Your search keyword '"Garro R"' showing total 63 results

1. Predictive and prognostic role of immunohistochemical analyses of CD44, PDL1 and ATG7 in 40 squamous cell carcinomas

Author

Tinnirello, G., Salvatorelli, L., Mazzucchelli, M., Puzzo, L., and Garro, R.

Published

2022

2. Rare soft tissue tumors of the oral cavity

Author

Lin, 2. C. C., Salvatorelli, L., Puzzo, L., Broggi, G., Vecchio, G. M., Garro, R., and Magro, G.

Published

2022

3. Signalling in Viroid Pathogenesis

Author

Conejero, V., Bellés, J. M., García-Breijo, F., Garro, R., Hernández-Yago, J., Rodrigo, I., Vera, P., and Fraser, Ron S. S., editor

Published

1990

4. #77: Impact of Targeted Tacrolimus Levels on BK Polyomavirus DNAemia Among Pediatric Kidney Transplant Recipients

Author

Yildirim, I, primary, Liverman, R, additional, Serluco, S, additional, George, R, additional, Garro, R, additional, and Winterberg, P, additional

Published

2021

5. Abstracts of presentations on plant protection issues at the fifth international Mango Symposium Abstracts of presentations on plant protection issues at the Xth international congress of Virology: September 1–6, 1996 Dan Panorama Hotel, Tel Aviv, Israel August 11-16, 1996 Binyanei haoma, Jerusalem, Israel

Author

Peña, J. E., Wysoki, M., Singh, Gajendra, Boscán de M., Nancy, Godoy, Freddy J., Obligado, A., Rossetto, C. J., Ribeiro, I. J. A., Gallo, P. B., Soares, N. B., Sabino, J. C., Martins, A. L. M., Bortoletto, N., Ploetz, R. C., Benscher, D., Vázquez, Aimé, Colls, A., Nagel, Julianne, Schaffer, B., Pinkas, Y., Maymon, M., Freeman, S., Bostros Bastawros, Mikhail, Gosbee, M. J., Johnson, G. I., Joyce, D. C., Irwin, J. A. G., Saaiman, W. C., Prusky, D., Falik, E., Kobiler, I., Fuchs, Y., Zauberman, G., Pesis, E., Ackerman, M., Roth, I., Weksler, A., Yekutiely, O., Waisblum, A., Keinan, A., Ofek, G., Reved, R., Barak, R., Bel, P., Artes, L., Visarathanonth, N., Xu, Z., Ponce de León, L., Muñoz, C., Pérez, L., Diaz de León, F., Kerbel, C., Esparza, S., Bósquez, E., Trinidad, M., Coates, L. M., Cooke, A. W., Dean, J. R., Lucia Duarte, Ana, Alberto Otto, Paulo, Malavasi, Aldo, Lizado, M. C. C., Bautista, M. L., Artes, L. A., Bacalangco, N. S., Farungsang, U., Farungsang, N., Waskar, D. P., Masalkar, S. D., Gaikwad, R. S., Damame, S. V., Bally, Ian S. E., O’Hare, Tim J., Holmes, Rowland J., Atabekov, J. G., Fauquet, Claude M., Tomori, O., Nuss, D. L., Ahlquist, P., Díez, J., Ishikawa, M., Janda, M., Price, B. D., Restrepo-Hartwig, M., Bol, J. F., van Rossum, C. M. A., Garcia, M. L., van der Vossen, E. A. G., Reusken, Chantal B. E. M., Canto, T. R., Gal-On, A., Palukaitis, P., Roossinck, M. J., Flasinski, S., Restrepo-Hartwig, Maria A., Ahlquist, Paul, Smirnyagina, Ekaterina, Lin, Na-Sheng, Nagy, Peter D., Figlerowicz, Marek, Bujarski, Jozef J., Proll, D. F., Guyatt, K. J., Davidson, A. D., Kim, Kook-Hyung, Miller, Eric, Hemenway, Cynthia, Havelda, Z., Dalmay, T., Burgyán, J., Kearney, C. M., Thomson, M., Roland, K. E., Dawson, W. O., Bao, Y., Carter, S. A., Nelson, R. S., Derrick, P. M., Shun Ding, Xin, Eskarous, J. K., Sarkar, S., El-Shamy, M., Chen, J., Sako, N., Yuichiro, W., Ohshima, K., Okada, Y., Felden, Brice, Kuznetsov, Yuri G., Malkin, Alexander J., Greenwood, Aaron, McPherson, Alexander, Ivanov, K. I., Dorokhov, Y. L., Kim, C. H., Sálanki, Katalin, Carrére, Isabelle, Jacquemond, Mireille, Tepfer, Mark, Balazs, Ervin, Sanz, A. I., Serra, M. T., García-Luque, I., Revers, F., Candresse, T., LeGall, O., Souche, S., Lot, H., Dunez, J., Cecchini, E., Milner, J., Al-Kaff, N., Covey, S., Gong, Z., Geri, C., Covey, S. N., Richert-Pöggeler, K. R., Shepherd, R. J., Casper, R., Meiri, Eti, Raccah, B., Gera, A., Singer, S., Allam, E. K., El Afifi, Soheir I., Abo El Nasr, M. A., Abd El Ghaffar, M. H., Elisabeth Johansen, I., Keller, K. E., Hampton, R. O., SÕrensen, Karina, Bishnoi, S. S., Rishi, Narayan, Gumedzoe, M. Y. D., Atissime, K., Yedibahoma, S., Wellink, Joan, Verver, Jan, Bertens, Peter, van Lent, Jan, Goldbach, Rob W., van Kammen, Ab, Lekkerkerker, Annemarie, Taylor, K. M., Spall, V. E., Lomonossoff, G. P., Yu. Morozov, S., Solovyev, A. G., Zelenina, D. A., Savenkov, E. I., Grdzelishvili, V. Z., Morozov, S. Y., Jansen, K. A. J., Wolfs, C. J. A. M., Lohuis, H., Verduin, B. J. M., Stein-Margolina, V. A., Hsu, Y. H., Chang, B. Y., Lin, N. S., Pilartz, Marcel, Jeske, Holger, Verchot, Jeanmarie, Baulcombe, David C., English, David J., Müller, E., Baulcombe, D. C., Malcuit, Isabelle, Kavanagh, Tony, Valkonen, J. P. T., Puurand, Ü., Merits, A., Rabinstein, F., Sorri, O., Saarma, M., Liao, Y. C., Vaquero-Martin, C., Monecke, M., Rohde, W., Prüfer, D., Fischer, R., Antignus, Y., Lachman, O., Pearlsman, M., Cohen, S., Qiu, W. P., Moyer, J. W., Feldhoff, A., Kikkert, M., Kormelink, R., Krczal, G., Peters, D., Szittya, György, Burgyán, József, Wvpijewski, K., Paduch-Cichal, E., Rezler, A., Skrzeczkowska, S., Augustyniak, J., Nemchinov, L., Maiss, E., Hadidi, A., Wittner, Anita, Palkovics, László, Balázs, Ervin, Crescenzi, A., Piazzolla, P., Kheyr-Pour, A., Dafalla, G. A., Lecoq, H., Gronenborn, B., Bauer, U., Laux, I., Hajimorad, M. R., Ding, X. S., Flasinski, Stanislaw, Cassidy, Pour G., Dugdale, B., Beetham, P. R., Harding, R. M., Dale, J. L., Qiu, G., Shaw, J. G., Molnár, A., Más, P., Balsalobre, J. M., Sánchez-Pina, M. A., Pallás, V., Rahontei, J., López, L., Lázara, J. J., Barón, M., Owens, R. A., Steger, G., Hu, Y., Fels, A., Hammond, R. W., Riesner, D., Schröder, A. R. W., Góra, A., Pawlowicz, J., Kierzek, A., Zagorski, W., Baumstark, T., Schiebel, W., Schiebel, R., Axmann, A., Haas, B., Sänger, H. L., Xicai, Yang, Yin, Yie, Feng, Zhu, Yule, Liu, Liangyi, Kang, Po, Tien, Poliyka, H., Staub, U., Wagner, M., Gross, H. J., Sano, Teruo, Ishiguro, Akiro, Fayos, J., Garro, R., Bellés, J. M., Conejero, V., Bonfiglioli, R. G., Webb, D. R., Symons, R. H., El-Dougdoug, K. A., Abo-Zeid, A. A., Ambrós, S., Hernandez, C., Desvignes, J. C. C., Flores, R., d’Aquilio, M., Lisa, V., Boccardo, G., Vera, A., Daròs, J. A., Henkel, J., Spieker, R., Higgins, C., Turley, R., Chamberlain, D., Bateson, M., Dale, J., d’Aquino, L., Ragozzino, A., Henderson, J., Bateson, M. F., Chaleeprom, W., Gibbs, A. J., Graichen, K., Rabenstein, F., Schliephake, E., Smith, H. G., Stevens, M., Sadowy, E., Hulanicka, D., Wegener, B., Martin, M. T., Wetzel, T., Cook, G., Kasdorf, G. G. F., Pietersen, G., Braithwaite, Kathryn S., Gambley, Cherie F., Smith, Grant R., Druka, Arnis, Villegas, Lucille, Dahal, Ganesh, Hull, Roger, Senchugova, N. A., Büchen-Osmond, C., Dallwitz, M. J., Blaine, L. D., Naik, P. S., Sonone, A. B., Kolaskar, A. S., Sgro, J. Y., Palmenberg, A. C., Leclerc, Denis, Hohn, Thomas, Moriones, E., Batlle, A., Luis, M., Alvarez, J., Bernal, J. J., Alonso, J. L., Spak, J., Kubelkova, D., Kuo, T. T., Gachechiladze, K. K., Adamia, R. S., Balardshishvili, N. S., Chanishvili, T. G., Krüger, D. H., Nagy, Tibor, Élö, Péter, Papp, Péter, Orosz, László, Licis, N., Berzins, V., Sariol-Carbelo, Carlos A., RodrCarlos, C. M., Janzen, D., Ward, Colin W., Scott, S. W., Shiel, P. J., Berger, P. H., Aleman, M. E., Beachy, R. N., Fauquet, C. M., Salm, S. N., Rybicki, E. P., Rey, M. E. C., Briddon, R. W., Harper, G., Druka, A., Phillips, S., Brunt, A. A., Hull, R., Hay, Jo, Dasgupta, Indranil, Zaifeng, Fan, Meehan, Brian M., Todd, Daniel, Bunk, Hans-Jörk, Grieco, F., Martelli, G. P., Saldarelli, P., Minafra, A., Morag, A., Mumcuoglu, M., Baybikov, T., Schlesinger, M., Zakay-Rones, Z., Shohat, B., Shohat, M., Miller, M., Shaklay, M., Kalvatchev, Z., Walder, R., Garzaro, D., Barrios, M., Karagöz, Ali, Kuru, Avni, Karim, M. R., Johnson, A. J., Takida, S., Thompson, M. C., Omer, H. M. K., Omer, O. L. M., Biyiti, L., Amvam, R. H., Lamaty, G., Bouchet, P., Xu, J., Hefferon, K. L., Abou Haidar, M. G., and Meng, A. X. X.

