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23. The Italian multi-centre project on evaluation of MRI and other imaging modalities in early detection of breast cancer in subjects at high genetic risk

Author

Podo, F, Sardanelli, F, Canese, R, D'agnolo, G, Natali, Pg, Crecco, M, Grandinetti, Ml, Musumeci, R, Trecate, G, Bergonzi, S, De Simone, T, Costa, C, Pasini, B, Manuokian, S, Spatti, Gb, Vergnaghi, D, Morassut, S, Boiocchi, M, Dolcetti, R, Viel, A, De Giacomi, C, Veronesi, A, Coran, F, Silingardi, V, Turchett, D, Cortesi, L, De Santis, M, Federico, M, Romagnoli, R, Ferrari, S, Bevilacqua, G, Bartolozzi, C, Caligo, Ma, Cilotti, A, Marini, C, Cirillo, S, Marra, V, Martincich, L, Contegiacomo, A, Pensabene, M, Capuano, I, Burgazzi, Gb, Petrillo, A, Bonomo, L, Carriero, A, Mariani-costantini, R, Battista, P, Cama, A, Palca, G, Nullc, Di, Maggio, C, D'andrea, E, Bazzocchi, M, Francescutti, Ge, Zuiani, C, Londero, V, Zunnui, I, Gustavino, C, Centurioni, Mg, Iozzelli, A, Panizza, P, DEL MASCHIO, ALESSANDRO, Podo, F, Sardanelli, F, Canese, R, D'Agnolo, G, Natali, Pg, Crecco, M, Grandinetti, Ml, Musumeci, R, Trecate, G, Bergonzi, S, De Simone, T, Costa, C, Pasini, B, Manuokian, S, Spatti, Gb, Vergnaghi, D, Morassut, S, Boiocchi, M, Dolcetti, R, Viel, A, De Giacomi, C, Veronesi, A, Coran, F, Silingardi, V, Turchett, D, Cortesi, L, De Santis, M, Federico, M, Romagnoli, R, Ferrari, S, Bevilacqua, G, Bartolozzi, C, Caligo, Ma, Cilotti, A, Marini, C, Cirillo, S, Marra, V, Martincich, L, Contegiacomo, A, Pensabene, M, Capuano, I, Burgazzi, Gb, Petrillo, A, Bonomo, L, Carriero, A, Mariani-costantini, R, Battista, P, Cama, A, Palca, G, Nullc, Di, Maggio, D'Andrea, E, Bazzocchi, M, Francescutti, Ge, Zuiani, C, Londero, V, Zunnui, I, Gustavino, C, Centurioni, Mg, Iozzelli, A, Panizza, P, and DEL MASCHIO, Alessandro

Published
2002

24. Comment on 'Cancer genetic counselling' by P. Mandich et al

Author

Contegiacomo, A, Pensabene, M, Capuano, I, Tauchmanova, L, Federico, Massimo, Turchetti, D, Cortesi, L, Marchetti, P, Ricevuto, E, Cianci, G, Barbieri, Viola, Venuta, S, and Silingardi, Vittorio

Subjects
genetic counselling, Mandich, cancer
Published
2005

25. Anaemia in CKD 1-5

Author

Hirata, M., primary, Tashiro, Y., additional, Aizawa, K., additional, Endo, K., additional, Hirata, M., additional, Serizawa, K., additional, Yogo, K., additional, Cases, A., additional, Portoles, J., additional, Calls, J., additional, Martinez-Castelao, A., additional, Munar, M. A., additional, Segarra, A., additional, Samouilidou, E., additional, Pantelias, K., additional, Petras, D., additional, Mpakirtzi, T., additional, Pipili, C., additional, Chatzivasileiou, G., additional, Vasiliou, K., additional, Denda, E., additional, Grapsa, E., additional, Tzanatos, H., additional, Shoji, S., additional, Inaba, M., additional, Tomosugi, N., additional, Okuno, S., additional, Ichii, M., additional, Yamakawa, T., additional, Kurihara, S., additional, Barsan, L., additional, Stanciu, A., additional, Stancu, S., additional, Capusa, C., additional, Bratescu, L., additional, Mircescu, G., additional, Kuo, K.-L., additional, Hung, S.-C., additional, Lee, T.-S., additional, Tarng, D.-C., additional, Nistor, I., additional, Covic, A., additional, Goldsmith, D., additional, Garrido, P., additional, Fernandes, J., additional, Ribeiro, S., additional, Vala, H., additional, Parada, B., additional, Alves, R., additional, Belo, L., additional, Costa, E., additional, Santos-Silva, A., additional, Reis, F., additional, Abdulnabi, K., additional, Ullah, A., additional, Abdulateef, A., additional, Howse, M., additional, Khalil, A., additional, Fouqueray, B., additional, Hoffmann, M., additional, Addison, J., additional, Manamley, N., additional, Stamopoulos, D., additional, Mpakirtzi, N., additional, Afentakis, N., additional, Yu, K.- H., additional, Chou, J., additional, Klaus, S., additional, Schaddelee, M., additional, Kashiwa, M., additional, Takada, A., additional, Neff, T., additional, Galle, J., additional, Claes, K., additional, Di Giulio, S., additional, Guerin, A., additional, Herlitz, H., additional, Kiss, I., additional, Wirnsberger, G., additional, Froissart, M., additional, Winearls, C., additional, Martinez Castelao, A., additional, Cases Amenos, A., additional, Torre Carballada, A., additional, Torralba Iranzo, F. J., additional, Bronsoms Artero, J. M., additional, Toran Monserrat, D., additional, Valles Prats, M., additional, Merino, J. L., additional, Espejo, B., additional, Bueno, B., additional, Amezquita, Y., additional, Paraiso, V., additional, Kiss, Z., additional, Kerkovits, L., additional, Ambrus, C., additional, Kulcsar, I., additional, Szegedi, J., additional, Benke, A., additional, Borbas, B., additional, Ferenczi, S., additional, Hengsperger, M., additional, Kazup, S., additional, Nagy, L., additional, Nemeth, J., additional, Rozinka, A., additional, Szabo, T., additional, Szelestei, T., additional, Toth, E., additional, Varga, G., additional, Wagner, G., additional, Zakar, G., additional, Gergely, L., additional, Exarchou, K., additional, Tanahill, N., additional, Anthoney, A., additional, Ahmed, S., additional, Oprican, R., additional, Lipan, M., additional, Chirculescu, B., additional, Roger, S., additional, Malecki, R., additional, Farouk, M., additional, Dellanna, F., additional, Thomas, M., additional, Touam, M., additional, Chantrel, F., additional, Bouiller, M., additional, Hurot, J.-M., additional, Raphael, T., additional, Testa, A., additional, Veillon, S., additional, Vendrely, B., additional, Masoumi, Z., additional, Ahmadpoor, P., additional, Ghaderian, S. M. H., additional, Nafar, M., additional, Samavat, S., additional, Samadian, F., additional, Poorrezagholi, F., additional, Shahidi, M., additional, Riccio, E., additional, Visciano, B., additional, Capuano, I., additional, Memoli, A., additional, Mozzillo, G., additional, Memoli, B., additional, and Pisani, A., additional

