has as yet been proven effective in clinical studies in patients with ALI.12–18 Because of their pharmacologic profile, prostanoids represent a potentially interesting category as adjuvant treatment of ALI patients.19 Several ischemia-reperfusion studies described the use of prostaglandins for reduction of postischemic tissue injuries, and even recently both PGE1 and PGI2 appeared as potent inhibitors of reflow-paradox in a preclinical model of reperfusion injury.20 Iloprost is a widely studied synthetic analogue of prostacyclin, with a 10-fold higher half-life than the native compound, and indicated in the treatment of severe chronic limb ischemia.1,21–23 Results from pilot studies and case reports also described the positive effects of iloprost in the management of acute ischemia secondary to various causes, particularly after accidental intra-arterial administration of drugs or toxic agents.24–26 Several preclinical studies have assessed the effects of iloprost in experimental ischemia-reperfusion injury and documented the actions of the compound on different pathophysiologic mechanisms potentially relevant for damage following ALI.27–32 A diagram indicating where iloprost can interfere in the mechanisms, leading from ischemia and reperfusion, to the development of no-reflow and reflow-paradox, is reported in Figure 1. 33 FIGURE 1. Pathobiological mechanisms leading from ischemia-reperfusion, to “no-reflow”/“reflow-paradox.” Points where iloprost can act are indicated (from de Donato et al33). Some years ago, we performed a placebo-controlled, double-blind pilot study in 30 patients with ALI undergoing Fogarty's thromboembolectomy. Encouraging results were obtained with the use of intraoperative and postoperative iloprost (lower incidence of major clinical events, more evident metabolic improvement by means of transcutaneous tensiometry).34 In this paper, we report the results of ILoprost in Acute Ischemia of Lower Limbs (ILAILL) study, a larger, multicenter trial including patients undergoing all types of surgical revascularization, who received iloprost or placebo administration during intervention and therefore for 4 to 7 days, and were observed for a 3-month postoperative period.

Published
2006
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8. Trattamento della lussazione mediale di rotula mediante trasposizione della tuberosità tibiale nel cane: analisi retrospettiva e contributo casistico

Author

Testa A., Reale S., Drago V., Nardella L., NAVAS, LUIGI, MENNONNA, GIUSEPPINA, FATONE, GERARDO, Testa, A., Reale, S., Navas, Luigi, Drago, V., Nardella, L., Mennonna, Giuseppina, and Fatone, Gerardo

Subjects
trasposizione tuberosità tibiale, lussazione rotulea, cane
Abstract

La lussazione rotulea è un'affezione di comune riscontro nei cani di piccola taglia. Il malallineamento del meccanismo estensore del ginocchio si rende responsabile di differenti segni clinici classificati da Singleton in 4 gruppi. La Trasposizione della Tuberosità Tibiale (TTT) rappresenta uno dei diversi trattamenti chirurgici della lussazione rotulea. Lo scopo di questo studio clinico è di valutare l'efficacia della TTT ed identificare una possibile correlazione tra il grado di lussazione e la soddisfazione dei proprietari relativamente all'utilizzo dell'arto nell'immediato postoperatorio e nel follow-up successivo

Published
2008

9. Ernia Perineale nel cane: protocolli terapeutici a confronto

Author

REALE, SALVATORE, PASOLINI, MARIA PIA, LAMAGNA, BARBARA, LAMAGNA, FRANCESCO, Nardella L, Testa A, Nieddu A, Reale, Salvatore, Pasolini, MARIA PIA, Nardella, L, Testa, A, Nieddu, A, Lamagna, Barbara, and Lamagna, Francesco

Subjects
trasposizione del muscolo otturatore interno, ernia perineale, cane
Abstract

Le cause che determinano il cedimento della muscolatura del diaframma pelvico, rendendosi responsabili di ernia di organi pelvici o addominali nella regione perineale sottocutanea non sono state ancora chiarite. lo scopo del presente studio è quello di realizzare un confronto tra l'incidenza di complicanze che si determinano dopo il trattamento dell'ernia perineale con erniorraffia tradizionale e l'incidenza di complicanze secondarie al trattamento con trasposizione del muscolo otturatore interno. l'analisi dei dati in nostro possesso ha evidenziato una incidenza significativamente minore di complicanze dopo il trattamento mediante trasposizione del muscolo otturatore interno, in confronto con l'erniorraffia tradizionale

Published
2008

11. Acute limb ischemia in elderly patients: Can iloprost be useful as an adjuvant to surgery? Results from the ILAILL study

Author

de Donato G, Gussoni G, Cao P, Setacci C, Pratesi C, Mazzone A, Ferrari M, Veglia F, Bonizzoni E, Settembrini P, Ebner H, Martino A, Palombo D, Paroni G, Odero A, de Laurentiis R, Bianco G, Baldi I, Pulli R, Romano E, la Marca G, Sbraga P, Zaraca F, Spinelli F, Mandolfino T, Benedetto F, Baccellieri D, Adami D, Del Corso A, Ruggieri M, Novali C, Mangiacotti B, Ponzio F, Capaldi G, Parente B, Parlani G, Maltempi P, Ferrero S, Colotto P, Nardella L, Pastorino S, Rauti G, Marone EM, Setacci F, Bertoglio C, Caristiani AM, Carissimi T, Deriu G, Antonello M, Nessi F, Cumbo P, Ferrero E, Mattassi R, Callini E, Ippoliti A, Ascoli Marchetti A, di Giulio L, Spartera C, Petrassi C, Saracino G, Biasi G, Mingazzini P, Regina G, Impedovo G, Lillo A, Angiletta D, Marotta V., CHIESA , ROBERTO, TSHOMBA, YAMUME, de Donato, G, Gussoni, G, Cao, P, Setacci, C, Pratesi, C, Mazzone, A, Ferrari, M, Veglia, F, Bonizzoni, E, Settembrini, P, Ebner, H, Martino, A, Palombo, D, Paroni, G, Odero, A, de Laurentiis, R, Bianco, G, Baldi, I, Pulli, R, Romano, E, la Marca, G, Sbraga, P, Zaraca, F, Spinelli, F, Mandolfino, T, Benedetto, F, Baccellieri, D, Adami, D, Del Corso, A, Ruggieri, M, Novali, C, Mangiacotti, B, Ponzio, F, Capaldi, G, Parente, B, Parlani, G, Maltempi, P, Ferrero, S, Colotto, P, Nardella, L, Pastorino, S, Rauti, G, Chiesa, Roberto, Marone, Em, Setacci, F, Bertoglio, C, Caristiani, Am, Carissimi, T, Deriu, G, Antonello, M, Nessi, F, Cumbo, P, Ferrero, E, Mattassi, R, Callini, E, Ippoliti, A, Ascoli Marchetti, A, di Giulio, L, Spartera, C, Petrassi, C, Saracino, G, Biasi, G, Mingazzini, P, Tshomba, Yamume, Regina, G, Impedovo, G, Lillo, A, Angiletta, D, and Marotta, V.