Published

1997

6. BALLOON CELL MELANOMA: AN UNCOMMON ENTITY REPRESENTING A DIAGNOSTIC PITFALL IN DERMATOPATHOLOGY

Author

Broggi, G., Garro, R., Terranova, M., Argenziano, G., Puzzo, L., and Caltabiano, R.

Published

2019

7. Potential prognostic role of mif in discoid lupus erythematosus

Author

Broggi, G., Piombino, E., Garro, R., De Pasquale, R., Vecchio, G. M., and Caltabiano, R.

Published

2019

8. Abstracts of presentations on plant protection issues at the fifth international Mango Symposium Abstracts of presentations on plant protection issues at the Xth international congress of Virology: September 1-6, 1996 Dan Panorama Hotel, Tel Aviv, Israel August 11-16, 1996 Binyanei haoma, Jerusalem, Israel

Author

Peña, J., Wysoki, M., Singh, Gajendra, Boscán de M., Nancy, Godoy, Freddy, Obligado, A., Rossetto, C., Ribeiro, I., Gallo, P., Soares, N., Sabino, J., Martins, A., Bortoletto, N., Ploetz, R., Benscher, D., Vázquez, Aimé, Colls, A., Nagel, Julianne, Schaffer, B., Pinkas, Y., Maymon, M., Freeman, S., Bostros Bastawros, Mikhail, Gosbee, M., Johnson, G., Joyce, D., Irwin, J., Saaiman, W., Prusky, D., Falik, E., Kobiler, I., Fuchs, Y., Zauberman, G., Pesis, E., Ackerman, M., Roth, I., Weksler, A., Yekutiely, O., Waisblum, A., Keinan, A., Ofek, G., Reved, R., Barak, R., Bel, P., Artes, L., Visarathanonth, N., Xu, Z., Ponce de León, L., Muñoz, C., Pérez, L., Diaz de León, F., Kerbel, C., Esparza, S., Bósquez, E., Trinidad, M., Coates, L., Cooke, A., Dean, J., Lucia Duarte, Ana, Alberto Otto, Paulo, Malavasi, Aldo, Lizado, M., Bautista, M., Bacalangco, N., Farungsang, U., Farungsang, N., Waskar, D., Masalkar, S., Gaikwad, R., Damame, S., Bally, Ian, O'Hare, Tim, Holmes, Rowland, Atabekov, J., Fauquet, Claude, Tomori, O., Nuss, D., Ahlquist, P., Díez, J., Ishikawa, M., Janda, M., Price, B., Restrepo-Hartwig, M., Bol, J., van Rossum, C., Garcia, M., van der Vossen, E., Reusken, Chantal, Canto, T., Gal-On, A., Palukaitis, P., Roossinck, M., Flasinski, S., Restrepo-Hartwig, Maria, Ahlquist, Paul, Smirnyagina, Ekaterina, Lin, Na-Sheng, Nagy, Peter, Figlerowicz, Marek, Bujarski, Jozef, Proll, D., Guyatt, K., Davidson, A., Kim, Kook-Hyung, Miller, Eric, Hemenway, Cynthia, Havelda, Z., Dalmay, T., Burgyán, J., Kearney, C., Thomson, M., Roland, K., Dawson, W., Bao, Y., Carter, S., Nelson, R., Derrick, P., Shun Ding, Xin, Eskarous, J., Sarkar, S., El-Shamy, M., Chen, J., Sako, N., Yuichiro, W., Ohshima, K., Okada, Y., Felden, Brice, Kuznetsov, Yuri, Malkin, Alexander, Greenwood, Aaron, McPherson, Alexander, Ivanov, K., Dorokhov, Y., Kim, C., Sálanki, Katalin, Carrére, Isabelle, Jacquemond, Mireille, Tepfer, Mark, Balazs, Ervin, Sanz, A., Serra, M., García-Luque, I., Revers, F., Candresse, T., LeGall, O., Souche, S., Lot, H., Dunez, J., Cecchini, E., Milner, J., Al-Kaff, N., Covey, S., Gong, Z., Geri, C., Richert-Pöggeler, K., Shepherd, R., Casper, R., Meiri, Eti, Raccah, B., Gera, A., Singer, S., Allam, E., El Afifi, Soheir, Abo El Nasr, M., Abd El Ghaffar, M., Elisabeth Johansen, I., Keller, K., Hampton, R., SÕrensen, Karina, Bishnoi, S., Rishi, Narayan, Gumedzoe, M., Atissime, K., Yedibahoma, S., Wellink, Joan, Verver, Jan, Bertens, Peter, van Lent, Jan, Goldbach, Rob, van Kammen, Ab, Lekkerkerker, Annemarie, Taylor, K., Spall, V., Lomonossoff, G., Yu. Morozov, S., Solovyev, A., Zelenina, D., Savenkov, E., Grdzelishvili, V., Morozov, S., Jansen, K., Wolfs, C., Lohuis, H., Verduin, B., Stein-Margolina, V., Hsu, Y., Chang, B., Lin, N., Pilartz, Marcel, Jeske, Holger, Verchot, Jeanmarie, Baulcombe, David, English, David, Müller, E., Baulcombe, D., Malcuit, Isabelle, Kavanagh, Tony, Valkonen, J., Puurand, Ü., Merits, A., Rabinstein, F., Sorri, O., Saarma, M., Liao, Y., Vaquero-Martin, C., Monecke, M., Rohde, W., Prüfer, D., Fischer, R., Antignus, Y., Lachman, O., Pearlsman, M., Cohen, S., Qiu, W., Moyer, J., Feldhoff, A., Kikkert, M., Kormelink, R., Krczal, G., Peters, D., Szittya, György, Burgyán, József, Wvpijewski, K., Paduch-Cichal, E., Rezler, A., Skrzeczkowska, S., Augustyniak, J., Nemchinov, L., Maiss, E., Hadidi, A., Wittner, Anita, Palkovics, László, Balázs, Ervin, Crescenzi, A., Piazzolla, P., Kheyr-Pour, A., Dafalla, G., Lecoq, H., Gronenborn, B., Bauer, U., Laux, I., Hajimorad, M., Ding, X., Flasinski, Stanislaw, Cassidy, Pour, Dugdale, B., Beetham, P., Harding, R., Dale, J., Qiu, G., Shaw, J., Molnár, A., Más, P., Balsalobre, J., Sánchez-Pina, M., Pallás, V., Rahontei, J., López, L., Lázara, J., Barón, M., Owens, R., Steger, G., Hu, Y., Fels, A., Hammond, R., Riesner, D., Schröder, A., Góra, A., Pawlowicz, J., Kierzek, A., Zagorski, W., Baumstark, T., Schiebel, W., Schiebel, R., Axmann, A., Haas, B., Sänger, H., Xicai, Yang, Yin, Yie, Feng, Zhu, Yule, Liu, Liangyi, Kang, Po, Tien, Poliyka, H., Staub, U., Wagner, M., Gross, H., Sano, Teruo, Ishiguro, Akiro, Fayos, J., Garro, R., Bellés, J., Conejero, V., Bonfiglioli, R., Webb, D., Symons, R., El-Dougdoug, K., Abo-Zeid, A., Ambrós, S., Hernandez, C., Desvignes, J., Flores, R., d'Aquilio, M., Lisa, V., Boccardo, G., Vera, A., Daròs, J., Henkel, J., Spieker, R., Higgins, C., Turley, R., Chamberlain, D., Bateson, M., d'Aquino, L., Ragozzino, A., Henderson, J., Chaleeprom, W., Gibbs, A., Graichen, K., Rabenstein, F., Schliephake, E., Smith, H., Stevens, M., Sadowy, E., Hulanicka, D., Wegener, B., Martin, M., Wetzel, T., Cook, G., Kasdorf, G., Pietersen, G., Braithwaite, Kathryn, Gambley, Cherie, Smith, Grant, Druka, Arnis, Villegas, Lucille, Dahal, Ganesh, Hull, Roger, Senchugova, N., Büchen-Osmond, C., Dallwitz, M., Blaine, L., Naik, P., Sonone, A., Kolaskar, A., Sgro, J., Palmenberg, A., Leclerc, Denis, Hohn, Thomas, Moriones, E., Batlle, A., Luis, M., Alvarez, J., Bernal, J., Alonso, J., Spak, J., Kubelkova, D., Kuo, T., Gachechiladze, K., Adamia, R., Balardshishvili, N., Chanishvili, T., Krüger, D., Nagy, Tibor, Élö, Péter, Papp, Péter, Orosz, László, Licis, N., Berzins, V., Sariol-Carbelo, Carlos, RodrCarlos, C., Janzen, D., Ward, Colin, Scott, S., Shiel, P., Berger, P., Aleman, M., Beachy, R., Fauquet, C., Salm, S., Rybicki, E., Rey, M., Briddon, R., Harper, G., Druka, A., Phillips, S., Brunt, A., Hull, R., Hay, Jo, Dasgupta, Indranil, Zaifeng, Fan, Meehan, Brian, Todd, Daniel, Bunk, Hans-Jörk, Grieco, F., Martelli, G., Saldarelli, P., Minafra, A., Morag, A., Mumcuoglu, M., Baybikov, T., Schlesinger, M., Zakay-Rones, Z., Shohat, B., Shohat, M., Miller, M., Shaklay, M., Kalvatchev, Z., Walder, R., Garzaro, D., Barrios, M., Karagöz, Ali, Kuru, Avni, Karim, M., Johnson, A., Takida, S., Thompson, M., Omer, H., Omer, O., Biyiti, L., Amvam, R., Lamaty, G., Bouchet, P., Xu, J., Hefferon, K., Abou Haidar, M., and Meng, A.