Published
2013
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26. Genetic diseases and molecular genetics

Author

Legendre, C., primary, Cohen, D., additional, Delmas, Y., additional, Feldkamp, T., additional, Fouque, D., additional, Furman, R., additional, Gaber, O., additional, Greenbaum, L., additional, Goodship, T., additional, Haller, H., additional, Herthelius, M., additional, Hourmant, M., additional, Licht, C., additional, Moulin, B., additional, Sheerin, N., additional, Trivelli, A., additional, Bedrosian, C. L., additional, Loirat, C., additional, Legendre, C., additional, Babu, S., additional, Jungraithmayr, T., additional, Lebranchu, Y., additional, Riedl, M., additional, Gaber, A. O., additional, Bedrosian, C., additional, Muus, P., additional, Douglas, K., additional, Remuzzi, G., additional, Kourouklaris, A., additional, Ioannou, K., additional, Athanasiou, I., additional, Demetriou, K., additional, Panagidou, A., additional, Zavros, M., additional, Rodriguez C, N. Y., additional, Blasco, M., additional, Arcal, C., additional, Quintana, L. F., additional, Rodriguez de Cordoba, S., additional, Campistol, J. M., additional, Bachmann, N., additional, Eisenberger, T., additional, Decker, C., additional, Bolz, H. J., additional, Bergmann, C., additional, Pesce, F., additional, Cox, S. N., additional, Serino, G., additional, De Palma, G., additional, Sallustio, F. P., additional, Schena, F., additional, Falchi, M., additional, Pieri, M., additional, Stefanou, C., additional, Zaravinos, A., additional, Erguler, K., additional, Lapathitis, G., additional, Dweep, H., additional, Sticht, C., additional, Anastasiadou, N., additional, Zouvani, I., additional, Voskarides, K., additional, Gretz, N., additional, Deltas, C. C., additional, Ruiz, A., additional, Bonny, O., additional, Sallustio, F., additional, Curci, C., additional, Cox, S., additional, Kemter, E., additional, Sklenak, S., additional, Aigner, B., additional, Wanke, R., additional, Kitzler, T. M., additional, Moskowitz, J. L., additional, Piret, S. E., additional, Lhotta, K., additional, Tashman, A., additional, Velez, E., additional, Thakker, R. V., additional, Kotanko, P., additional, Leierer, J., additional, Rudnicki, M., additional, Perco, P., additional, Koppelstaetter, C., additional, Mayer, G., additional, Sa, M. J. N., additional, Alves, S., additional, Storey, H., additional, Flinter, F., additional, Willems, P. J., additional, Carvalho, F., additional, Oliveira, J., additional, Arsali, M., additional, Papazachariou, L., additional, Demosthenous, P., additional, Lazarou, A., additional, Hadjigavriel, M., additional, Stavrou, C., additional, Yioukkas, L., additional, Deltas, C., additional, Pierides, A., additional, Kkolou, M., additional, Toka, H. R., additional, Dibartolo, S., additional, Lanske, B., additional, Brown, E. M., additional, Pollak, M. R., additional, Familiari, A., additional, Zavan, B., additional, Sanna Cherchi, S., additional, Fabris, A., additional, Cristofaro, R., additional, Gambaro, G., additional, D'Angelo, A., additional, Anglani, F., additional, Toka, H., additional, Mount, D., additional, Pollak, M., additional, Curhan, G., additional, Sengoge, G., additional, Bajari, T., additional, Kupczok, A., additional, von Haeseler, A., additional, Schuster, M., additional, Pfaller, W., additional, Jennings, P., additional, Weltermann, A., additional, Blake, S., additional, Sunder-Plassmann, G., additional, Kerti, A., additional, Csohany, R., additional, Wagner, L., additional, Javorszky, E., additional, Maka, E., additional, Tulassay, T., additional, Tory, K., additional, Kingswood, J., additional, Nikolskaya, N., additional, Mbundi, J., additional, Jozwiak, S., additional, Belousova, E., additional, Frost, M., additional, Kuperman, R., additional, Bebin, M., additional, Korf, B., additional, Flamini, R., additional, Kohrman, M., additional, Sparagana, S., additional, Wu, J., additional, Brechenmacher, T., additional, Stein, K., additional, Bissler, J., additional, Franz, D., additional, Zonnenberg, B., additional, Cheung, W., additional, Wang, J., additional, Lam, D., additional, Budde, K., additional, Ivanitskiy, L., additional, Sowershaewa, E., additional, Krasnova, T., additional, Samokhodskaya, L., additional, Safarikova, M., additional, Jana, R., additional, Jitka, S., additional, Obeidova, L., additional, Kohoutova, M., additional, Tesar, V., additional, Evrengul, H., additional, Ertan, P., additional, Serdaroglu, E., additional, Yuksel, S., additional, Mir, S., additional, Yang n Ergon, E., additional, Berdeli, A., additional, Zawada, A., additional, Rogacev, K., additional, Rotter, B., additional, Winter, P., additional, Fliser, D., additional, Heine, G., additional, Bataille, S., additional, Moal, V., additional, Berland, Y., additional, Daniel, L., additional, Rosado, C., additional, Bueno, E., additional, Fraile, P., additional, Lucas, C., additional, Garcoa-Cosmes, P., additional, Tabernero, J. M., additional, Gonzalez, R., additional, Garcia-Cosmes, P., additional, Silska-Dittmar, M., additional, Zaorska, K., additional, Malke, A., additional, Musielak, A., additional, Ostalska-Nowicka, D., additional, Zachwieja, J., additional, K d r, V., additional, Uz, E., additional, Yigit, A., additional, Altuntas, A., additional, Yigit, B., additional, Inal, S., additional, Sezer, M., additional, Yilmaz, R., additional, Visciano, B., additional, Porto, C., additional, Acampora, E., additional, Russo, R., additional, Riccio, E., additional, Capuano, I., additional, Parenti, G., additional, Pisani, A., additional, Feriozzi, S., additional, Perrin, A., additional, West, M., additional, Nicholls, K., additional, Torras, J., additional, Cybulla, M., additional, Conti, M., additional, Angioi, A., additional, Floris, M., additional, Melis, P., additional, Asunis, A. M., additional, Piras, D., additional, Pani, A., additional, Warnock, D., additional, Guasch, A., additional, Thomas, C., additional, Wanner, C., additional, Campbell, R., additional, Vujkovac, B., additional, Okur, I., additional, Biberoglu, G., additional, Ezgu, F., additional, Tumer, L., additional, Hasanoglu, A., additional, Bicik, Z., additional, Akin, Y., additional, Mumcuoglu, M., additional, Ecder, T., additional, Paliouras, C., additional, Mattas, G., additional, Papagiannis, N., additional, Ntetskas, G., additional, Lamprianou, F., additional, Karvouniaris, N., additional, and Alivanis, P., additional

Published
2013
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28. Clustered inactivating mutations and benign polymorphisms of the calcium receptor gene in familial benign hypocalciuric hypercalcemia suggest receptor functional domains.