Subjects
Male, medicine.medical_specialty, Time Factors, medicine.medical_treatment, Acute limb ischemia, Elderly patients, Iloprost, Reperfusion, Surgical revascularization, Acute Disease, Aged, Aged, 80 and over, Cardiovascular Agents, Chemotherapy, Adjuvant, Double-Blind Method, Extremities, Female, Humans, Incidence, Ischemia, Kaplan-Meier Estimate, Proportional Hazards Models, Risk Factors, Treatment Outcome, Amputation, Vascular Surgical Procedures, Surgery, Cardiology and Cardiovascular Medicine, Placebo, Amputation, Surgical, Bolus (medicine), medicine, 80 and over, Chemotherapy, Adjuvant, Medicine(all), business.industry, Hazard ratio, Perioperative, Acute limb ischemia, Elderly patients, Iloprost, Reperfusion, Surgical revascularization, Relative risk, Cardiovascular agent, acute limb ischemia, elderly patients, iloprost, business, medicine.drug
Abstract

Objectives To evaluate the effects of iloprost, in addition to surgery, on the outcome of acute lower limb ischemia (ALLI). Design Post-hoc analysis of a randomized, double-blind, placebo-controlled study. Methods In the context of the ILAILL (ILoprost in Acute Ischemia of Lower Limbs) study, 192 elderly patients (>70 years old) undergoing surgery for ALLI were assigned to receive perioperative iloprost (intra-arterial, intra-operative bolus of 3000ng, plus intravenous infusion of 0.5–2.0ng/kg/min for six hours/day for 4–7 days following surgery), or placebo (iloprost: n =100; placebo: n =92). Patients were followed-up for three-months following surgical revascularization. Results The combined incidence of death and amputation (primary study end-point) was significantly reduced in patients treated with iloprost (16.0% vs 27.2% in the placebo group; hazard ratio 1.99, 95% confidence interval 1.05–3.75, p =0.03). A statistically significant lower mortality (6.0%) was reported in patients receiving iloprost, compared to controls (15.2%) (hazard ratio 2.93, 1.11–7.71, p =0.03). The overall incidence of death and major cardiovascular events was lower in patients receiving iloprost compared to those assigned placebo (24.0% and 35.9%, respectively), at the limits of statistical significance (relative risk 1.64, 0.97–2.79, p =0.06). Conclusions These results confirm the poor outcome in elderly patients with ALLI. Based on a subgroup analysis iloprost, as an adjuvant to surgery, appears to reduce the combined end-point of death and amputation.

Published
2007

12. Variabili tecniche nell’esecuzione dell’anestesia tronculare dei nervi digitali palmari/plantari nel cavallo

Author

Pasolini, M. P., Fatone, G., Luigi Auletta, Potena, A., Russo, M., Nardella, L., Greco, M., Pasolini, MARIA PIA, Fatone, Gerardo, Auletta, Luigi, Potena, Agostino, M., Russo, Nardella, Laura, and Greco, Michele

Subjects
technical errors, palmar/plantar digital nerve, Perineural block
Abstract

Anatomical studies on the palmar and plantar digital nerves (NDP) distribution, clinical trials about the effectiveness of nerve blocks and the availability of modern imaging techniques in equine practice questioned the specificity and the reliability of this diagnostic ancillary test. Aim of this study was to evaluate the influence of the human error and of the operator’s skill on the results of the test; meanwhile, the utility for didactic purpose and the learning curve were evaluated, using parts of limb from slaughtered animals. One experienced (operator 3) and two untrained operators (operators 1 and 2) performed the perineural injections on 50 limbs. A score was assigned to the difficulty, the time of execution and the precision of the inoculation respectively; type and incidence of the errors occurred were also recorded. Statistical analysis of the data concerning 200 injections revealed that frequency and severity of the mistakes of operator 1 were greater both compared to the other untrained operator (operator 2) and to the experienced operator (operator 3); both inexperienced operators made more errors than the skilled operator. The most frequent error was the accidental inoculation into the digital tendon sheath; other errors occurred were the injection into the digital vein, distance of the inoculation from the nerve greater than 5 mm and a poor amount of anaesthetic. Regard to the site of injection, unskilled operators failed more often in performing perineural blocks in the hind limb. Besides, it has been observed for both the untrained operators a gradual and significant reduction in frequency and severity of the errors. Statistic analysis of data demonstrated that the human error influences the test only when performed by unskilled operators. The use of isolated limbs is a valid aid to acquire a correct skill and the learning curve is influenced by individual variable