Published

2018

9. Effect of the initial live weight on carcass, viscera and beef cuts parameters of feedlot-finished steers

Author

Gelid, Lucas Fernando, Alende, Mariano, Ortiz, Daniela Alejandra, Camiletti, F., Murcia, V., Hurtado, A., Porta, Fernando, Garro, R., Camilletti, M., and Volpi-Lagreca, Gabriela

Published

2018

10. Cytomegalovirus (CMV) Infection in Pediatric Solid Organ Transplant Recipients and Role of Prophylaxis

Author

Nance, G., primary, Serluco, A., additional, Deshpande, S.R., additional, Garro, R., additional, George, R.P., additional, Kelleman, M.S., additional, and Liverman, R., additional

Published

2018

11. (932) - Cytomegalovirus (CMV) Infection in Pediatric Solid Organ Transplant Recipients and Role of Prophylaxis

Author

Nance, G., Serluco, A., Deshpande, S.R., Garro, R., George, R.P., Kelleman, M.S., and Liverman, R.

Published

2018

12. Metodología para la cría de parásitos del minador de hojas de cítricos Phyllocnistis citrella

Author

Serrano, C., Capilla, M. A., Franch, J. J., Ripollés, José Luis, Mazzini, M. C., Monton, E., Vercher, Rosa, Garro, R., Costa Comelles, J., and García-Marí, Ferran

Subjects

Cría de insectos, H10 Pests of plants, Phyllocnistis citrella, L72 Pests of animals, Enemigos naturales, Insectarios, Ageniaspis citricola, Parásitos

Abstract

El minador de hojas de cítricos Phyllocnystis citrella Stainton (Lepidoptera: Gracillariidae) es una plaga originaria del Sudeste asiático que inicia al principio de la década de los 90 un extraordinario proceso de expansión por las restantes zonas del mundo productoras de cítricos. Entre 1993 y 1996 se expande por toda la zona mediterránea y el continente americano con gran rapidez. En la Comunidad Valenciana alcanza niveles poblacionales muy elevados y causa daños muy importantes a las brotaciones de verano en los dos últimos años, 1995 y 1996. De manera inmediata se han tomado medidas de tipo químico para su control, pero se considera que a largo plazo sus poblaciones deben ser reguladas mediante el control biológico.

Published

1996

13. “ITʼS ALL IN HIS HEAD”: OBSESSIVE-COMPULSIVE DISORDER LEADS TO CEREBRAL VENOUS THROMBOSIS.

Author

Garro, R., primary, Estes, M. R., additional, Lucas, M. A., additional, and Smalligan, R. D., additional

Published

2007

14. Lewis acid-containing mesoporous molecular sieves as solid efficient catalysts for solvent-free Mukaiyama-type aldol condensation

Author

GARRO, R, primary, NAVARRO, M, additional, PRIMO, J, additional, and CORMA, A, additional

Published

2005

15. C7(P32) and C6(P34) PR proteins induced in tomato leaves by citrus exocortis viroid infection are chitinases

Author

Breijo, F.J.García, primary, Garro, R., additional, and Conejero, V., additional

Published

1990

16. Introduction of Aedes albopictus into a La Crosse virus--enzootic site in Illinois.

Author

Kitron, Uriel, Swanson, Jack, Crandell, Michael, Sullivan, Patrick J., Anderson, Justin, Garro, Robert, Haramis, Linn D., Grimstad, Paul R., Kitron, U, Swanson, J, Crandell, M, Sullivan, P J, Anderson, J, Garro, R, Haramis, L D, and Grimstad, P R

Subjects

AEDES albopictus, VIRUS diseases

Abstract

In late summer and fall 1997, Aedes albopictus mosquitoes were found in Peoria, Illinois, a long recognized focus of La Crosse virus transmission. Larvae were found in tires and other artificial containers, biting adults were recovered, and eggs were collected in oviposition traps within a 25-ha area. One chipmunk trapped < 0.25 km from the infested area tested positive for neutralizing antibodies against La Crosse virus. [ABSTRACT FROM AUTHOR]

Published

1998

17. Abstracts of presentations on plant protection issues at the fifth international Mango Symposium Abstracts of presentations on plant protection issues at the Xth international congress of Virology: September 1-6, 1996 Dan Panorama Hotel, Tel Aviv, Israel August 11-16, 1996 Binyanei haoma, Jerusalem, Israel