Author

Heath, H, primary, Odelberg, S, additional, Jackson, C E, additional, Teh, B T, additional, Hayward, N, additional, Larsson, C, additional, Buist, N R, additional, Krapcho, K J, additional, Hung, B C, additional, Capuano, I V, additional, Garrett, J E, additional, and Leppert, M F, additional

Published
1996
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29. Molecular cloning and functional expression of human parathyroid calcium receptor cDNAs.

Author

Garrett, J E, Capuano, I V, Hammerland, L G, Hung, B C, Brown, E M, Hebert, S C, Nemeth, E F, and Fuller, F

Abstract

Parathyroid cells express a cell surface receptor, coupled to the mobilization of intracellular Ca2+, that is activated by increases in the concentration of extracellular Ca2+ and by a variety of other cations. This "Ca2+ receptor" (CaR) serves as the primary physiological regulator of parathyroid hormone secretion. Alterations in the CaR have been proposed to underlie the increases in Ca2+ set-point seen in primary hyperparathyroidism due to parathyroid adenoma. We have isolated human CaR cDNAs from an adenomatous parathyroid gland. The cloned receptor, expressed in Xenopus oocytes, responds to extracellular application of physiologically relevant concentrations of Ca2+ and other CaR agonists. The rank order of potency of CaR agonists displayed by the native receptor (Gd3+ > neomycin B > Ca2+ > Mg2+) is maintained by the expressed receptor. The nucleotide sequence of the human CaR cDNA predicts a protein of 1078 amino acids with high sequence similarity to a bovine CaR, and displays seven putative membrane-spanning regions common to G protein-coupled receptors. The deduced protein sequence shows potential sites for N-linked glycosylation and phosphorylation by protein kinase C and has a low level of sequence similarity to the metabotropic glutamate receptors. Comparison of the cDNA sequence to that of the normal human CaR gene showed no alteration in the coding region sequence of the CaR in this particular instance of parathyroid adenoma. Human cDNA clones with differing 5'-untranslated regions were isolated, suggesting alternative splicing of the parathyroid CaR mRNA. A rare variant cDNA clone representing a 10 amino acid insertion into the extracellular domain was also isolated. Northern blot analysis of normal and adenomatous parathyroid gland mRNA identified a predominant transcript of approximately 5.4 kilobases, and less abundant transcripts of approximately 10, 4.8 and 4.2 kilobases in RNA from the adenoma. While there is no evidence for alteration of the primary amino acid sequence of the CaR in this adenoma, modulation of CaR biosynthesis through alternative RNA processing may play a role in set-point alterations.

Published
1995

30. Anastomotic leakage following laparoscopic resection of low and mid rectal cancer

Author

Shalaby, M., Thabet, W., Rulli, F., Palmieri, F., Saraceno, F., Capuano, I., Buonomo, O., Giarratano, G., Petrella, G., Morshed, M., Farid, M., Pierpaolo Sileri, Shalaby, M, Thabet, W, Rulli, F, Palmieri, F, Saraceno, F, Capuano, I, Buonomo, O, Giarratano, G, Petrella, G, Morshed, M, Farid, M, and Sileri, P

Abstract

PURPOSE: Anastomotic leakage is considered the commonest major complication after surgery for rectal cancer. MATERIALS AND METHODS: Patients who underwent laparoscopic LAR or ULAR for rectal cancer were recruited. The primary outcome was the incidence of the AL during 30 days postoperative. RESULTS: Fifty-nine consecutive patients were included in the study. Fifty-three patients underwent LAR with stapled colorectal anastomoses, while the remaining 6 patients underwent ULAR with hand-sewn coloanal anastomoses. The median duration of operation was 195 minutes (range; 120-315). The defunctioning ileostomy was created in 24 (7%) patients. Overall, there was no recorded mortality. Only 10 (17%) patients developed complications. There were only 4 patients who developed AL. Three patients had a subclinical AL as they had defunctioning ileostomy at the time of the initial procedure, the diagnosis was made by CT with rectal contrast. They were treated conservatively with transanal anastomotic drainage under endoscopic guidance. One patient had a clinically significant AL, demonstrated as a peritonitis. This patient required reoperation during which pelvic abscess was drained, resection of the previous anastomosis, and hartmann's colostomy was performed. CONCLUSION: Standardization of a definition, as well as, criteria for the diagnosis of AL, will help in comparison of the results and the surgical techniques in order to optimize the required care offered to rectal cancer patients. On expert hands, it is feasible to perform a laparoscopic sphincter-saving total mesorectal excision, additionally, it provides the advantages of a clear view of the deep pelvis and facilitates a precise sharp dissection.

31. Therapeutic advances in ADPKD: the future awaits

Author

Pasquale Buonanno, Antonio Pisani, Maria Amicone, Eleonora Riccio, Ivana Capuano, Capuano, I., Buonanno, P., Riccio, E., Amicone, M., and Pisani, A.

Subjects
TRPP Cation Channels, Molecular pathway, medicine.medical_treatment, 030232 urology & nephrology, Autosomal dominant polycystic kidney disease, Apoptosis, 030204 cardiovascular system & hematology, Total kidney volume, urologic and male genital diseases, Bioinformatics, End stage renal disease, Targeted therapy, Cell therapy, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Glomerular filtration rate, education, education.field_of_study, PKD1, business.industry, Genetic disorder, Cell cycle, Polycystic Kidney, Autosomal Dominant, medicine.disease, Polycystin 2, Nephrology, Tolvaptan, Kidney Failure, Chronic, Calcium, business
Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is a heterogeneous genetic disorder included in ciliopathies, representing the fourth cause of end stage renal disease (ESRD), with an estimated prevalence between 1:1000 and 1:2500. It is mainly caused by mutations in the PKD1 and PKD2 genes encoding for polycystin 1 (PC1) and polycystin 2 (PC2), which regulate differentiation, proliferation, survival, apoptosis, and autophagy. The advances in the knowledge of multiple molecular pathways involved in the pathophysiology of ADPKD led to the development of several treatments which are currently under investigation. Recently, the widespread approval of tolvaptan and, in Italy, of long-acting release octreotide (octreotide-LAR), represents but the beginning of the new therapeutic management of ADPKD patients. Encouraging results are expected from ongoing randomized controlled trials (RCTs), which are investigating not only drugs acting on the calcium/cyclic adenosin monoposphate (cAMP) pathway, the most studied target so far, but also molecules targeting specific pathophysiological pathways (e.g. epidermal growth factor (EGF) receptor, AMP-activated protein kinase (AMPK) and KEAP1-Nrf2) and sphingolipids. Moreover, studies on animal models and cultured cells have also provided further promising therapeutic strategies based on the role of intracellular calcium, cell cycle regulation, MAPK pathway, epigenetic DNA, interstitial inflammation, and cell therapy. Thus, in a near future, tailored therapy could be the key to changing the natural history of ADPKD thanks to the vigorous efforts that are being made to implement clinical and preclinical studies in this field. Our review aimed to summarize the spectrum of drugs that are available in the clinical practice and the most promising molecules undergoing clinical, animal, and cultured cell studies. Graphical abstract: [Figure not available: see fulltext.]