Published
2010

13. Long-term mortality and its predictors in patients with critical leg ischemia

Author

Belgrano, Ea, Nardella, L, Ponzio, E, Nessi, E, Guala, A, Mazzucchetti, S, Graziano, L, Urban, I, Palombo, D, Brustia, P, Calzoni, D, Bellone, M, Altieri, M, Agus, Gb, De Angelis, R, Marrocu, R, Grossi, A, Frigerio, D, Biasi, Gm, Piglionica, Mr, Agrifoglio, G, Costantini, A, Della Vedova, Mr, Miglierina, L, Lavorato, E, Emanuelli, G, Rossi, R, Flandoli, C, Ponti, Gb, Berra, S, Losapio, Gm, Ambrosi, R, Inzoli, Mr, Lombardi, G, Tarantola, P, Zocca, N, Sforza, M, Russo, R, Tenchini, P, Bruni, T, Fontanili, M, Guidetti, D, Odero, A, Salvini, M, Pedeferri, G, Bordoni, Mc, Visconti, W, Vedovato, E, Bittolo Bon, G, Maffei, L, Marcon, G, Dell'Olivo, I, Gracco, L, Petralia, G, Cordiano, C, Dorucci, V, Pagnan, A, Visona', A, Tonietto, G, Agresta, E, Burigo, E, Giansante, C, Fiotti, N, Pamich, G, Santirocco, C, Mozzon, L, Gonano, N, Petrilli, Gl, Puzzo, A, Baldino, G, Podestà, A, Guastini, A, Traversaro, A, Zinicola, N, Baglietto, F, Borgatti, E, Filippini, M, Ferrari, E, Tuscano, G, Lonardi, R, Botta, Gc, Banchini, E, Pavarini, E, Delmonte, E, Bucherini, E, Moratti, A, Ieran, M, Bertini, D, Pratesi, C, Corsi, C, Pollastri, M, Marrapodi, E, Vanni, D, Ralli, L, Cecchi, M, Bigalli, A, Del Carratore, G, Mosca, E, Vatteroni, F, Setacci, C, Cao, Piergiorgio, Verzini, Fabio, Mannarino, Elmo, Pasqualini, L, Fedeli, E, Alò, E, Ioannidis, G, Spartera, C, Marino, G, Medori, M, Pola, P, Dal Lago, Aa, Di Giovanani, V, Colli, R, Maniscalco, G, Bartolo, M, Todini, Ar, Benedetti Valentini, E, Irace, L, Fiorani, P, Taurino, M, Marcialis, A, Valitutti, P, Vigliotti, G, Regina, G, Fullone, M, Rizzo, S, Rolli, E, Pascali, M, Lucentini, L, Grilli, M, Correra, H, Florena, M, Cassina, I, Notarbartolo, A, Belvedere, M, Andreozzi, Gm, Di Pino, L, Martini, R, Signorelli, S, Romeo, S, Cormaci, Of, Costanzo, C, Grasso, A, Avanzini, F, Bedoni, P, Bertele', V, Colombo, F, Fellin, G, Pangrazzi, J, Roncaglioni, Mc, Samori, G, Tognoni, G, De Gaetano, G, Garattini, S, and Tognoni, G.

Subjects
Critical leg ischaemia, Peripheral vascular disease, Mortality, Predictive variables
Published
1997

14. A prospective epidemiological survey of the natural history of chronic leg ischaemia. Evidence of the severity of prognosis and need for large-scale clinical trials

Author

Belgrano, Ea, Nardella, L, Ponzio, E, Nessi, E, Guala, A, Mazzucchetti, S, Graziano, L, Urban, I, Palombo, D, Brustia, P, Calzoni, D, Bellone, M, Altieri, M, Agus, Gb, De Angelis, R, Marrocu, R, Grossi, A, Frigerio, D, Biasi, Gm, Piglionica, Mr, Agrifoglio, G, Costantini, A, Della Vedova MR, Miglierina, L, Lavorato, E, Emanuelli, G, Rossi, R, Flandoli, C, Ponti, Gb, Berra, S, Losapio, Gm, Ambrosi, R, Inzoli, Mr, Lombardi, G, Tarantola, P, Zocca, N, Sforza, M, Russo, R, Tenchini, P, Bruni, T, Fontanili, M, Guidetti, D, Odero, A, Salvini, M, Pedeferri, G, Bordoni, Mc, Visconti, W, Vedovato, E, Bittolo Bon, G, Maffei, L, Marcon, G, Dell'Olivo, I, Gracco, L, Petralia, G, Cordiano, C, Dorucci, V, Pagnan, A, Visona', A, Tonietto, G, E Favretti E, Agresta, Burigo, E, Giansante, C, Fiotti, N, Pamich, G, Santirocco, C, Mozzon, L, Gonano, N, Petrilli, Gl, Puzzo, A, Baldino, G, Podestà, A, Guastini, A, Traversaro, A, Zinicola, N, Baglietto, F, Borgatti, E, Filippini, M, E Ridolfi Coppi G, Ferrari, Tuscano, G, Lonardi, R, Botta, Gc, Banchini, E, Pavarini, E, Delmonte, E, Bucherini, E, Moratti, A, Ieran, M, Bertini, D, Pratesi, C, Corsi, C, Pollastri, M, Marrapodi, E, Vanni, D, Ralli, L, Cecchi, M, Bigalli, A, Del Carratore, G, Mosca, E, Vatteroni, F, Setacci, C, Cao, P, Verzini, F, Mannarino, E, Pasqualini, L, Fedeli, E, Alò, E, Ioannidis, G, Spartera, C, Marino, G, Medori, M, Pola, P, Dal Lago AA, Di Giovanani, V, Colli, R, Maniscalco, G, Bartolo, M, Todini, Ar, Benedetti-Valentini, E, Irace, L, Fiorani, P, Taurino, M, Marcialis, A, Valitutti, P, Vigliotti, G, Regina, G, Fullone, M, Rizzo, S, Rolli, E, Pascali, M, Lucentini, L, Grilli, M, Correra, H, Florena, M, Cassina, I, Notarbartolo, A, Belvedere, M, Andreozzi, Gm, Di Pino, L, Martini, R, Signorelli, S, Romeo, S, Cormaci, Of, Costanzo, C, Grasso, A, Avanzini, F, Bedoni, P, Bertele', V, Colombo, F, Fellin, G, Pangrazzi, J, Roncaglioni, Mc, Samori, G, Tognoni, G, De Gaetano, G, and Garattini, S

Subjects
Epidemiology, Critical leg ischaemia, Peripheral vascular disease
Published
1996

20. [Composite bypass using endarterectomized autologous superficial femoral artery. A valid concept in the extension of lower limb salvage surgery]

Author

Sergio Ferrero, Ea, Belgrano, Nardella L, Musso L, Maiolo F, and Palladino F

Subjects
Adult, Aged, 80 and over, Male, Leg, Time Factors, Anastomosis, Surgical, Endarterectomy, Middle Aged, Blood Vessel Prosthesis, Femoral Artery, Evaluation Studies as Topic, Ischemia, Humans, Female, Saphenous Vein, Aged, Follow-Up Studies, Ultrasonography
Abstract

Saphenous vein is nowadays the material of choice performing on femoro-distal revascularisation; when this is not available, it is important to use a material which gives the closest approximation of an ideal conduit and for same time an easy handling during the execution of the anastomosis. Although vein's degenerative alterations are very rare, it has now been shown that there is widespread destruction of the endothelium among infrainguinal vein grafting, producing a relatively thrombogenic surface. These factors may contribute to the initial failure rate of these bypasses. For this reason we suggest to employ a segment of thromboendarterectomized SFA (superficial femoral artery) as a distal part of a composite bypass. Twenty-four composite bypasses were performed using three different methods over a total of 123 femoro-distal revascularizations. Eighteen months follow-up showed more than 50% and more than 75% patency rate comparing type B (graft or thromboendarterectomized SFA + autogenous saphenous vein) and type C (thromboendarterectomyied SFA + graft). We believe, waiting for a wider follow-up, that this technique could be a valid alternative to a femoro-distal revascularization when saphenous vein is not available.