Author

Peña, J., Wysoki, M., Singh, Gajendra, Boscán de M., Nancy, Godoy, Freddy, Obligado, A., Rossetto, C., Ribeiro, I., Gallo, P., Soares, N., Sabino, J., Martins, A., Bortoletto, N., Ploetz, R., Benscher, D., Vázquez, Aimé, Colls, A., Nagel, Julianne, Schaffer, B., Pinkas, Y., Maymon, M., Freeman, S., Bostros Bastawros, Mikhail, Gosbee, M., Johnson, G., Joyce, D., Irwin, J., Saaiman, W., Prusky, D., Falik, E., Kobiler, I., Fuchs, Y., Zauberman, G., Pesis, E., Ackerman, M., Roth, I., Weksler, A., Yekutiely, O., Waisblum, A., Keinan, A., Ofek, G., Reved, R., Barak, R., Bel, P., Artes, L., Visarathanonth, N., Xu, Z., Ponce de León, L., Muñoz, C., Pérez, L., Diaz de León, F., Kerbel, C., Esparza, S., Bósquez, E., Trinidad, M., Coates, L., Cooke, A., Dean, J., Lucia Duarte, Ana, Alberto Otto, Paulo, Malavasi, Aldo, Lizado, M., Bautista, M., Bacalangco, N., Farungsang, U., Farungsang, N., Waskar, D., Masalkar, S., Gaikwad, R., Damame, S., Bally, Ian, O'Hare, Tim, Holmes, Rowland, Atabekov, J., Fauquet, Claude, Tomori, O., Nuss, D., Ahlquist, P., Díez, J., Ishikawa, M., Janda, M., Price, B., Restrepo-Hartwig, M., Bol, J., van Rossum, C., Garcia, M., van der Vossen, E., Reusken, Chantal, Canto, T., Gal-On, A., Palukaitis, P., Roossinck, M., Flasinski, S., Restrepo-Hartwig, Maria, Ahlquist, Paul, Smirnyagina, Ekaterina, Lin, Na-Sheng, Nagy, Peter, Figlerowicz, Marek, Bujarski, Jozef, Proll, D., Guyatt, K., Davidson, A., Kim, Kook-Hyung, Miller, Eric, Hemenway, Cynthia, Havelda, Z., Dalmay, T., Burgyán, J., Kearney, C., Thomson, M., Roland, K., Dawson, W., Bao, Y., Carter, S., Nelson, R., Derrick, P., Shun Ding, Xin, Eskarous, J., Sarkar, S., El-Shamy, M., Chen, J., Sako, N., Yuichiro, W., Ohshima, K., Okada, Y., Felden, Brice, Kuznetsov, Yuri, Malkin, Alexander, Greenwood, Aaron, McPherson, Alexander, Ivanov, K., Dorokhov, Y., Kim, C., Sálanki, Katalin, Carrére, Isabelle, Jacquemond, Mireille, Tepfer, Mark, Balazs, Ervin, Sanz, A., Serra, M., García-Luque, I., Revers, F., Candresse, T., LeGall, O., Souche, S., Lot, H., Dunez, J., Cecchini, E., Milner, J., Al-Kaff, N., Covey, S., Gong, Z., Geri, C., Richert-Pöggeler, K., Shepherd, R., Casper, R., Meiri, Eti, Raccah, B., Gera, A., Singer, S., Allam, E., El Afifi, Soheir, Abo El Nasr, M., Abd El Ghaffar, M., Elisabeth Johansen, I., Keller, K., Hampton, R., SÕrensen, Karina, Bishnoi, S., Rishi, Narayan, Gumedzoe, M., Atissime, K., Yedibahoma, S., Wellink, Joan, Verver, Jan, Bertens, Peter, van Lent, Jan, Goldbach, Rob, van Kammen, Ab, Lekkerkerker, Annemarie, Taylor, K., Spall, V., Lomonossoff, G., Yu. Morozov, S., Solovyev, A., Zelenina, D., Savenkov, E., Grdzelishvili, V., Morozov, S., Jansen, K., Wolfs, C., Lohuis, H., Verduin, B., Stein-Margolina, V., Hsu, Y., Chang, B., Lin, N., Pilartz, Marcel, Jeske, Holger, Verchot, Jeanmarie, Baulcombe, David, English, David, Müller, E., Baulcombe, D., Malcuit, Isabelle, Kavanagh, Tony, Valkonen, J., Puurand, Ü., Merits, A., Rabinstein, F., Sorri, O., Saarma, M., Liao, Y., Vaquero-Martin, C., Monecke, M., Rohde, W., Prüfer, D., Fischer, R., Antignus, Y., Lachman, O., Pearlsman, M., Cohen, S., Qiu, W., Moyer, J., Feldhoff, A., Kikkert, M., Kormelink, R., Krczal, G., Peters, D., Szittya, György, Burgyán, József, Wvpijewski, K., Paduch-Cichal, E., Rezler, A., Skrzeczkowska, S., Augustyniak, J., Nemchinov, L., Maiss, E., Hadidi, A., Wittner, Anita, Palkovics, László, Balázs, Ervin, Crescenzi, A., Piazzolla, P., Kheyr-Pour, A., Dafalla, G., Lecoq, H., Gronenborn, B., Bauer, U., Laux, I., Hajimorad, M., Ding, X., Flasinski, Stanislaw, Cassidy, Pour, Dugdale, B., Beetham, P., Harding, R., Dale, J., Qiu, G., Shaw, J., Molnár, A., Más, P., Balsalobre, J., Sánchez-Pina, M., Pallás, V., Rahontei, J., López, L., Lázara, J., Barón, M., Owens, R., Steger, G., Hu, Y., Fels, A., Hammond, R., Riesner, D., Schröder, A., Góra, A., Pawlowicz, J., Kierzek, A., Zagorski, W., Baumstark, T., Schiebel, W., Schiebel, R., Axmann, A., Haas, B., Sänger, H., Xicai, Yang, Yin, Yie, Feng, Zhu, Yule, Liu, Liangyi, Kang, Po, Tien, Poliyka, H., Staub, U., Wagner, M., Gross, H., Sano, Teruo, Ishiguro, Akiro, Fayos, J., Garro, R., Bellés, J., Conejero, V., Bonfiglioli, R., Webb, D., Symons, R., El-Dougdoug, K., Abo-Zeid, A., Ambrós, S., Hernandez, C., Desvignes, J., Flores, R., d'Aquilio, M., Lisa, V., Boccardo, G., Vera, A., Daròs, J., Henkel, J., Spieker, R., Higgins, C., Turley, R., Chamberlain, D., Bateson, M., d'Aquino, L., Ragozzino, A., Henderson, J., Chaleeprom, W., Gibbs, A., Graichen, K., Rabenstein, F., Schliephake, E., Smith, H., Stevens, M., Sadowy, E., Hulanicka, D., Wegener, B., Martin, M., Wetzel, T., Cook, G., Kasdorf, G., Pietersen, G., Braithwaite, Kathryn, Gambley, Cherie, Smith, Grant, Druka, Arnis, Villegas, Lucille, Dahal, Ganesh, Hull, Roger, Senchugova, N., Büchen-Osmond, C., Dallwitz, M., Blaine, L., Naik, P., Sonone, A., Kolaskar, A., Sgro, J., Palmenberg, A., Leclerc, Denis, Hohn, Thomas, Moriones, E., Batlle, A., Luis, M., Alvarez, J., Bernal, J., Alonso, J., Spak, J., Kubelkova, D., Kuo, T., Gachechiladze, K., Adamia, R., Balardshishvili, N., Chanishvili, T., Krüger, D., Nagy, Tibor, Élö, Péter, Papp, Péter, Orosz, László, Licis, N., Berzins, V., Sariol-Carbelo, Carlos, RodrCarlos, C., Janzen, D., Ward, Colin, Scott, S., Shiel, P., Berger, P., Aleman, M., Beachy, R., Fauquet, C., Salm, S., Rybicki, E., Rey, M., Briddon, R., Harper, G., Druka, A., Phillips, S., Brunt, A., Hull, R., Hay, Jo, Dasgupta, Indranil, Zaifeng, Fan, Meehan, Brian, Todd, Daniel, Bunk, Hans-Jörk, Grieco, F., Martelli, G., Saldarelli, P., Minafra, A., Morag, A., Mumcuoglu, M., Baybikov, T., Schlesinger, M., Zakay-Rones, Z., Shohat, B., Shohat, M., Miller, M., Shaklay, M., Kalvatchev, Z., Walder, R., Garzaro, D., Barrios, M., Karagöz, Ali, Kuru, Avni, Karim, M., Johnson, A., Takida, S., Thompson, M., Omer, H., Omer, O., Biyiti, L., Amvam, R., Lamaty, G., Bouchet, P., Xu, J., Hefferon, K., Abou Haidar, M., Meng, A., Peña, J., Wysoki, M., Singh, Gajendra, Boscán de M., Nancy, Godoy, Freddy, Obligado, A., Rossetto, C., Ribeiro, I., Gallo, P., Soares, N., Sabino, J., Martins, A., Bortoletto, N., Ploetz, R., Benscher, D., Vázquez, Aimé, Colls, A., Nagel, Julianne, Schaffer, B., Pinkas, Y., Maymon, M., Freeman, S., Bostros Bastawros, Mikhail, Gosbee, M., Johnson, G., Joyce, D., Irwin, J., Saaiman, W., Prusky, D., Falik, E., Kobiler, I., Fuchs, Y., Zauberman, G., Pesis, E., Ackerman, M., Roth, I., Weksler, A., Yekutiely, O., Waisblum, A., Keinan, A., Ofek, G., Reved, R., Barak, R., Bel, P., Artes, L., Visarathanonth, N., Xu, Z., Ponce de León, L., Muñoz, C., Pérez, L., Diaz de León, F., Kerbel, C., Esparza, S., Bósquez, E., Trinidad, M., Coates, L., Cooke, A., Dean, J., Lucia Duarte, Ana, Alberto Otto, Paulo, Malavasi, Aldo, Lizado, M., Bautista, M., Bacalangco, N., Farungsang, U., Farungsang, N., Waskar, D., Masalkar, S., Gaikwad, R., Damame, S., Bally, Ian, O'Hare, Tim, Holmes, Rowland, Atabekov, J., Fauquet, Claude, Tomori, O., Nuss, D., Ahlquist, P., Díez, J., Ishikawa, M., Janda, M., Price, B., Restrepo-Hartwig, M., Bol, J., van Rossum, C., Garcia, M., van der Vossen, E., Reusken, Chantal, Canto, T., Gal-On, A., Palukaitis, P., Roossinck, M., Flasinski, S., Restrepo-Hartwig, Maria, Ahlquist, Paul, Smirnyagina, Ekaterina, Lin, Na-Sheng, Nagy, Peter, Figlerowicz, Marek, Bujarski, Jozef, Proll, D., Guyatt, K., Davidson, A., Kim, Kook-Hyung, Miller, Eric, Hemenway, Cynthia, Havelda, Z., Dalmay, T., Burgyán, J., Kearney, C., Thomson, M., Roland, K., Dawson, W., Bao, Y., Carter, S., Nelson, R., Derrick, P., Shun Ding, Xin, Eskarous, J., Sarkar, S., El-Shamy, M., Chen, J., Sako, N., Yuichiro, W., Ohshima, K., Okada, Y., Felden, Brice, Kuznetsov, Yuri, Malkin, Alexander, Greenwood, Aaron, McPherson, Alexander, Ivanov, K., Dorokhov, Y., Kim, C., Sálanki, Katalin, Carrére, Isabelle, Jacquemond, Mireille, Tepfer, Mark, Balazs, Ervin, Sanz, A., Serra, M., García-Luque, I., Revers, F., Candresse, T., LeGall, O., Souche, S., Lot, H., Dunez, J., Cecchini, E., Milner, J., Al-Kaff, N., Covey, S., Gong, Z., Geri, C., Richert-Pöggeler, K., Shepherd, R., Casper, R., Meiri, Eti, Raccah, B., Gera, A., Singer, S., Allam, E., El Afifi, Soheir, Abo El Nasr, M., Abd El Ghaffar, M., Elisabeth Johansen, I., Keller, K., Hampton, R., SÕrensen, Karina, Bishnoi, S., Rishi, Narayan, Gumedzoe, M., Atissime, K., Yedibahoma, S., Wellink, Joan, Verver, Jan, Bertens, Peter, van Lent, Jan, Goldbach, Rob, van Kammen, Ab, Lekkerkerker, Annemarie, Taylor, K., Spall, V., Lomonossoff, G., Yu. Morozov, S., Solovyev, A., Zelenina, D., Savenkov, E., Grdzelishvili, V., Morozov, S., Jansen, K., Wolfs, C., Lohuis, H., Verduin, B., Stein-Margolina, V., Hsu, Y., Chang, B., Lin, N., Pilartz, Marcel, Jeske, Holger, Verchot, Jeanmarie, Baulcombe, David, English, David, Müller, E., Baulcombe, D., Malcuit, Isabelle, Kavanagh, Tony, Valkonen, J., Puurand, Ü., Merits, A., Rabinstein, F., Sorri, O., Saarma, M., Liao, Y., Vaquero-Martin, C., Monecke, M., Rohde, W., Prüfer, D., Fischer, R., Antignus, Y., Lachman, O., Pearlsman, M., Cohen, S., Qiu, W., Moyer, J., Feldhoff, A., Kikkert, M., Kormelink, R., Krczal, G., Peters, D., Szittya, György, Burgyán, József, Wvpijewski, K., Paduch-Cichal, E., Rezler, A., Skrzeczkowska, S., Augustyniak, J., Nemchinov, L., Maiss, E., Hadidi, A., Wittner, Anita, Palkovics, László, Balázs, Ervin, Crescenzi, A., Piazzolla, P., Kheyr-Pour, A., Dafalla, G., Lecoq, H., Gronenborn, B., Bauer, U., Laux, I., Hajimorad, M., Ding, X., Flasinski, Stanislaw, Cassidy, Pour, Dugdale, B., Beetham, P., Harding, R., Dale, J., Qiu, G., Shaw, J., Molnár, A., Más, P., Balsalobre, J., Sánchez-Pina, M., Pallás, V., Rahontei, J., López, L., Lázara, J., Barón, M., Owens, R., Steger, G., Hu, Y., Fels, A., Hammond, R., Riesner, D., Schröder, A., Góra, A., Pawlowicz, J., Kierzek, A., Zagorski, W., Baumstark, T., Schiebel, W., Schiebel, R., Axmann, A., Haas, B., Sänger, H., Xicai, Yang, Yin, Yie, Feng, Zhu, Yule, Liu, Liangyi, Kang, Po, Tien, Poliyka, H., Staub, U., Wagner, M., Gross, H., Sano, Teruo, Ishiguro, Akiro, Fayos, J., Garro, R., Bellés, J., Conejero, V., Bonfiglioli, R., Webb, D., Symons, R., El-Dougdoug, K., Abo-Zeid, A., Ambrós, S., Hernandez, C., Desvignes, J., Flores, R., d'Aquilio, M., Lisa, V., Boccardo, G., Vera, A., Daròs, J., Henkel, J., Spieker, R., Higgins, C., Turley, R., Chamberlain, D., Bateson, M., d'Aquino, L., Ragozzino, A., Henderson, J., Chaleeprom, W., Gibbs, A., Graichen, K., Rabenstein, F., Schliephake, E., Smith, H., Stevens, M., Sadowy, E., Hulanicka, D., Wegener, B., Martin, M., Wetzel, T., Cook, G., Kasdorf, G., Pietersen, G., Braithwaite, Kathryn, Gambley, Cherie, Smith, Grant, Druka, Arnis, Villegas, Lucille, Dahal, Ganesh, Hull, Roger, Senchugova, N., Büchen-Osmond, C., Dallwitz, M., Blaine, L., Naik, P., Sonone, A., Kolaskar, A., Sgro, J., Palmenberg, A., Leclerc, Denis, Hohn, Thomas, Moriones, E., Batlle, A., Luis, M., Alvarez, J., Bernal, J., Alonso, J., Spak, J., Kubelkova, D., Kuo, T., Gachechiladze, K., Adamia, R., Balardshishvili, N., Chanishvili, T., Krüger, D., Nagy, Tibor, Élö, Péter, Papp, Péter, Orosz, László, Licis, N., Berzins, V., Sariol-Carbelo, Carlos, RodrCarlos, C., Janzen, D., Ward, Colin, Scott, S., Shiel, P., Berger, P., Aleman, M., Beachy, R., Fauquet, C., Salm, S., Rybicki, E., Rey, M., Briddon, R., Harper, G., Druka, A., Phillips, S., Brunt, A., Hull, R., Hay, Jo, Dasgupta, Indranil, Zaifeng, Fan, Meehan, Brian, Todd, Daniel, Bunk, Hans-Jörk, Grieco, F., Martelli, G., Saldarelli, P., Minafra, A., Morag, A., Mumcuoglu, M., Baybikov, T., Schlesinger, M., Zakay-Rones, Z., Shohat, B., Shohat, M., Miller, M., Shaklay, M., Kalvatchev, Z., Walder, R., Garzaro, D., Barrios, M., Karagöz, Ali, Kuru, Avni, Karim, M., Johnson, A., Takida, S., Thompson, M., Omer, H., Omer, O., Biyiti, L., Amvam, R., Lamaty, G., Bouchet, P., Xu, J., Hefferon, K., Abou Haidar, M., and Meng, A.