Published
2021

32. Stepwise shortening of agalsidase beta infusion duration in Fabry disease: Clinical experience with infusion rate escalation protocol

Author

Maria Amicone, Pasquale Buonanno, Eleonora Riccio, Monica Franzese, Antonio Pisani, Ivana Capuano, Lucia Ferreri, Mario Zanfardino, Riccio, E., Zanfardino, M., Franzese, M., Capuano, I., Buonanno, P., Ferreri, L., Amicone, M., and Pisani, A.

Subjects
Adult, Male, 0301 basic medicine, infusion‐associated reactions, QH426-470, 030105 genetics & heredity, Drug Administration Schedule, 03 medical and health sciences, Quality of life, infusion-associated reaction, Genetics, Humans, Medicine, infusion-associated reactions, Infusions, Intravenous, Patient compliance, Molecular Biology, Genetics (clinical), Aged, Fabry disease, business.industry, Significant difference, Original Articles, Enzyme replacement therapy, Middle Aged, medicine.disease, AGALSIDASE BETA, Isoenzymes, 030104 developmental biology, Tolerability, infusion rate escalation protocol, alpha-Galactosidase, Anesthesia, Cohort, agalsidase beta, Original Article, Female, business, enzyme replacement therapy
Abstract

Background Although enzyme replacement therapy with agalsidase beta resulted in a variety of clinical benefits, life‐long biweekly intravenous infusion may impact on patients’ quality of life. Moreover, regular infusions are time‐consuming: although a stepwise shortening of infusion duration is allowed up to a minimum of 1.5 hr, in most centers it remains ≥3 hr, and no data exists about the safety and tolerability of agalsidase beta administration at maximum tolerated infusion rate. Methods In this study, we reported our experience with a stepwise infusion rate escalation protocol developed in our center in a cohort of 53 Fabry patients (both already receiving and treatment‐naΪve), and explored factors predictive for the infusion rate increase tolerability. Results Fifty‐two patients (98%) reduced infusion duration ≤3 hr; of these, 38 (72%) even reached a duration ≤2 hr. We found a significant difference between the mean duration reached by already treated and naΪve patients (p, Although enzyme replacement therapy with agalsidase beta resulted in a variety of clinical benefits, life‐long biweekly intravenous infusion may impact on patients’ quality of life because regular infusions are time‐consuming. In this study, we reported our experience with a stepwise infusion rate escalation protocol developed in our center in a cohort of 53 Fabry patients (both already receiving and treatment‐naΪve), and explored factors predictive for the infusion rate increase tolerability. We showed that our infusion rate escalation protocol is safe and could improve patient compliance, satisfaction and quality of life.

Published
2021

33. The effects of somatostatin analogues on liver volume and quality of life in polycystic liver disease: a meta-analysis of randomized controlled trials

Author

Carlo Garofalo, Ivana Capuano, Luigi Pennino, Ilaria De Gregorio, Eleonora Riccio, Michele Provenzano, Felice Crocetto, Pasquale Buonanno, Savio Domenico Pandolfo, Michele Andreucci, Antonio Pisani, Garofalo, Carlo, Capuano, Ivana, Pennino, Luigi, De Gregorio, Ilaria, Riccio, Eleonora, Provenzano, Michele, Crocetto, Felice, Buonanno, Pasquale, Pandolfo, Savio Domenico, Andreucci, Michele, Pisani, Antonio, Garofalo, C., Capuano, I., Pennino, L., De Gregorio, I., Riccio, E., Provenzano, M., Crocetto, F., Buonanno, P., Pandolfo, S. D., Andreucci, M., and Pisani, A.

Subjects
Multidisciplinary, Cysts, Liver Diseases, Science, Gastroenterology, Organ Size, Middle Aged, Polycystic Kidney, Autosomal Dominant, Article, Liver, Nephrology, Quality of Life, Humans, Medicine, Somatostatin, Randomized Controlled Trials as Topic
Abstract

A clear evidence on the benefits of somatostatin analogues (SA) on liver outcome in patients affected by polycystic liver disease is still lacking. We performed a meta-analysis of RCTs and a trial sequential analysis (TSA) evaluating the effects of SA in adult patients with polycystic liver disease on change in liver volume. As secondary outcome, we evaluated the effects on quality of life as measured by SF36-questionnaire. Six RCTs were selected with an overall sample size of 332 adult patients with polycystic liver disease (mean age: 46 years). Mean liver volume at baseline was 3289 ml in SA group and 3089 ml in placebo group. Overall, unstandardized mean difference in liver volume was − 176 ml (95%CI, − 406, 54; p 2:0%, p p = 0.036). Cumulative Z-curve in TSA did not reach either significance and futility boundaries or required information size. Three RCTs have evaluated Quality of life parameters measured by SF36-QOL questionnaire for a total of 124 patients; no significant difference was found on the effect of SA on QOL parameters when compared with placebo. The present meta-analysis revealed a potential effect of SA on reduction of liver volume and quality of life parameters, but results did not reach a statistical significance. These data could be explained by the need of further studies, as demonstrated through TSA, to reach an adequate sample size to confirm the beneficial outcomes of SAs treatment.

Published
2021

34. Early Biomarkers of Fabry Nephropathy: A Review of the Literature

Author

Eleonora Riccio, Massimo Sabbatini, Antonio Pisani, Ivana Capuano, Riccio, E, Sabbatini, M, Capuano, I, and Pisani, A

Subjects
Male, Proteomics, medicine.medical_specialty, 030232 urology & nephrology, Renal function, Disease, 030204 cardiovascular system & hematology, Urine, Nephropathy, Fabry nephropathy, 03 medical and health sciences, 0302 clinical medicine, Alpha-Globulins, medicine, Humans, Enzyme Replacement Therapy, Cystatin C, Intensive care medicine, Kidney, Proteinuria, business.industry, Cysts, Trihexosylceramides, Enzyme replacement therapy, medicine.disease, Fabry disease, Early marker, medicine.anatomical_structure, Early Diagnosis, Albuminuria, Fabry Disease, Female, medicine.symptom, business, Biomarkers, Glomerular Filtration Rate
Abstract

Progressive nephropathy is one of the main features of Fabry disease. Although some clinical signs of Fabry nephropathy are already present in childhood, patients are often diagnosed relatively late in the course of the disease due to the absence of specific clinical markers, while a timely diagnosis and the prompt start of enzyme replacement therapy may be beneficial in stabilizing renal function or slowing its decline. Proteinuria/albuminuria has been accepted as the most important marker for Fabry nephropathy; however, a large proportion of renal impairment occurs in nonalbuminuric state. Therefore, early biomarkers may be useful for early identification of kidney involvement. The aim of this article is to review the current available literature on all biomarkers of Fabry nephropathy, with a comprehensive and critical description of their utilization in early recognition of renal damage.