22. Rationale and methodology of the ICAI study, a randomised clinical trial of alprostadil in the treatment of chronic critical leg ischemia

Author

Belgrano, Ea, Nardella, L., Guala, A., Mazzucchetti, S., Marinoni, V., Calzoni, D., Bedoni, P., Confalonieri, Ma, Agus, Gb, Mondani, P., Deangelis, R., Biasi, Gm, Piglionica, MR, Abbritti, F., Agrifoglio, G., Costantini, A., DellaVedova, MR, Miglierina, L., Marrocu, R., Bragherio, G., Zanoni, Ce, Borin, F., Alderi, G., Emanuelli, G., Flandoli, C., Colzani, M., Ponti, Gb, Berra, S., Bevilacqua, A., Bocca, M., Invernizzi, C., Deangelis, E., Tacconi, A., Dangelo, F., Vaghi, M., Arzini, A., Boccalon, L., Losapio, Gm, Ambrosi, R., Briolini, F., Inzoli, MR, Lombardi, G., Tarantola, P., Zocca, N., Tenchini, P., Bruni, T., Fontanili, M., Guidetti, D., Pedeferri, G., Bordoni, Mc, Catalano, A., Visconti, W., Vedovato, F., Zucchella, M., Bittolo, Bg, Busetto, Mt, Zambon, C., Carlassara, Gb, Barbato, O., Zambelli, V., Mazzilli, G., Lino, M., Pavan, S., Pagnan, A., Visona, A., Perissinotto, C., Tonietto, G., Michelet, I., Agresta, F., Favretti, F., Burigo, E., Delazzer, L., Giansante, C., Fiotti, N., Grego, S., Mozzon, L., Gonano, N., Pfeiffer, P., Petrilli, Gl, Puzzo, A., Giuseppe Baldino, Podesta, A., Guastini, A., Traversaro, A., Zinicola, N., Baglietto, F., Arnuzzo, L., Defabritiis, A., Filippini, M., Ferrari, F., Martini, L., Testoni, P., Accorsi, F., Maurizi, P., Evangelisti, G., Roffi, A., Marzara, G., Fini, C., Coppi, G., Camparini, S., Tusini, N., Tuscano, G., Lonardi, R., Rozza, A., Botta, Gc, Villani, Lg, Pavarini, E., Campanella, P., Moratti, A., Ieran, M., Bertini, D., Pratesi, C., Narcetti, S., Corsi, C., Pollastri, M., Marrapodi, E., Melillo, E., Iabichella, Ml, Setacci, C., Sozio, G., Cao, P., Verzini, F., Mannarino, E., Pasqualini, L., Vaudo, G., Alo, F., Ioannidis, G., Spartera, C., Marino, G., Bafile, G., Anselmi, E., Maniscalco, G., Longo, P., Digiovanni, V., Colli, R., Fabbri, Mc, Bracale, G., Bernardo, B., Perretti, B., Valitutti, P., Vigliotti, G., Cimino, G., Rolli, F., Pascali, M., Sabella, G., Grilli, M., Correra, M., Palese, E., Florena, M., Cassina, I., Cumbo, P., Comande, C., Notarbartolo, A., Novo, S., Belvedere, M., Caruso, R., Verghi, F., Cavallaro, S., Martello, G., Romeo, S., Cormaci, Of, Binaghi, F., Fronteddu, P., Cannas, F., Degaetano, G., Tognoni, G., Avanzini, F., Bertele, V., Digiulio, P., Pangrazzi, J., Roncaglioni, Mc, Colombo, F., Fellin, G., Terzian, E., Coccheri, S., Delfavero, A., Geraci, E., Janzon, L., Vermylen, J., Beghi, E., Coen, D., and Turazza, F.

23. Wee1 Rather Than Plk1 Is Inhibited by AZD1775 at Therapeutically Relevant Concentrations

Author

Rosa Della Monica, Roberta Visconti, Domenico Grieco, Giuseppe D'Alterio, Angela Flavia Serpico, Luca Nardella, Cinzia Vetrei, Serpico, A. F., D'Alterio, G., Vetrei, C., Monica, R. D., Nardella, L., Visconti, R., and Grieco, D.

Subjects
0301 basic medicine, Cancer Research, concentration range, Wee1 inhibitor, PLK1, lcsh:RC254-282, Article, Plk1 inhibitor, combination therapy, 03 medical and health sciences, 0302 clinical medicine, Cyclin-dependent kinase, Mitotic catastrophe, Mitosis, Cyclin-dependent kinase 1, biology, Kinase, Chemistry, DNA replication checkpoint, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Wee1, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer cell, biology.protein, Cancer research
Abstract

Wee1 kinase is an inhibitor of cyclin-dependent kinase (cdk)s, crucial cell cycle progression drivers. By phosphorylating cdk1 at tyrosine 15, Wee1 inhibits activation of cyclin B-cdk1 (Cdk1), preventing cells from entering mitosis with incompletely replicated or damaged DNA. Thus, inhibiting Wee1, alone or in combination with DNA damaging agents, can kill cancer cells by mitotic catastrophe, a tumor suppressive response that follows mitosis onset in the presence of under-replicated or damaged DNA. AZD1775, an orally available Wee1 inhibitor, has entered clinical trials for cancer treatment following this strategy, with promising results. Recently, however, AZD1775 has been shown to inhibit also the polo-like kinase homolog Plk1 in vitro, casting doubts on its mechanism of action. Here we asked whether, in the clinically relevant concentration range, AZD1775 inhibited Wee1 or Plk1 in transformed and non-transformed human cells. We found that in the clinically relevant, nanomolar, concentration range AZD1775 inhibited Wee1 rather than Plk1. In addition, AZD1775 treatment accelerated mitosis onset overriding the DNA replication checkpoint and hastened Plk1-dependent phosphorylation. On the contrary selective Plk1 inhibition exerted opposite effects. Thus, at therapeutic concentrations, AZD1775 inhibited Wee1 rather than Plk1. This information will help to better interpret results obtained by using AZD1775 both in the clinical and experimental settings and provide a stronger rationale for combination therapies.