18. Microvascular Inflammation of Kidney Allografts and Clinical Outcomes.

Author

Sablik M, Sannier A, Raynaud M, Goutaudier V, Divard G, Astor BC, Weng P, Smith J, Garro R, Warady BA, Zahr RS, Twombley K, Dharnidharka VR, Dandamudi RS, Fila M, Huang E, Sellier-Leclerc AL, Tönshoff B, Rabant M, Verine J, Del Bello A, Berney T, Boyer O, Catar RA, Danger R, Giral M, Yoo D, Girardin FR, Alsadi A, Gourraud PA, Morelon E, Le Quintrec M, Try M, Villard J, Zhong W, Bestard O, Budde K, Chauveau B, Couzi L, Brouard S, Hogan J, Legendre C, Anglicheau D, Aubert O, Kamar N, Lefaucheur C, and Loupy A

Abstract

Background: The heterogeneous clinical presentation of graft microvascular inflammation poses a major challenge to successful kidney transplantation. The effect of microvascular inflammation on allograft outcomes is unclear., Methods: We conducted a cohort study that included kidney-transplant recipients from more than 30 transplantation centers in Europe and North America who had undergone allograft biopsy between 2004 and 2023. We integrated clinical and pathological data to classify biopsy specimens according to the 2022 Banff Classification of Renal Allograft Pathology, which includes two new diagnostic categories: probable antibody-mediated rejection and microvascular inflammation without evidence of an antibody-mediated response. We then assessed the association between the newly recognized microvascular inflammation phenotypes and allograft survival and disease progression., Results: A total of 16,293 kidney-transplant biopsy specimens from 6798 patients were assessed. We identified the newly recognized microvascular inflammation phenotypes in 788 specimens, of which 641 were previously categorized as specimens with no evidence of rejection. As compared with patients without rejection, the hazard ratio for graft loss was 2.1 (95% confidence interval [CI], 1.5 to 3.1) among patients with microvascular inflammation without evidence of an antibody-mediated response and 2.7 (95% CI, 2.2 to 3.3) among patients with antibody-mediated rejection. Patients with a diagnosis of probable antibody-mediated rejection had a higher risk of graft failure beyond year 5 after biopsy than those without rejection (hazard ratio, 1.7; 95% CI, 0.8 to 3.5). Patients with a diagnosis of either newly recognized microvascular inflammation phenotype had a higher risk of progression of transplant glomerulopathy during follow-up than patients without microvascular inflammation., Conclusions: Microvascular inflammation in kidney allografts includes distinct phenotypes, with various disease progression and allograft outcomes. Our findings support the clinical use of additional rejection phenotypes to standardize diagnostics for kidney allografts. (Funded by OrganX. ClinicalTrials.gov number, NCT06496269.)., (Copyright © 2024 Massachusetts Medical Society.)