Published
2019

35. Additional Nodal Disease Prediction in Breast Cancer with Sentinel Lymph Node Metastasis Based on Clinicopathological Features

Author

Alessandra Vittoria Granai, Ilaria Capuano, Ilaria Portarena, Adriano De Majo, Emanuele Caredda, Oreste Claudio Buonomo, Marco Materazzo, Paolo Orsaria, Gianluca Vanni, Giuseppe Petrella, Federica Genova, Pierpaolo Sileri, Leonardo Palombi, Orsaria, P, Caredda, E, Genova, F, Materazzo, M, Capuano, I, Vanni, G, Granai, Av, De Majo, A, Portarena, I, Sileri, P, Petrella, G, Palombi, L, and Buonomo, Oc

Subjects
Oncology, Cancer Research, Lymphovascular invasion, Receptor, ErbB-2, Metastasis, ErbB-2, 0302 clinical medicine, Risk Factors, Ductal, 80 and over, Breast, Prospective cohort study, Aged, 80 and over, medicine.diagnostic_test, Carcinoma, Ductal, Breast, General Medicine, Middle Aged, Prognosis, medicine.anatomical_structure, nodal metastasis, 030220 oncology & carcinogenesis, Lymphatic Metastasis, Breast neoplasms, sentinel lymph node, Adult, Aged, Axilla, Breast Neoplasms, Female, Humans, Lymph Node Excision, Retrospective Studies, Sentinel Lymph Node, Sentinel Lymph Node Biopsy, 030211 gastroenterology & hepatology, Receptor, medicine.medical_specialty, Sentinel lymph node, 03 medical and health sciences, Breast cancer, Internal medicine, Biopsy, medicine, business.industry, Carcinoma, Axillary Lymph Node Dissection, medicine.disease, Settore MED/18 - Chirurgia Generale, business
Abstract

Aim: The standard-of-care in breast cancer (BC) with positive sentinel lymph node (SLN) metastasis includes complete axillary lymph node dissection (ALND); however, almost half of such cases have no further tumor burden. This study aimed to assess the clinicopathological factors that predict non-SLN metastasis to define subgroups of SLN-positive patients in whom the axilla may be staged by SLN biopsy alone, while avoiding unnecessary overtreatment. Patients and Methods: The records of 191 patients with histologically-proven primary BC who underwent a positive (SLN) biopsy between 2005 and 2017 were reviewed. Patients with at least one tumor-involved SLN who underwent completion ALND were enrolled. Demographic and clinicopathological characteristics, including age, primary tumor size and histological grade, lymphovascular invasion, ratio of positive SLNs to the harvested SLNs, SLN metastasis size, and molecular subtype classification according to immunohistochemical biomarker status [estrogen receptor (ER), progesterone receptor (PR), and human epidermal growth factor receptor 2 (HER2)], were evaluated. Data were collected retrospectively and analyzed using the Mann-Whitney and Chi-square tests (statistical significance: p0.67 [odds ratio (OR)=2.55, p=0.032], luminal BC subtype (OR=2.67, p=0.06), HER2 overexpression (OR=0.4, p=0.016), and ER(+)PR(-)HER2(-) profile (OR=2.95, p=0.027). There was a tendency (statistically insignificant; p>0.05) toward higher incidence of non SLN metastasis with increasing age and histological grade, which could be attributed to the small sample size. Conclusion: According to this study, sentinel nodal ratio and BC subtypes as per ER, PR, and HER2 status significantly predicted the likelihood of additional lymphatic involvement. Validation of these parameters in prospective studies is indicated, and may help individualize treatment modalities.

Published
2018

36. Laparoscopic ventral rectopexy using biologic mesh for the treatment of obstructed defaecation syndrome and/or faecal incontinence in patients with internal rectal prolapse: a critical appraisal of the first 100 cases

Author

Federica Giorgi, Luana Franceschilli, C Ciangola, Ilaria Capuano, Pierpaolo Sileri, D. Varvaras, G. Boehm, A.L. Gaspari, Franceschilli, L, Varvaras, D, Capuano, I, Ciangola, Ci, Giorgi, F, Boehm, G, Gaspari, Al, and Sileri, P

Subjects
Adult, medicine.medical_specialty, Operative Time, Anal Canal, Biocompatible Materials, Postoperative Complications, Recurrence, medicine, Humans, Prospective Studies, Defecation, Laparoscopy, Prospective cohort study, Digestive System Surgical Procedures, Aged, Aged, 80 and over, medicine.diagnostic_test, business.industry, Rectocele, Rectum, Gastroenterology, Rectal Prolapse, Length of Stay, Middle Aged, Surgical Mesh, medicine.disease, Colorectal surgery, Surgery, Rectal prolapse, Critical appraisal, Treatment Outcome, Female, Complication, business, Constipation, Fecal Incontinence, Intestinal Obstruction, Follow-Up Studies, Abdominal surgery
Abstract

Laparoscopic ventral mesh rectopexy (LVR) is gaining wider acceptance as the preferred procedure to correct internal as well as external rectal prolapse associated with obstructed defaecation syndrome and/or faecal incontinence. Very few reports exist on the use of biologic mesh for LVR. The aim of our study was to report the complication and recurrence rate of our first 100 cases of LVR for symptomatic internal rectal prolapse and/or rectocele using a porcine dermal collagen mesh. Prospectively collected data on LVR for internal rectal prolapse were analysed. Surgical complications and functional results in terms of faecal incontinence (measured with the Faecal Incontinence Severity Index = FISI) and constipation (measured with the Wexner Constipation Score = WCS) at 3, 6 and 12 months were analysed. It was considered an improvement if FISI or WCS scores were reduced by at least 25 % and a cure if the FISI score decreased to < 10 and the WCS decreased to < 5. Between April 2009 and April 2013, 100 consecutive female patients (mean age 63 years, range 24-88 years) underwent LVR. All patients had internal rectal prolapse (grade III [n = 25] and grade IV [n = 75] according to the Oxford classification) and rectocele. Mean operative time was 85 +/- A 40 min. Conversion rate to open technique was 1 %. There was no post-operative mortality. Overall 16 patients (16 %) experienced 18 complications, including rectal perforation (n = 1), small bowel obstruction (n = 2), urinary tract infection (n = 8), subcutaneous emphysema (n = 3), wound haematoma (n = 2), long lasting sacral pain (n = 1) and incisional hernia (1). Median post-operative length of stay was 2 days. Ninety-eight out of 100 patients completed follow-up. At the end of follow-up, the mean FISI score improved from 8.4 (+/- 4.0 standard deviation (SD) p = 0.003) to 3.3 +/- 2.3 SD (p = 0.04). Incontinence improved in 37 out of 43 patients (86 %), and 31 patients (72 %) were cured. Similarly, the mean WCS score improved from 18.4 +/- 11.6 SD to 5.4 +/- 4.1 SD (p = 0.04). Constipation improved in 82 out of 89 patients (92 %), and 70 patients (79 %) were cured. No worsening of continence status, constipation or sexual function was observed. Fourteen patients (14 %) experienced persistence or recurrence of prolapse. LVR using biologic mesh is a safe and effective procedure for improving symptoms of obstructed defaecation and faecal incontinence in patients with internal rectal prolapse associated with rectocele.