Published
2019
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24. Nucleoporin 153 deficiency in adult neural stem cells defines a pathological protein-network signature and defective neurogenesis in a mouse model of AD.

Author

Colussi C, Bertozzi A, Leone L, Rinaudo M, Sollazzo R, Conte F, Paccosi E, Nardella L, Aceto G, Li Puma DD, Ripoli C, Vita MG, Marra C, D'Ascenzo M, and Grassi C

Subjects
Animals, Humans, Mice, Hippocampus metabolism, Induced Pluripotent Stem Cells metabolism, Induced Pluripotent Stem Cells cytology, Proteomics, Alzheimer Disease metabolism, Alzheimer Disease genetics, Alzheimer Disease pathology, Disease Models, Animal, Neural Stem Cells metabolism, Neural Stem Cells cytology, Neurogenesis, Nuclear Pore Complex Proteins metabolism, Nuclear Pore Complex Proteins genetics
Abstract

Background: Reduction of adult hippocampal neurogenesis is an early critical event in Alzheimer's disease (AD), contributing to progressive memory loss and cognitive decline. Reduced levels of the nucleoporin 153 (Nup153), a key epigenetic regulator of NSC stemness, characterize the neural stem cells isolated from a mouse model of AD (3×Tg) (AD-NSCs) and determine their altered plasticity and gene expression., Methods: Nup153-regulated mechanisms contributing to NSC function were investigated: (1) in cultured NSCs isolated from AD and wild type (WT) mice by proteomics; (2) in vivo by lentiviral-mediated delivery of Nup153 or GFP in the hippocampus of AD and control mice analyzing neurogenesis and cognitive function; (3) in human iPSC-derived brain organoids obtained from AD patients and control subjects as a model of neurodevelopment., Results: Proteomic approach identified Nup153 interactors in WT- and AD-NSCs potentially implicated in neurogenesis regulation. Gene ontology (GO) analysis showed that Nup153-bound proteins in WT-NSCs were involved in RNA metabolism, nuclear import and epigenetic mechanisms. Nup153-bound proteins in AD-NSCs were involved in pathways of neurodegeneration, mitochondrial dysfunction, proteasomal processing and RNA degradation. Furthermore, recovery of Nup153 levels in AD-NSCs reduced the levels of oxidative stress markers and recovered proteasomal activity. Lentiviral-mediated delivery of Nup153 in the hippocampal niche of AD mice increased the proliferation of early progenitors, marked by BrdU/DCX and BrdU/PSANCAM positivity and, later, the integration of differentiating neurons in the cell granule layer (BrdU/NeuN + cells) compared with GFP-injected AD mice. Consistently, Nup153-injected AD mice showed an improvement of cognitive performance in comparison to AD-GFP mice at 1 month after virus delivery assessed by Morris Water Maze. To validate the role of Nup153 in neurogenesis we took advantage of brain organoids derived from AD-iPSCs characterized by fewer neuroepithelial progenitor loops and reduced differentiation areas. The upregulation of Nup153 in AD organoids recovered the formation of neural-like tubes and differentiation., Conclusions: Our data suggest that the positive effect of Nup153 on neurogenesis is based on a complex regulatory network orchestrated by Nup153 and that this protein is a valuable disease target., (© 2024. The Author(s).)

Published
2024
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25. Glycine-induced activation of GPR158 increases the intrinsic excitability of medium spiny neurons in the nucleus accumbens.

Author

Aceto G, Nardella L, Nanni S, Pecci V, Bertozzi A, Nutarelli S, Viscomi MT, Colussi C, D'Ascenzo M, and Grassi C

Subjects
Animals, Male, Mice, Mice, Inbred C57BL, Receptors, Glycine metabolism, Patch-Clamp Techniques, Phosphorylation drug effects, Medium Spiny Neurons, Glycine pharmacology, Glycine metabolism, Nucleus Accumbens metabolism, Nucleus Accumbens drug effects, Nucleus Accumbens cytology, Neurons metabolism, Neurons drug effects, Receptors, G-Protein-Coupled metabolism, Action Potentials drug effects
Abstract

It has been recently established that GPR158, a class C orphan G protein-coupled receptor, serves as a metabotropic glycine receptor. GPR158 is highly expressed in the nucleus accumbens (NAc), a major input structure of the basal ganglia that integrates information from cortical and subcortical structures to mediate goal-directed behaviors. However, whether glycine modulates neuronal activity in the NAc through GPR158 activation has not been investigated yet. Using whole-cell patch-clamp recordings, we found that glycine-dependent activation of GPR158 increased the firing rate of NAc medium spiny neurons (MSNs) while it failed to significantly affect the excitability of cholinergic interneurons (CIN). In MSNs GPR158 activation reduced the latency to fire, increased the action potential half-width, and reduced action potential afterhyperpolarization, effects that are all consistent with negative modulation of potassium M-currents, that in the central nervous system are mainly carried out by Kv7/KCNQ-channels. Indeed, we found that the GPR158-induced increase in MSN excitability was associated with decreased M-current amplitude, and selective pharmacological inhibition of the M-current mimicked and occluded the effects of GPR158 activation. In addition, when the protein kinase A (PKA) or extracellular signal-regulated kinase (ERK) signaling was pharmacologically blocked, modulation of MSN excitability by GPR158 activation was suppressed. Moreover, GPR158 activation increased the phosphorylation of ERK and Kv7.2 serine residues. Collectively, our findings suggest that GPR158/PKA/ERK signaling controls MSN excitability via Kv7.2 modulation. Glycine-dependent activation of GPR158 may significantly affect MSN firing in vivo, thus potentially mediating specific aspects of goal-induced behaviors., (© 2024. The Author(s).)