Published

2024

19. Cell-free DNA for the detection of kidney allograft rejection.

Author

Aubert O, Ursule-Dufait C, Brousse R, Gueguen J, Racapé M, Raynaud M, Van Loon E, Pagliazzi A, Huang E, Jordan SC, Chavin KD, Gupta G, Kumar D, Alhamad T, Anand S, Sanchez-Garcia J, Abdalla BA, Hogan J, Garro R, Dadhania DM, Jain P, Mandelbrot DA, Naesens M, Dandamudi R, Dharnidharka VR, Anglicheau D, Lefaucheur C, and Loupy A

Subjects

Humans, Male, Female, Middle Aged, Adult, Allografts immunology, Biomarkers blood, Tissue Donors, Transplantation, Homologous, Aged, Graft Rejection diagnosis, Graft Rejection immunology, Graft Rejection genetics, Kidney Transplantation adverse effects, Cell-Free Nucleic Acids blood, Cell-Free Nucleic Acids genetics

Abstract

Donor-derived cell-free DNA (dd-cfDNA) is an emerging noninvasive biomarker that has the potential to detect allograft injury. The capacity of dd-cfDNA to detect kidney allograft rejection and its added clinical value beyond standard of care patient monitoring is unclear. We enrolled 2,882 kidney allograft recipients from 14 transplantation centers in Europe and the United States in an observational population-based study. The primary analysis included 1,134 patients. Donor-derived cell-free DNA levels strongly correlated with allograft rejection, including antibody-mediated rejection (P < 0.0001), T cell-mediated rejection (P < 0.0001) and mixed rejection (P < 0.0001). In multivariable analysis, circulating dd-cfDNA was significantly associated with allograft rejection (odds ratio 2.275; 95% confidence interval (CI) 1.902-2.739; P < 0.0001) independently of standard of care patient monitoring parameters. The inclusion of dd-cfDNA to a standard of care prediction model showed improved discrimination (area under the curve 0.777 (95% CI 0.741-0.811) to 0.821 (95% CI 0.784-0.852); P = 0.0011) and calibration. These results were confirmed in the external validation cohorts (n = 1,748) including a cohort of African American patients (n = 439). Finally, dd-cfDNA showed high predictive value to detect subclinical rejection in stable patients. Our study provides insights on the potential value of assessing dd-cfDNA, in addition to standard of care monitoring, to improve the detection of allograft rejection. ClinicalTrials.gov registration: NCT05995379 ., (© 2024. The Author(s).)

Published

2024

20. BK polyomavirus DNAemia, allograft rejection, and de novo donor-specific antibodies after lowering target tacrolimus levels in pediatric kidney transplant recipients.

Author

Huang HX, Xiang Y, George R, Winterberg P, Serluco A, Liverman R, Yildirim I, and Garro R

Subjects

Humans, Retrospective Studies, Male, Female, Child, Adolescent, Child, Preschool, DNA, Viral blood, Infant, Postoperative Complications blood, Postoperative Complications etiology, Postoperative Complications prevention & control, Postoperative Complications virology, Kidney Transplantation, BK Virus, Graft Rejection prevention & control, Graft Rejection blood, Graft Rejection immunology, Tacrolimus therapeutic use, Immunosuppressive Agents therapeutic use, Polyomavirus Infections blood, Tumor Virus Infections blood, Tumor Virus Infections immunology

Abstract

Background: BK polyomavirus (BKV) DNAemia is a challenging infectious complication after kidney transplant (KT). Reduction of immunosuppression is the mainstay of management, and tacrolimus is often the first immunosuppressive medication adjusted upon the diagnosis of BKV DNAemia. This study aimed to evaluate the impact of a new institutional protocol with lower target tacrolimus levels on BKV DNAemia, allograft rejection, and de novo donor-specific antibodies (dnDSA) among pediatric KT recipients., Methods: We conducted a retrospective chart review of all KT episodes between January 2013 and December 2018. The new protocol with lower target tacrolimus levels was implemented in March 2015. One hundred twenty-seven patients were included in primary analysis. All patients received induction with basiliximab and methylprednisolone and were maintained on a steroid-based immunosuppressive regimen., Results: In the post-intervention cohort, cumulative incidence of BKV DNAemia at 100 days (13.4% vs. 17.8%, p = .605) and 18 months post-KT (34.1% vs. 26.7%, p = .504) was not significantly different from the pre-intervention cohort. Biopsy-proven rejection rate did not change. However, we observed a trend toward earlier development of dnDSA in the post-intervention cohort using the Kaplan-Meier survival analysis (log-rank p = .06). Younger recipient age at the time of transplant was found to slightly increase the risk of BKV DNAemia (OR: 1.09, 95% CI [1.01, 1.16], p = .024). There was an association between BKV DNAemia and biopsy-proven rejection of any type ( adjusted OR: 2.77, 95% CI [1.26, 6.23], p = .012), especially acute T-cell-mediated rejection grade 1A and above ( adjusted OR: 2.95, 95% CI [1.06, 8.30], p = .037), after adjusted for recipient age at the time of transplant., Conclusions: Targeting lower tacrolimus levels did not decrease the incidence of BKV DNAemia within 100 days or 18 months post-KT, nor did it increase the risk of biopsy-proven rejection among pediatric KT recipients in our center. However, there was a trend toward earlier development of dnDSA, which may portend worse long-term graft outcome post-KT. Our findings highlight the need for individualized immunosuppressive regimens based on immunologic and infectious risk factors and the importance of implementing innovative biomarkers to guide therapy and improve outcomes., (© 2024 Wiley Periodicals LLC.)

Published

2024

21. Antibody-mediated rejection in pediatric kidney transplant recipients: A report from the Pediatric Nephrology Research Consortium.

Author

Ashoor IF, Engen RM, Puliyanda D, Hayde N, Peterson CG, Zahr RS, Solomon S, Kallash M, Garro R, Jain A, Harshman LA, McEwen ST, Mansuri A, Gregoski MJ, and Twombley KE

Subjects

Humans, Child, Adolescent, Isoantibodies, Graft Rejection diagnosis, Kidney pathology, Transplant Recipients, Graft Survival, Kidney Transplantation, Nephrology

Abstract

Background: Antibody-mediated rejection (AMR) is a major cause of kidney allograft loss. There is a paucity of large-scale pediatric-specific data regarding AMR treatment outcomes., Methods: Data were obtained from 14 centers within the Pediatric Nephrology Research Consortium. Kidney transplant recipients aged 1-18 years at transplant with biopsy-proven AMR between 2009 and 2019 and at least 12 months of follow-up were included. The primary outcome was graft failure or an eGFR <20 mL/min/1.73 m 2 at 12 months following AMR treatment. AMR treatment choice, histopathology, and DSA class were also examined., Results: We reviewed 123 AMR episodes. Median age at diagnosis was 15 years at a median 22 months post-transplant. The primary outcome developed in 27.6%. eGFR <30 m/min/1.73 m 2 at AMR diagnosis was associated with a 5.6-fold higher risk of reaching the composite outcome. There were no significant differences in outcome by treatment modality. Histopathology scores and DSA class at time of AMR diagnosis were not significantly associated with the primary outcome., Conclusions: In this large cohort of pediatric kidney transplant recipients with AMR, nearly one-third of patients experienced graft failure or significant graft dysfunction within 12 months of diagnosis. Poor graft function at time of diagnosis was associated with higher odds of graft failure., (© 2024 Wiley Periodicals LLC.)

Published

2024

22. Multidisciplinary and multidimensional approaches to transplantation in children with rare genetic kidney diseases.

Author

George RP, Winterberg PD, and Garro R

Subjects

Child, Humans, Quality of Life, Kidney, Kidney Transplantation methods, Kidney Diseases genetics, Kidney Diseases surgery, Urinary Tract

Abstract

In this review, we describe the multidisciplinary, multidimensional care required to optimize outcomes for pediatric transplant recipients with rare genetic kidney diseases. Transplant success, recipient survival, and improvement in quality of life depend on collaboration between patients, families, and a team of specialists with medical, as well as nonmedical expertise. A multidisciplinary transplant team composed of experts from medicine, surgery, nursing, nutrition, social services, transplant coordination, psychology, and pharmacology, is now standard in most transplant centers and is critical to the success of a transplant. In addition to these professionals, other specialists, such as cardiologists, urologists, geneticists, metabolic disease specialists, occupational therapists, case management, child life, chaplain, and palliative care services, have a crucial role to play in the preparation, surgery, and follow-up care, especially when a pediatric patient has a rare genetic disorder leading to renal involvement, and the need for transplantation. In order to describe this multidisciplinary care, we divide the genetic renal diseases into five subgroups-metabolic and tubular disorders, glomerular diseases, congenital anomalies of the kidney and urinary tract, ciliopathies including cystic diseases, and miscellaneous renal conditions; and describe for each, the need for care beyond that provided by the standard transplant team members., (© 2023 Wiley Periodicals LLC.)

Published

2023

23. Validation of a prediction system for risk of kidney allograft failure in pediatric kidney transplant recipients: An international observational study.

Author

Hogan J, Divard G, Aubert O, Garro R, Boyer O, Donald Cooper LA, Farris AB, Fila M, Seifert M, Sellier-Leclerc AL, Smith J, Fichtner A, Tönshoff B, Twombley K, Warady B, Pearl M, Zahr RS, Lefaucheur C, Patzer R, and Loupy A

Subjects

Adult, Humans, Child, United States, Creatinine urine, Transplantation, Homologous, Kidney, Glomerular Filtration Rate, Transplant Recipients, Allografts, Kidney Transplantation adverse effects, Renal Insufficiency

Abstract

Predicting long-term kidney allograft failure is an unmet need for clinical care and clinical trial optimization in children. We aimed to validate a kidney allograft failure risk prediction system in a large international cohort of pediatric kidney transplant recipients. Patients from 20 centers in Europe and the United States, transplanted between 2004 and 2017, were included. Allograft assessment included estimated glomerular filtration rate, urine protein-to-creatinine ratio, circulating antihuman leukocyte antigen donor-specific antibody, and kidney allograft histology. Individual predictions of allograft failure were calculated using the integrative box (iBox) system. Prediction performances were assessed using discrimination and calibration. The allograft evaluations were performed in 706 kidney transplant recipients at a median time of 9.1 (interquartile range, 3.3-19.2) months posttransplant; mean estimated glomerular filtration rate was 68.7 ± 28.1 mL/min/1.73 m 2 , and median urine protein-to-creatinine ratio was 0.1 (0.0-0.4) g/g, and 134 (19.0%) patients had antihuman leukocyte antigen donor-specific antibodies. The iBox exhibited accurate calibration and discrimination for predicting the outcomes up to 10 years after evaluation, with a C-index of 0.81 (95% confidence interval, 0.75-0.87). This study confirms the generalizability of the iBox to predict long-term kidney allograft failure in children, with performances similar to those reported in adults. These results support the use of the iBox to improve patient monitoring and facilitate clinical trials in children., (Copyright © 2023. Published by Elsevier Inc.)