Published
2015

37. Erosion after laparoscopic ventral mesh rectopexy with a biological mesh

Author

Mostafa Shalaby, A. Matarangolo, Giuseppe Petrella, Pierpaolo Sileri, Ilaria Capuano, Shalaby, M, Matarangolo, A, Capuano, I, Petrella, G, and Sileri, P

Subjects
medicine.medical_specialty, Mesh rectopexy, business.industry, Gastroenterology, Colorectal surgery, Surgery, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Medicine, 030211 gastroenterology & hepatology, business, Abdominal surgery
Published
2017

38. Modified laparoscopic ventral mesh rectopexy

Author

Pierpaolo Sileri, Federica Giorgi, A.L. Gaspari, Luana Franceschilli, Ilaria Capuano, Sileri, P, Capuano, I, Franceschilli, L, Giorgi, F, and Gaspari, Al

Subjects
Adult, medicine.medical_specialty, Mesh rectopexy, Operative Time, Mesh fixation, Humans, Medicine, Aged, Mesorectal, business.industry, Gastroenterology, Rectal Prolapse, Anatomy, Length of Stay, Middle Aged, Surgical Mesh, Colorectal surgery, Surgical mesh, Operative time, Female, Laparoscopy, Surgery, Sacral promontory, business, Constipation, Fecal Incontinence
Abstract

We present a modified laparoscopic ventral mesh rectopexy procedure using biological mesh and bilateral anterior mesh fixation. The rectopexy is anterior with a minimal posterior mobilization. The rectum is symmetrically suspended to the sacral promontory through a mesorectal window.

Published
2014

39. Small-Bowel Obstruction Secondary to Adhesions After Open or Laparoscopic Colorectal Surgery

Author

Paolo Angelucci G, Luana Franceschilli, Di Lorenzo N, Ilaria Capuano, Silvia Quaresima, Sebastian Smolarek, Pierpaolo Sileri, Mostafa Shalaby, Giulia Missori, Smolarek, S, Shalaby, M, Angelucci, Gp, Missori, G, Capuano, I, Franceschilli, L, Quaresima, S, Di Lorenzo, N, and Sileri, P

Subjects
Adult, Male, Reoperation, medicine.medical_specialty, Time Factors, Adolescent, Incisional hernia, 030230 surgery, Scientific Paper, Young Adult, 03 medical and health sciences, Postoperative Complications, 0302 clinical medicine, adult, aged, aged, 80 and over, colorectal surgery, female, humans, intestinal obstruction, laparoscopy, male, middle aged, postoperative complications, reoperation, retrospective studies, risk factors, time factors, young adult, intestine small, Risk Factors, Intestine, Small, 80 and over, medicine, Humans, Surgical emergency, Risk factor, Laparoscopy, Aged, Retrospective Studies, Aged, 80 and over, medicine.diagnostic_test, business.industry, Middle Aged, medicine.disease, Colorectal surgery, Settore MED/18, Surgery, Bowel obstruction, 030220 oncology & carcinogenesis, Female, business, Colorectal Surgery, Intestinal Obstruction, Cohort study, Abdominal surgery
Abstract

Background and Objectives: Small-bowel obstruction (SBO) is a common surgical emergency that occurs in 9% of patients after abdominal surgery. Up to 73% are caused by peritoneal adhesions. The primary purpose of this study was to compare the rate of SBOs between patients who underwent laparoscopic (LPS) and those who had open (OPS) colorectal surgery. The secondary reasons were to evaluate the rate of adhesive SBO in a cohort of patients who underwent a range of colorectal resections and to assess risk factors for the development of SBO. Method: This was a retrospective observational cohort study. Data were analyzed from a prospectively collected database and cross checked with operating theater records and hospital patient management systems. Results: During the study period, 707 patients underwent colorectal resection, 350 of whom (49.5%) were male. Median follow-up was 48.3 months. Of the patients included, 178 (25.2%) underwent LPS, whereas 529 (74.8%) had OPS. SBO occurred in 72 patients (10.2%): 20 (11.2%) in the LPS group and 52 (9.8%) in the OPS group [P = .16; hazards ratio (HR) 1.4 95% CI 0.82-2.48] within the study period. Conversion to an open procedure was associated with increased risk of SBO (P = .039; HR 2.82; 95% CI 0.78-8.51). Stoma formation was an independent risk factor for development of SBO (P = .049; HR, 0.63; 95% CI 0.39 -1.03). The presence of an incisional hernia in the OPS group was associated with SBO (P = .0003; HR, 2.85; 95% CI 1.44 -5.283). There was no difference in SBO between different types of procedures: right colon, left colon, and rectal surgery. Patients who developed early small-bowel obstruction (ESBO) were more often treated surgically compared to late SBO (P= .0001). Conclusion: The use of laparoscopy does not influence the rate of SBO, but conversion from laparoscopic to open surgery is associated with an increased risk of SBO. Stoma formation is associated with a 2-fold increase in SBO. Development of ESBO is highly associated with a need for further surgical intervention.

Published
2016

40. Comment on 'Cancer genetic counselling' by P. Mandich et al. (Ann Oncol 2005; 16: 171)

Author

A. Contegiacomo, Viola Barbieri, Matilde Pensabene, Massimo Federico, Laura Cortesi, Enrico Ricevuto, Libuse Tauchmanovà, Daniela Turchetti, Paolo Marchetti, Vittorio Silingardi, I. Capuano, G. Cianci, Salvatore Venuta, Contegiacomo A., Pensabene M., Capuano I., Tauchmanova L., Federico M., Turchetti D., Cortesi L., Marchetti P., Ricevuto E., Cianci G., Barbieri V., Venuta S., and Silingardi V.

Subjects
Genetics, Oncology, medicine.medical_specialty, business.industry, Internal medicine, Genetic counseling, medicine, Cancer, Hematology, medicine.disease, business
Published
2005

41. Pain-free today, weak tomorrow: a case of electrolyte disorder due to diclofenac misuse.

Author

De Marco O, Buonanno P, Riccio E, Pisani A, and Capuano I

Subjects
Humans, Male, Middle Aged, Back Pain drug therapy, Diclofenac adverse effects, Anti-Inflammatory Agents, Non-Steroidal adverse effects, Water-Electrolyte Imbalance chemically induced
Abstract

Background: The nephrotoxic effects of non-steroidal anti-inflammatory drugs (NSAIDs) are widely acknowledged. In particular, diclofenac is the most commonly prescribed NSAIDs, but no previous findings of electrolyte disturbances were reported following its administration., Case Report: We presented the case of a man who experienced significant weakness associated with severe deficiencies in potassium, calcium, and magnesium after misusing diclofenac because of severe back pain., Conclusions: This case emphasizes the need of awareness about the electrolyte imbalances and electrolyte disturbances associated with the misuse of diclofenac, which is a widely available drug. This is a case report which does not need a Clinical Trial Number., (© 2024. The Author(s).)

Published
2024
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42. Increased Expression of Orexin-A in Patients Affected by Polycystic Kidney Disease.