Published
2024
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26. Structure-specific rigid dose accumulation dosimetric analysis of ablative stereotactic MRI-guided adaptive radiation therapy in ultracentral lung lesions.

Author

Bryant JM, Cruz-Chamorro RJ, Gan A, Liveringhouse C, Weygand J, Nguyen A, Keit E, Sandoval ML, Sim AJ, Perez BA, Dilling TJ, Redler G, Andreozzi J, Nardella L, Naghavi AO, Feygelman V, Latifi K, and Rosenberg SA

Abstract

Background: Definitive local therapy with stereotactic ablative radiation therapy (SABR) for ultracentral lung lesions is associated with a high risk of toxicity, including treatment related death. Stereotactic MR-guided adaptive radiation therapy (SMART) can overcome many of the challenges associated with SABR treatment of ultracentral lesions., Methods: We retrospectively identified 14 consecutive patients who received SMART to ultracentral lung lesions from 10/2019 to 01/2021. Patients had a median distance from the proximal bronchial tree (PBT) of 0.38 cm. Tumors were most often lung primary (64.3%) and HILUS group A (85.7%). A structure-specific rigid registration approach was used for cumulative dose analysis. Kaplan-Meier log-rank analysis was used for clinical outcome data and the Wilcoxon Signed Rank test was used for dosimetric data., Results: Here we show that SMART dosimetric improvements in favor of delivered plans over predicted non-adapted plans for PBT, with improvements in proximal bronchial tree DMax of 5.7 Gy (p = 0.002) and gross tumor 100% prescription coverage of 7.3% (p = 0.002). The mean estimated follow-up is 17.2 months and 2-year local control and local failure free survival rates are 92.9% and 85.7%, respectively. There are no grade ≥ 3 toxicities., Conclusions: SMART has dosimetric advantages and excellent clinical outcomes for ultracentral lung tumors. Daily plan adaptation reliably improves target coverage while simultaneously reducing doses to the proximal airways. These results further characterize the therapeutic window improvements for SMART. Structure-specific rigid dose accumulation dosimetric analysis provides insights that elucidate the dosimetric advantages of SMART more so than per fractional analysis alone., (© 2024. The Author(s).)

Published
2024
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27. Magnetic Resonance-Guided Stereotactic Body Radiation Therapy/Hypofractionated Radiation therapy for Metastatic and Primary Central and Ultracentral Lung Lesions.

Author

Sandoval ML, Sim AJ, Bryant JM, Bhandari M, Wuthrick EJ, Perez BA, Dilling TJ, Redler G, Andreozzi J, Nardella L, Feygelman V, Latifi K, and Rosenberg SA

Abstract

Introduction: The recent results from the Nordic-HILUS study indicate stereotactic body radiation therapy (SBRT) is associated with high-grade toxicity for ultracentral (UC) tumors. We hypothesized that magnetic resonance-guided SBRT (MRgSBRT) or hypofractionated radiation therapy (MRgHRT) enables the safe delivery of high-dose radiation to central and UC lung lesions., Methods: Patients with UC or central lesions were treated with MRgSBRT/MRgHRT with real-time gating or adaptation. Central lesions were defined as per the Radiation Therapy Oncology Group and UC as per the HILUS study definitions: (1) group A or tumors less than 1 cm from the trachea and/or mainstem bronchi; or (2) group B or tumors less than 1 cm from the lobar bronchi. The Kaplan-Meier estimate and log-rank test were used to estimate survival. Associations between toxicities and other patient factors were tested using the Mann-Whitney U test and Fisher's exact test., Results: A total of 47 patients were included with a median follow-up of 22.9 months (95% confidence interval: 16.4-29.4). Most (53%) had metastatic disease. All patients had central lesions and 55.3% (n = 26) had UC group A. The median distance from the proximal bronchial tree was 6.0 mm (range: 0.0-19.0 mm). The median biologically equivalent dose (α/β = 10) was 105 Gy (range: 75-151.2). The most common radiation schedule was 60 Gy in eight fractions (40.4%). Most (55%) had previous systemic therapy, 32% had immunotherapy and 23.4% had previous thoracic radiation therapy. There were 16 patients who underwent daily adaptation. The 1-year overall survival was 82% (median = not reached), local control 87% (median = not reached), and progression-free survival 54% (median = 15.1 mo, 95% confidence interval: 5.1-25.1). Acute toxicity included grade 1 (26%) and grade 2 (21%) with only two patients experiencing grade 3 (4.3%) in the long term. No grade 4 or 5 toxicities were seen., Conclusions: Previous studies noted high rates of toxicity after SBRT to central and UC lung lesions, with reports of grade 5 toxicities. In our cohort, the use of MRgSBRT/MRgHRT with high biologically effective doses was well tolerated, with two grade 3 toxicities and no grade 4/5., (© 2023 The Authors.)

Published
2023
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28. Acute restraint stress impairs histamine type 2 receptor ability to increase the excitability of medium spiny neurons in the nucleus accumbens.

Author

Aceto G, Nardella L, Lazzarino G, Tavazzi B, Bertozzi A, Nanni S, Colussi C, D'Ascenzo M, and Grassi C

Subjects
Mice, Animals, Action Potentials physiology, Medium Spiny Neurons, Patch-Clamp Techniques, Nucleus Accumbens, Histamine
Abstract

Histamine, a monoamine implicated in stress-related arousal states, is synthesized in neurons exclusively located in the hypothalamic tuberomammillary nucleus (TMN) from where they diffusely innervate striatal and mesolimbic networks including the nucleus accumbens (NAc), a vital node in the limbic loop. Since histamine-containing TMN neuron output increases during stress, we hypothesized that exposure of mice to acute restrain stress (ARS) recruits endogenous histamine type 2 receptor (H2R) signaling in the NAc, whose activation increases medium spiny neurons (MSNs) intrinsic excitability via downregulation of A-type K + currents. We employed an ARS paradigm in which mice were restrained for 120 min, followed by a 20-min recovery period, after which brain slices were prepared for ex vivo electrophysiology. Using whole-cell patch-clamp recordings, we found that pharmacological activation of H2R failed to affect MSN excitability and A-type K + currents in mice that underwent ARS. Interestingly, in mice treated with H2R-antagonist prior to ARS paradigm, H2R activation increased evoked firing and decreased A-type K + currents similarly to what observed in control mice. Furthermore, H2R-antagonist treatment ameliorated anxiety-like behavior in ARS mice. Together, our findings indicate that ARS paradigm recruits endogenous H2R signaling in MSNs and suggest the involvement of H2R signaling in stress-related motivational states., Competing Interests: Declaration of competing interest All authors declare that the research was conducted in the absence of any commercial and financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2022
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29. Activation of histamine type 2 receptors enhances intrinsic excitability of medium spiny neurons in the nucleus accumbens.