Published

2023

24. Immunohistochemical expression of cAMP in fluoroedenite‑induced malignant pleural mesothelioma: Preliminary results.

Author

Broggi G, Filetti V, Magro G, Morante B, Garro R, Ledda C, Rapisarda V, Lombardo C, Loreto C, and Caltabiano R

Subjects

Male, Female, Humans, Middle Aged, Aged, Aged, 80 and over, Mesothelioma, Malignant, Mesothelioma chemically induced, Mesothelioma metabolism, Lung Neoplasms pathology, Asbestos

Abstract

Despite advances in understanding of the biology of malignant pleural mesothelioma (MPM), the prognosis of this malignancy remains poor. Although asbestos still remains the main pathogenic agent of MPM, other asbestos‑like fibers such as fluoro‑edenite (FE) fibers, induce MPM. Notable incidence and mortality rates of MPM have been found in Biancavilla, Italy, where FE fibers have been extracted from building materials for >50 years. Cyclic adenosine monophosphate (cAMP) is a secondary messenger that plays a key role in several physiological and pathological mechanisms regulating protein kinase A (PKA) and the CREB pathway. Hyperactivation of the cAMP/PKA/CREB pathway is involved in many neoplastic processes, including tumor cell proliferation, invasion and metastatic spread. The present study investigated immunohistochemical expression of cAMP in patients with FE‑induced MPM, which included six males and four females with an age range of 50‑93 years. There was high immunoexpression of cAMP in 5 out of 10 tumors while the remaining 5 cases showed low immunoexpression. In addition, there was a correlation between cAMP overexpression and decreased survival times (mean overall survival times, 7.5 months in high expression group vs. 18 months in low expression group).

Published

2023

25. Persistent Increase in Serum Ferritin Levels despite Converting to Permanent Vascular Access in Pediatric Hemodialysis Patients: Pediatric Nephrology Research Consortium Study.

Author

Onder AM, Ansari MAY, Deng F, Grinsell MM, Patterson L, Jetton J, Fathallah-Shaykh S, Ranch D, Aviles D, Copelovitch L, Ellis E, Chadha V, Elmaghrabi A, Lin JJ, Butani L, Haddad M, Marsenic O, Brakeman P, Quigley R, Shin HS, Garro R, Raina R, and Langman CB

Abstract

Our objective was to examine serum ferritin trends after conversion to permanent vascular access (PVA) among children who started hemodialysis (HD) using tunneled cuffed catheters (TCC). Retrospective chart reviews were completed on 98 subjects from 20 pediatric HD centers. Serum ferritin levels were collected at the creation of PVA and for two years thereafter. There were 11 (11%) arteriovenous grafts (AVG) and 87 (89%) arteriovenous fistulae (AVF). Their mean TCC use was 10.4 ± 17.3 months. Serum ferritin at PVA creation was elevated at 562.64 ± 492.34 ng/mL, increased to 753.84 ± 561.54 ng/mL ( p = < 0.001) in the first year and remained at 759.60 ± 528.11 ng/mL in the second year ( p = 0.004). The serum ferritin levels did not show a statistically significant linear association with respective serum hematocrit values. In a multiple linear regression model, there were three predictors of serum ferritin during the first year of follow-up: steroid-resistant nephrotic syndrome as primary etiology ( p = 0.035), being from a center that enrolled >10 cases ( p = 0.049) and baseline serum ferritin level ( p = 0.017). Increasing serum ferritin after conversion to PVA is concerning. This increase is not associated with serum hematocrit trends. Future studies should investigate the correlation of serum transferrin saturation and ferritin levels in pediatric HD patients.

Published

2023

26. Incidence of cytomegalovirus DNAemia in pediatric kidney, liver, and heart transplant recipients: Efficacy and risk factors associated with failure of weight-based dosed valganciclovir prophylaxis.

Author

Liverman R, Serluco A, Nance G, George R, Rodriguez DS, Deshpande S, Mao C, Garro R, and Yildirim I

Subjects

Humans, Child, Child, Preschool, Valganciclovir therapeutic use, Cytomegalovirus genetics, Antiviral Agents, Incidence, Retrospective Studies, Risk Factors, Transplant Recipients, Kidney, Liver, Ganciclovir therapeutic use, Cytomegalovirus Infections etiology, Cytomegalovirus Infections prevention & control, Cytomegalovirus Infections drug therapy, Heart Transplantation adverse effects

Abstract

Background: Cytomegalovirus (CMV) is associated with morbidity and mortality in solid organ transplant recipients (SOTR). Valganciclovir (VGC) is extensively used for prophylaxis. Optimal dosing in children, risk factors for failure, and the impact of dose adjustments on CMV DNAemia is not well established., Methods: This retrospective cohort study of pediatric SOTR transplanted between 2010-2018 evaluated the epidemiology of CMV DNAemia and used Cox-regression to assess the risk factors for CMV DNAemia within one-year following SOTR., Results: In 393 pediatric SOTR (heart [96, 24.4%], kidney [180, 45.6%], liver [117, 29.8%]; median age 9.5 ± 0.3 years), overall CMV DNAemia incidence was 6.6/10 000 days (95%CI 5.1/10 000-7.9/10 000) and varied by organ groups: heart 8.2/10 000 days (95%CI 4.9/10 000-11.4/10 000), kidney 5.8/10 000 days (95%CI 3.9/10 000-7.8/10 000), liver 6.2/10 000 days (95%CI 3.7/10 000-8.7/10 000). CMV DNAemia was detected in 75 of 275 (27.2%) patients who received prophylaxis (40 cases occurred during prophylaxis and 35 occurred after completion of prophylaxis). The median VGC dose given according to institutional weight-based algorithm was approximately 1.5-fold lower than the manufacturer-recommended dose. This discordance was more prominent at younger age groups (3.2-fold lower in <2-year-old [100 mg versus 325 mg], 2.5-fold lower in <6-year-old [200 mg versus 447 mg]). Dose reduction due to adverse events was an independent risk factor for breakthrough CMV DNAemia (hazard ratio 2.2, 95%CI 1.2-3.8) among patients with similar age, CMV risk stratification, starting VGC dose, immunosuppressive therapy, and organ group., Conclusion: CMV events occurred while on VGC prophylaxis. Weight-based VGC may prevent supratherapeutic VGC exposure especially in younger children. Dose reduction of VGC prophylaxis for adverse event management places patients at an increased risk for CMV DNAemia suggesting other agents with fewer adverse effects should be considered and need to be studied in children., (© 2023 Wiley Periodicals LLC.)

Published

2023

27. Successful Use of Fosmanogepix for Treatment of Rare Highly Resistant Cutaneous Fusariosis in a Pediatric Patient With STAT3 Hyper-Immunoglobulin E Syndrome and End-Stage Kidney Disease.

Author

Goggin KP, Londeree J, Freeman AF, Garro R, and George RP

Abstract

We describe the successful use of the novel antifungal drug fosmanogepix to treat a chronic case of multidrug-resistant cutaneous Fusarium suttonianum infection in a pediatric patient with STAT3 hyper-IgE syndrome and end-stage kidney disease on peritoneal dialysis., Competing Interests: Potential conflicts of interest. All authors: No reported conflicts of interest., (© The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America.)

Published

2023

28. A randomized controlled trial of preemptive rituximab to prevent recurrent focal segmental glomerulosclerosis post-kidney transplant (PRI-VENT FSGS): protocol and study design.