Author

Nigro E, D'Arco D, Moscatelli F, Pisani A, Amicone M, Riccio E, Capuano I, Argentino F, Monda M, Messina G, Daniele A, and Polito R

Subjects
Humans, Male, Female, Middle Aged, Adult, TRPP Cation Channels genetics, TRPP Cation Channels metabolism, Polycystic Kidney, Autosomal Dominant metabolism, Polycystic Kidney, Autosomal Dominant genetics, Polycystic Kidney, Autosomal Dominant blood, Case-Control Studies, Aged, Blood Pressure, Polycystic Kidney Diseases genetics, Polycystic Kidney Diseases metabolism, Polycystic Kidney Diseases blood, Orexins metabolism, Orexins genetics, Polymorphism, Single Nucleotide, Orexin Receptors metabolism, Orexin Receptors genetics
Abstract

Orexin-A is a neuropeptide product of the lateral hypothalamus that acts on two receptors, OX1R and OX2R. The orexinergic system is involved in feeding, sleep, and pressure regulation. Recently, orexin-A levels have been found to be negatively correlated with renal function. Here, we analyzed orexin-A levels as well as the incidence of SNPs in the hypocretin neuropeptide precursor (HCRT) and its receptors, HCRTR1 and HCRTR2, in 64 patients affected by autosomal dominant polycystic kidney disease (ADPKD) bearing truncating mutations in the PKD1 or PKD2 genes. Twenty-four healthy volunteers constituted the control group. Serum orexin-A was assessed by ELISA, while the SNPs were investigated through Sanger sequencing. Correlations with the main clinical features of PKD patients were assessed. PKD patients showed impaired renal function (mean eGFR 67.8 ± 34.53) and a statistically higher systolic blood pressure compared with the control group ( p < 0.001). Additionally, orexin-A levels in PKD patients were statistically higher than those in healthy controls (477.07 ± 69.42 pg/mL vs. 321.49 ± 78.01 pg/mL; p < 0.001). Furthermore, orexin-A inversely correlated with blood pressure ( p = 0.0085), while a direct correlation with eGFR in PKD patients was found. None of the analyzed SNPs showed any association with orexin-A levels in PKD. In conclusion, our data highlights the emerging role of orexin-A in renal physiology and its potential relevance to PKD. Further research is essential to elucidate the intricate mechanisms underlying orexin-A signaling in renal function and its therapeutic implications for PKD and associated cardiovascular complications.

Published
2024
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43. Cardiopulmonary determinants of reduced exercise tolerance in Fabry disease.

Author

De Marco O, Gambardella J, Bianco A, Fiordelisi A, Cerasuolo FA, Buonaiuto A, Avvisato R, Capuano I, Amicone M, Di Risi T, Riccio E, Spinelli L, Pisani A, Iaccarino G, and Sorriento D

Abstract

Fabry disease (FD), also known as Anderson-Fabry disease, is a hereditary disorder of glycosphingolipid metabolism, caused by a deficiency of the lysosomal alpha-galactosidase A enzyme. This causes a progressive accumulation of glycosphingolipids in tissues and organs which represents the main pathogenetic mechanism of FD. The disease is progressive and multisystemic and is characterized by early symptoms and late complications (renal, cardiac and neurological dysfunction). Fatigue and exercise intolerance are early common symptoms in FD patients but the specific causes are still to be defined. In this narrative review, we deal with the contribution of cardiac and pulmonary dysfunctions in determining fatigue and exercise intolerance in FD patients., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest. The author(s) declared that they were an editorial board member of Frontiers, at the time of submission. This had no impact on the peer review process and the final decision., (© 2024 De Marco, Gambardella, Bianco, Fiordelisi, Cerasuolo, Buonaiuto, Avvisato, Capuano, Amicone, Di Risi, Riccio, Spinelli, Pisani, Iaccarino and Sorriento.)

Published
2024
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44. Diet and Physical Activity in Fabry Disease: A Narrative Review.

Author

Muscogiuri G, De Marco O, Di Lorenzo T, Amicone M, Capuano I, Riccio E, Iaccarino G, Bianco A, Di Risi T, and Pisani A

Subjects
Humans, Quality of Life, Diet, Exercise, Nutritional Status, Fabry Disease therapy
Abstract

Fabry disease (FD) is caused by mutations in the galactosidase alpha (GLA) gene which lead to the accumulation of globotriaosylceramide (Gb-3). Enzyme replacement therapy (ERT) and oral chaperone therapy are the current pharmacological treatments for this condition. However, in the literature, there is a growing emphasis on exploring non-pharmacological therapeutic strategies to improve the quality of life of patients with FD. In particular, the nutritional approach to FD has been marginally addressed in the scientific literature, although specific dietary interventions may be useful for the management of nephropathy and gastrointestinal complications, which are often present in patients with FD. Especially in cases of confirmed diagnosis of irritable bowel syndrome (IBS), a low-FODMAP diet can represent an effective approach to improving intestinal manifestations. Furthermore, it is known that some food components, such as polyphenols, may be able to modulate some pathogenetic mechanisms underlying the disease, such as inflammation and oxidative stress. Therefore, the use of healthy dietary patterns should be encouraged in this patient group. Sports practice can be useful for patients with multi-organ involvement, particularly in cardiovascular, renal, and neurological aspects. Therefore, the aim of this review is to summarize current knowledge on the role of nutrition and physical activity in FD patients.

Published
2024
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45. Does Physical Exercise Ameliorate Chronic Kidney Disease-Related Complications? The Case of Anaemia and Chronic Kidney Disease-Mineral Bone Disorder.

Author

Aucella F, Amicone M, Perez Ys ADM, Aucella F, Gatta G, Prencipe MA, Riccio E, Capuano I, Pisani A, and Battaglia Y

Subjects
Humans, Chronic Kidney Disease-Mineral and Bone Disorder therapy, Renal Insufficiency, Chronic therapy, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic metabolism, Exercise, Anemia therapy, Anemia etiology
Abstract

Background: Physical exercise (PE) can regulate inflammation, cardiovascular health, sarcopenia, anaemia, and bone health in the chronic kidney disease (CKD) population. Experimental and clinical studies both help us better understand the mechanisms that underlie the beneficial effects of the exercise, especially in renal anaemia and CKD-mineral bone disorders (CKD-MBDs). Here, we summarize this evidence, exploring the biological pathways involved, locally released substances, and crosstalk between tissues, but also the shortcomings of current knowledge., Summary: Anaemia: Both in healthy and CKD subjects, PE may mimic hypoxia, inhibiting PHDs; so hydroxylate HIF-α subunits may be translocated into the nucleus, resulting in dimerization of HIF-1α and HIF-1β, recruitment of p300 and CBP, and ultimately, binding to HREs at target genes to cause activation. However, in CKD subjects acute PE causes higher levels of lactate, leading to iron restriction by upregulating hepatic hepcidin expression, while chronic PE allows an increased lactate clearance and HIF-α and VEGFα levels, stimulating both erythropoiesis and angiogenesis., Ckd-Mbd: PE may improve bone health decreasing bone resorption and increasing bone formation throughout at least three main pathways: (a) increasing osteoprotegerin and decreasing RANKL system; (b) decreasing cytokine levels; and (c) stimulating production of myokines and adipokines., Key Messages: Future research needs to be defined to develop evidence-based exercise guidance to provide optimal benefit for CKD using exercise interventions as adjuvant therapy for CKD-related complications such as anaemia and CKD-MBD., (© 2024 The Author(s). Published by S. Karger AG, Basel.)

Published
2024
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47. Inhaled Bacteriophage Therapy for Multi-Drug Resistant Achromobacter .