Author

Aceto G, Nardella L, Nanni S, Pecci V, Bertozzi A, Colussi C, D'Ascenzo M, and Grassi C

Subjects
Cyclic AMP-Dependent Protein Kinases metabolism, Neurons physiology, Receptors, Histamine H2, Histamine pharmacology, Nucleus Accumbens physiology
Abstract

Histaminergic neurons are exclusively located in the hypothalamic tuberomammillary nucleus, from where they project to many brain areas including the nucleus accumbens (NAc), a brain area that integrates diverse monoaminergic inputs to coordinate motivated behaviours. While the NAc expresses various histamine receptor subtypes, the mechanisms by which histamine modulates NAc activity are still poorly understood. Using whole-cell patch-clamp recordings, we found that pharmacological activation of histamine 2 (H2) receptors elevates the excitability of NAc medium spiny neurons (MSNs), while activation of H1 receptors failed to significantly affect MSN excitability. The evoked firing of MSNs increased after seconds of local H2 agonist administration and remained elevated for minutes. H2 receptor (H2R) activation accelerated subthreshold depolarization in response to current injection, reduced the latency to fire, diminished action potential afterhyperpolarization and increased the action potential half-width. The increased excitability was protein kinase A-dependent and associated with decreased A-type K + currents. In addition, selective pharmacological inhibition of the Kv4.2 channel, the main molecular determinant of A-type K + currents in MSNs, mimicked and occluded the increased excitability induced by H2R activation. Our results indicate that histaminergic transmission in the NAc increases MSN intrinsic excitability through H2R-dependent modulation of Kv4.2 channels. Activation of H2R will significantly alter spike firing in MSNs in vivo, and this effect could be an important mechanism by which these receptors mediate certain aspects of goal-induced behaviours. KEY POINTS: Histamine is synthesized and released by hypothalamic neurons of the tuberomammillary nucleus and serves as a general modulator for whole-brain activity including the nucleus accumbens. Histamine receptors type 2 (HR2), which are expressed in the nucleus accumbens, couple to Gαs/off proteins which elevate cyclic adenosine monophosphate levels and activate protein kinase A. Whole-cell patch-clamp recordings revealed that H2R activation increased the evoked firing in medium spiny neurons of the nucleus accumbens via protein kinase A-dependent mechanisms. HR2 activation accelerated subthreshold depolarization in response to current injection, reduced the latency to fire, diminished action potential medium after-hyperpolarization and increased the action potential half-width. HR2 activation also reduced A-type potassium current. Selective pharmacological inhibition of the Kv4.2 channel mimicked and occluded the increased excitability induced by H2R activation., (© 2022 The Authors. The Journal of Physiology published by John Wiley & Sons Ltd on behalf of The Physiological Society.)

Published
2022
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30. Triggered kV Imaging During Spine SBRT for Intrafraction Motion Management.

Author

Koo J, Nardella L, Degnan M, Andreozzi J, Yu HM, Penagaricano J, Johnstone PAS, Oliver D, Ahmed K, Rosenberg SA, Wuthrick E, Diaz R, Feygelman V, Latifi K, Moros EG, and Redler G

Subjects
Humans, Image Processing, Computer-Assisted, Imaging, Three-Dimensional, Particle Accelerators, Phantoms, Imaging, Radiotherapy Dosage, Radiotherapy, Image-Guided standards, Radiotherapy, Intensity-Modulated adverse effects, Radiotherapy, Intensity-Modulated standards, Tomography, X-Ray Computed, Dose Fractionation, Radiation, Motion, Radiotherapy Planning, Computer-Assisted methods, Radiotherapy, Image-Guided methods, Radiotherapy, Intensity-Modulated methods, Spine diagnostic imaging, Spine radiation effects
Abstract

Purpose: To monitor intrafraction motion during spine stereotactic body radiotherapy(SBRT) treatment delivery with readily available technology, we implemented triggered kV imaging using the on-board imager(OBI) of a modern medical linear accelerator with an advanced imaging package. Methods: Triggered kV imaging for intrafraction motion management was tested with an anthropomorphic phantom and simulated spine SBRT treatments to the thoracic and lumbar spine. The vertebral bodies and spinous processes were contoured as the image guided radiotherapy(IGRT) structures specific to this technique. Upon each triggered kV image acquisition, 2D projections of the IGRT structures were automatically calculated and updated at arbitrary angles for display on the kV images. Various shifts/rotations were introduced in x, y, z, pitch, and yaw. Gantry-angle-based triggering was set to acquire kV images every 45°. A group of physicists/physicians(n = 10) participated in a survey to evaluate clinical efficiency and accuracy of clinical decisions on images containing various phantom shifts. This method was implemented clinically for treatment of 42 patients(94 fractions) with 15 second time-based triggering. Result: Phantom images revealed that IGRT structure accuracy and therefore utility of projected contours during triggered imaging improved with smaller CT slice thickness. Contouring vertebra superior and inferior to the treatment site was necessary to detect clinically relevant phantom rotation. From the survey, detectability was proportional to the shift size in all shift directions and inversely related to the CT slice thickness. Clinical implementation helped evaluate robustness of patient immobilization. Based on visual inspection of projected IGRT contours on planar kV images, appreciable intrafraction motion was detected in eleven fractions(11.7%). Discussion: Feasibility of triggered imaging for spine SBRT intrafraction motion management has been demonstrated in phantom experiments and implementation for patient treatments. This technique allows efficient, non-invasive monitoring of patient position using the OBI and patient anatomy as a direct visual guide.

Published
2021
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31. Wee1 Rather Than Plk1 Is Inhibited by AZD1775 at Therapeutically Relevant Concentrations.

Author

Serpico AF, D'Alterio G, Vetrei C, Della Monica R, Nardella L, Visconti R, and Grieco D

Abstract

Wee1 kinase is an inhibitor of cyclin-dependent kinase (cdk)s, crucial cell cycle progression drivers. By phosphorylating cdk1 at tyrosine 15, Wee1 inhibits activation of cyclin B-cdk1 (Cdk1), preventing cells from entering mitosis with incompletely replicated or damaged DNA. Thus, inhibiting Wee1, alone or in combination with DNA damaging agents, can kill cancer cells by mitotic catastrophe, a tumor suppressive response that follows mitosis onset in the presence of under-replicated or damaged DNA. AZD1775, an orally available Wee1 inhibitor, has entered clinical trials for cancer treatment following this strategy, with promising results. Recently, however, AZD1775 has been shown to inhibit also the polo-like kinase homolog Plk1 in vitro, casting doubts on its mechanism of action. Here we asked whether, in the clinically relevant concentration range, AZD1775 inhibited Wee1 or Plk1 in transformed and non-transformed human cells. We found that in the clinically relevant, nanomolar, concentration range AZD1775 inhibited Wee1 rather than Plk1. In addition, AZD1775 treatment accelerated mitosis onset overriding the DNA replication checkpoint and hastened Plk1-dependent phosphorylation. On the contrary selective Plk1 inhibition exerted opposite effects. Thus, at therapeutic concentrations, AZD1775 inhibited Wee1 rather than Plk1. This information will help to better interpret results obtained by using AZD1775 both in the clinical and experimental settings and provide a stronger rationale for combination therapies.

Published
2019
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32. [Immediate reocclusion of the infrapopliteal segment after thrombolysis in acute ischemia of the lower limb of the thrombotic nature].

Author

Belgrano EA, Nardella L, and Palladino F

Subjects
Acute Disease, Aged, Blood Vessel Prosthesis adverse effects, Evaluation Studies as Topic, Female, Fibrinolytic Agents administration & dosage, Heparin administration & dosage, Humans, Infusions, Intravenous, Ischemia etiology, Ischemia surgery, Male, Plasminogen Activators administration & dosage, Recurrence, Thrombosis complications, Tissue Plasminogen Activator administration & dosage, Urokinase-Type Plasminogen Activator administration & dosage, Ischemia drug therapy, Leg blood supply, Thrombolytic Therapy
Abstract

Early reocclusion of below knee segment after fibrinolytic therapy is mainly due to thrombo-embolism, coagulopathy or to the arterial wall condition. 42 patients facing acute lower limb ischaemia because of iliofemoral thrombosis (prosthesis 19, native artery 23) underwent locoregional thrombolysis. UK was given in 33 cases while the others received rt-PA. The early reocclusion after fibrinolysis leads to a serious worsening in these patients; thrombosis in distal vessels and in microvasculature make any surgical approach unserviceable. Major amputation was required in 3 cases. We believe that fibrinolytic treatment has taken on great importance in making accurate diagnosing of thromboembolism and, once restored patency of distal vessels, allows to perform revascularization procedures.

Published
1995

33. [Composite bypass using endarterectomized autologous superficial femoral artery. A valid concept in the extension of lower limb salvage surgery].

Author

Ferrero S, Belgrano EA, Nardella L, Musso L, Maiolo F, and Palladino F

Subjects
Adult, Aged, Aged, 80 and over, Anastomosis, Surgical, Evaluation Studies as Topic, Female, Follow-Up Studies, Humans, Ischemia surgery, Male, Middle Aged, Time Factors, Ultrasonography, Blood Vessel Prosthesis, Endarterectomy, Femoral Artery transplantation, Leg blood supply, Saphenous Vein transplantation
Abstract

Saphenous vein is nowadays the material of choice performing on femoro-distal revascularisation; when this is not available, it is important to use a material which gives the closest approximation of an ideal conduit and for same time an easy handling during the execution of the anastomosis. Although vein's degenerative alterations are very rare, it has now been shown that there is widespread destruction of the endothelium among infrainguinal vein grafting, producing a relatively thrombogenic surface. These factors may contribute to the initial failure rate of these bypasses. For this reason we suggest to employ a segment of thromboendarterectomized SFA (superficial femoral artery) as a distal part of a composite bypass. Twenty-four composite bypasses were performed using three different methods over a total of 123 femoro-distal revascularizations. Eighteen months follow-up showed more than 50% and more than 75% patency rate comparing type B (graft or thromboendarterectomized SFA + autogenous saphenous vein) and type C (thromboendarterectomyied SFA + graft). We believe, waiting for a wider follow-up, that this technique could be a valid alternative to a femoro-distal revascularization when saphenous vein is not available.

Published
1991

34. Aneurysm of the abdominal aorta in a young woman. Atherosclerotic or inflammatory in origin?

Author

Nardella L, Belgrano EA, Palladino F, and Ferraro S

Subjects
Adult, Aorta, Abdominal, Female, Humans, Aortic Aneurysm etiology, Arteriosclerosis complications, Retroperitoneal Fibrosis complications
Abstract

The case is described of a 27 year old woman with aneurysms of the abdominal aorta. In the absence of any signs of atherosclerotic disease, an inflammatory aetiology was suspected, a view that was supported by the macroscopic intraoperative findings and preoperative autoimmune assays. The literature on this rare pathology is examined.

Published
1988

38. [Indications and treatment of popliteal aneurysm].

Author

Ferrero S, Belgrano EA, Nardella L, and Palladino F

Subjects
Aged, Aneurysm complications, Gangrene, Humans, Leg blood supply, Male, Middle Aged, Aneurysm surgery, Popliteal Artery surgery
Published
1986

39. [Severe chronic ischemia of the limbs. A retrospective study and check of the results].

Author

Belgrano EA, Nardella L, Palladino F, and Ferrero S

Subjects
Adult, Aged, Amputation, Surgical, Arterial Occlusive Diseases complications, Arterial Occlusive Diseases mortality, Arterial Occlusive Diseases surgery, Chronic Disease, Endarterectomy, Female, Humans, Ischemia etiology, Ischemia mortality, Leg surgery, Male, Middle Aged, Retrospective Studies, Ischemia surgery, Leg blood supply
Published
1989

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