Author

Winzig F, Gandhi S, Lee A, Würstle S, Stanley GL, Capuano I, Neuringer I, Koff JL, Turner PE, and Chan BK

Subjects
Humans, Anti-Bacterial Agents pharmacology, Bacteriophages, Phage Therapy, Achromobacter, Cystic Fibrosis therapy, Cystic Fibrosis complications
Abstract

The rise of antimicrobial resistant (AMR) bacteria is a global public health threat. AMR Achromobacter bacteria pose a challenging clinical problem, particularly for those with cystic fibrosis (CF) who are predisposed to chronic bacterial lung infections. Lytic bacteriophages (phages) offer a potential alternative to treat AMR infections, with the possible benefit that phage selection for resistance in target bacteria might coincide with reduced pathogenicity. The result is a genetic "trade-off," such as increased sensitivity to chemical antibiotics, and/or decreased virulence of surviving bacteria that are phage resistant. Here, we show that two newly discovered lytic phages against Achromobacter were associated with stabilization of respiratory status when deployed to treat a chronic pulmonary infection in a CF patient using inhaled (nebulized) phage therapy. The two phages demonstrate traits that could be generally useful in their development as therapeutics, especially the possibility that the phages can select for clinically useful trade-offs if bacteria evolve phage resistance following therapy. We discuss the limitations of the current study and suggest further work that should explore whether the phages could be generally useful in targeting pulmonary or other Achromobacter infections in CF patients., (Copyright ©2022, Yale Journal of Biology and Medicine.)

Published
2022

48. Randomized Controlled Trials on Renin Angiotensin Aldosterone System Inhibitors in Chronic Kidney Disease Stages 3-5: Are They Robust? A Fragility Index Analysis.

Author

Capuano I, Buonanno P, Riccio E, Bianco A, and Pisani A

Abstract

Inhibition of the renin-angiotensin-aldosterone system (RAAS) is broadly recommended in many nephrological guidelines to prevent chronic kidney disease (CKD) progression. This work aimed to analyze the robustness of randomized controlled trials (RCTs) investigating the renal and cardiovascular outcomes in CKD stages 3-5 patients treated with RAAS inhibitors (RAASi). We searched for RCTs in MEDLINE (PubMed), EMBASE databases, and the Cochrane register. Fragility indexes (FIs) for every primary and secondary outcome were calculated according to Walsh et al., who first described this novel metric, suggesting 8 as the cut-off to consider a study robust. Spearman coefficient was calculated to correlate FI to p value and sample size of statistically significant primary and secondary outcomes. Twenty-two studies met the inclusion criteria, including 80,455 patients. Sample size considerably varied among the studies (median: 1693.5, range: 73-17,276). The median follow-up was 38 months (range 24-58). The overall median of both primary and secondary outcomes was 0 (range 0-117 and range 0-55, respectively). The median of FI for primary and secondary outcomes with a p value lower than 0.05 was 6 (range: 1-117) and 7.5 (range: 1-55), respectively. The medians of the FI for primary outcomes with a p value lower than 0.05 in CKD and no CKD patients were 5.5 (range 1-117) and 22 (range 1-80), respectively. Only a few RCTs have been shown to be robust. Our analysis underlined the need for further research with appropriate sample sizes and study design to explore the real potentialities of RAASi in the progression of CKD.

Published
2022
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49. RAAS Inhibitor Prescription and Hyperkalemia Event in Patients With Chronic Kidney Disease: A Single-Center Retrospective Study.

Author

Riccio E, Capuano I, Buonanno P, Andreucci M, Provenzano M, Amicone M, Rizzo M, and Pisani A

Abstract

Hyperkalemia is common in patients treated with renin-angiotensin-aldosterone system inhibitors (RAASis), and it represents the main cause of the large gap reported between guideline recommendations and real-world practice in chronic kidney disease (CKD). We conducted a CKD-population-based restrospective study to determine the prevalence of patients with CKD treated with RAASis, incidence of hyperkalemia in patients with CKD treated with RAASis, and proportion of patients with RAASi medication change after experiencing incident hyperkalemia. Among 809 patients with CKD analyzed, 556 (68.7%) were treated with RAASis, and RAASi prescription was greater in stages 2-4 of CKD. Hyperkalemia occurred in 9.2% of RAASi-treated patients, and the adjusted rate of hyperkalemia among patients with stage 4-5 CKD was 3-fold higher compared with patients with eGFR > 60 ml/min/1.73 m 2 . RAASi treatment was discontinued in 55.3% of the patients after hyperkalemia event (74.2% discontinued therapy, 3.2% received a reduced dose, and 22.6% reduced the number of RAASi drugs). This study shows that the incidence of hyperkalemia is frequently observed in patients with CKD patients with RAASis, and that rates increase with deteriorating levels of kidney function from stages 1 to 3. RAASi medication change following an episode of hyperkalemia occurred in almost half of the patients after experiencing hyperkalemia., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Riccio, Capuano, Buonanno, Andreucci, Provenzano, Amicone, Rizzo and Pisani.)

Published
2022
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50. The effects of somatostatin analogues on liver volume and quality of life in polycystic liver disease: a meta-analysis of randomized controlled trials.

Author

Garofalo C, Capuano I, Pennino L, De Gregorio I, Riccio E, Provenzano M, Crocetto F, Buonanno P, Pandolfo SD, Andreucci M, and Pisani A

Subjects
Humans, Middle Aged, Polycystic Kidney, Autosomal Dominant drug therapy, Quality of Life, Randomized Controlled Trials as Topic, Cysts drug therapy, Liver drug effects, Liver Diseases drug therapy, Organ Size drug effects, Somatostatin analogs & derivatives, Somatostatin therapeutic use
Abstract

A clear evidence on the benefits of somatostatin analogues (SA) on liver outcome in patients affected by polycystic liver disease is still lacking. We performed a meta-analysis of RCTs and a trial sequential analysis (TSA) evaluating the effects of SA in adult patients with polycystic liver disease on change in liver volume. As secondary outcome, we evaluated the effects on quality of life as measured by SF36-questionnaire. Six RCTs were selected with an overall sample size of 332 adult patients with polycystic liver disease (mean age: 46 years). Mean liver volume at baseline was 3289 ml in SA group and 3089 ml in placebo group. Overall, unstandardized mean difference in liver volume was - 176 ml (95%CI, - 406, 54; p < 0.133). Heterogeneity was low (I 2 :0%, p < 0.992). However, we performed a moderator analysis and we found that a higher eGFR significantly correlates to a more pronounced effect of SA on liver volume reduction (p = 0.036). Cumulative Z-curve in TSA did not reach either significance and futility boundaries or required information size. Three RCTs have evaluated Quality of life parameters measured by SF36-QOL questionnaire for a total of 124 patients; no significant difference was found on the effect of SA on QOL parameters when compared with placebo. The present meta-analysis revealed a potential effect of SA on reduction of liver volume and quality of life parameters, but results did not reach a statistical significance. These data could be explained by the need of further studies, as demonstrated through TSA, to reach an adequate sample size to confirm the beneficial outcomes of SAs treatment., (© 2021. The Author(s).)

Published
2021
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