Author

Rheault MN, Amaral S, Bock M, Chambers ET, Chavers B, Ters ME, Garro R, Gbadegesin R, Govil A, Harshman L, Amer H, Hooper DK, Israni AK, Riad S, Sageshima J, Shapiro R, Seifert M, Smith J, Sung R, Thomas CP, Wang Q, and Verghese PS

Abstract

Background: Focal segmental glomerulosclerosis (FSGS) is a common cause of end-stage kidney disease requiring kidney transplantation and can recur in the allograft in 30-80% of recipients resulting in reduced graft survival. Plasmapheresis has shown efficacy in treating some cases of recurrent FSGS but isolated plasmapheresis has not demonstrated efficacy in preventing recurrent FSGS. Rituximab has had anecdotal success in preventing recurrence in a single center study but has not been studied in combination with plasmapheresis for preventing FSGS recurrence., Methods: We are conducting a randomized, controlled, multicenter clinical trial of adult and pediatric kidney transplant recipients with primary FSGS to assess whether plasmapheresis in combination with rituximab prevents recurrent disease post-transplantation., Discussion: Rituximab combined with plasmapheresis is a promising, novel therapy to prevent recurrent FSGS, a disease with limited therapeutic options and no consensus guidelines for prevention or treatment., Clinical Trial Registration: https://clinicaltrials.gov/ct2/show/NCT03763643, identifier NCT03763643., Competing Interests: Author MR is a site PI for unrelated clinical trials funded by Chinook, Kaneka, Travere, Reata, Sanofi and a consultant for Visterra. Author PV is a site PI for unrelated clinical trials funded by Akebia, Allosure, Otsuka, Pharmacosmos and Viracor and a consultant for NS Pharma. The remaining 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 © 2023 Rheault, Amaral, Bock, Chambers, Chavers, Ters, Garro, Gbadegesin, Govil, Harshman, Amer, Hooper, Israni, Riad, Sageshima, Shapiro, Seifert, Smith, Sung, Thomas, Wang and Verghese.)

Published

2023

29. An automated histological classification system for precision diagnostics of kidney allografts.

Author

Yoo D, Goutaudier V, Divard G, Gueguen J, Astor BC, Aubert O, Raynaud M, Demir Z, Hogan J, Weng P, Smith J, Garro R, Warady BA, Zahr RS, Sablik M, Twombley K, Couzi L, Berney T, Boyer O, Duong-Van-Huyen JP, Giral M, Alsadi A, Gourraud PA, Morelon E, Le Quintrec M, Brouard S, Legendre C, Anglicheau D, Villard J, Zhong W, Kamar N, Bestard O, Djamali A, Budde K, Haas M, Lefaucheur C, Rabant M, and Loupy A

Subjects

Adult, Humans, Male, Female, Child, Prospective Studies, Transplantation, Homologous, Allografts, Graft Rejection diagnosis, Biopsy, Kidney pathology, Kidney Transplantation adverse effects

Abstract

For three decades, the international Banff classification has been the gold standard for kidney allograft rejection diagnosis, but this system has become complex over time with the integration of multimodal data and rules, leading to misclassifications that can have deleterious therapeutic consequences for patients. To improve diagnosis, we developed a decision-support system, based on an algorithm covering all classification rules and diagnostic scenarios, that automatically assigns kidney allograft diagnoses. We then tested its ability to reclassify rejection diagnoses for adult and pediatric kidney transplant recipients in three international multicentric cohorts and two large prospective clinical trials, including 4,409 biopsies from 3,054 patients (62.05% male and 37.95% female) followed in 20 transplant referral centers in Europe and North America. In the adult kidney transplant population, the Banff Automation System reclassified 83 out of 279 (29.75%) antibody-mediated rejection cases and 57 out of 105 (54.29%) T cell-mediated rejection cases, whereas 237 out of 3,239 (7.32%) biopsies diagnosed as non-rejection by pathologists were reclassified as rejection. In the pediatric population, the reclassification rates were 8 out of 26 (30.77%) for antibody-mediated rejection and 12 out of 39 (30.77%) for T cell-mediated rejection. Finally, we found that reclassification of the initial diagnoses by the Banff Automation System was associated with an improved risk stratification of long-term allograft outcomes. This study demonstrates the potential of an automated histological classification to improve transplant patient care by correcting diagnostic errors and standardizing allograft rejection diagnoses.ClinicalTrials.gov registration: NCT05306795 ., (© 2023. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2023

30. Donor specific antibody surveillance among pediatric kidney transplant programs: A report from the improving renal outcome collaborative.

Author

Steinbach EJ, Barletta GM, Patel HP, Hooper DK, Garro R, and Harshman LA

Subjects

Humans, Child, Isoantibodies, Graft Rejection, Risk Factors, Graft Survival, Tissue Donors, HLA Antigens, Retrospective Studies, Kidney Transplantation

Abstract

Background: Kidney transplantation (KT) is the preferred treatment for children with end-stage kidney disease. Recent advances in immunosuppression and advances in donor specific antibody (DSA) testing have resulted in prolonged allograft survival; however, standardized approaches for surveillance DSA monitoring and management of de novo (dn) DSA are widely variable among pediatric KT programs., Methods: Pediatric transplant nephrologists in the multi-center Improving Renal Outcomes Collaborative (IROC) participated in a voluntary, web-based survey between 2019 and 2020. Centers provided information pertaining to frequency and timing of routine DSA surveillance and theoretical management of dnDSA development in the setting of stable graft function., Results: 29/30 IROC centers responded to the survey. Among the participating centers, screening for DSA occurs, on average, every 3 months for the first 12 months post-transplant. Antibody mean fluorescent intensity and trend most frequently directed changes in patient management. Increased creatinine above baseline was reported by all centers as an indication for DSA assessment outside of routine surveillance testing. 24/29 centers would continue to monitor DSA and/or intensify immunosuppression after detection of antibodies in the setting of stable graft function. In addition to enhanced monitoring, 10/29 centers reported performing an allograft biopsy upon detection of dnDSA, even in the setting of stable graft function., Conclusions: This descriptive report is the largest reported survey of pediatric transplant nephrologist practice patterns on this topic and provides a reference for monitoring dnDSA in the pediatric kidney transplant population., (© 2023 The Authors. Pediatric Transplantation published by Wiley Periodicals LLC.)

Published

2023

31. COVID-19 in pediatric kidney transplantation: a follow-up report of the Improving Renal Outcomes Collaborative.

Author

Varnell C Jr, Harshman LA, Liu C, Smith L, Al-Akash S, Barletta GM, Brakeman P, Chaudhuri A, Fadakar P, Galea L, Garro R, Gluck C, Kershaw DB, Matossian D, Patel HP, Peterson C, Pruette C, Ranabothu S, Rodig N, Singer P, Sebestyen VanSickle J, Weng PL, Danziger-Isakov L, Seifert ME, and Hooper DK

Subjects

Humans, Child, COVID-19 Testing, Follow-Up Studies, Prospective Studies, Kidney Transplantation adverse effects, COVID-19

Abstract

Background: We report follow-up data from an ongoing prospective cohort study of COVID-19 in pediatric kidney transplantation through the Improving Renal Outcomes Collaborative (IROC)., Methods: Patient-level data from the IROC registry were combined with testing, indication, and outcomes data collected to describe the epidemiology of COVID testing, treatment, and clinical outcomes; determine the incidence of a positive COVID-19 test; describe rates of COVID-19 testing; and assess for clinical predictors of a positive COVID-19 test., Results: From September 2020 to February 2021, 21 centers that care for 2690 patients submitted data from 648 COVID-19 tests on 465 patients. Most patients required supportive care only and were treated as outpatients, 16% experienced inpatient care, and 5% experienced intensive care. Allograft complications were rare, with acute kidney injury most common (7%). There was 1 case of respiratory failure and 1 death attributed to COVID-19. Twelve centers that care for 1730 patients submitted complete testing data on 351 patients. The incidence of COVID-19 among patients at these centers was 4%, whereas the incidence among tested patients was 19%. Risk factors to predict a positive COVID-19 test included age > 12 years, symptoms consistent with COVID-19, and close contact with a confirmed case of COVID-19., Conclusions: Despite the increase in testing and positive tests over this study period, the incidence of allograft loss or death related to COVID-19 remained extremely low, with allograft loss or death each occurring in < 1% of COVID-19-positive patients and in less than < 0.1% of all transplant patients within the IROC cohort. A higher resolution version of the Graphical abstract is available as Supplementary information., (© 2022. The Author(s), under exclusive licence to International Pediatric Nephrology Association.)

Published

2023

32. Vaccine Attitudes and COVID-19 Vaccine Intention Among Parents of Children With Kidney Disease or Primary Hypertension.

Author

Wang CS, Doma R, Westbrook AL, Johnson J, Anderson EJ, Greenbaum LA, Rana SA, George RP, Garro R, Khanna-Farber A, Escoffery C, and Bednarczyk RA

Subjects

Child, Humans, COVID-19 Vaccines therapeutic use, Intention, Attitude, Essential Hypertension, Parents, Health Knowledge, Attitudes, Practice, Influenza Vaccines therapeutic use, Influenza, Human, COVID-19 epidemiology, COVID-19 prevention & control, Kidney Diseases, Hypertension epidemiology

Abstract

Rationale & Objective: Children with kidney disease and primary hypertension may be more vulnerable to COVID-19. We examined COVID-19 vaccine hesitancy among parents of children with chronic kidney disease or hypertension., Study Design: Sequential explanatory mixed-methods design; survey followed by in-depth interviews., Setting & Participants: Parents of children aged <18 years with kidney disease or primary hypertension within a large pediatric practice., Exposure: Parental attitudes toward general childhood and influenza vaccines assessed by the Vaccine Hesitancy Scale. Kidney disease classification, demographic and socioeconomic factors, experiences with COVID-19, COVID-19 mitigation activities and self-efficacy, and sources of vaccine information., Outcome: Willingness to vaccinate child against COVID-19., Analytical Approach: Analysis of variance (ANOVA) test to compare parental attitudes toward general childhood and influenza vaccination with attitudes toward COVID-19 vaccination. Multinomial logistic regression to assess predictors of willingness to vaccinate against COVID-19. Thematic analysis of interview data to characterize influences on parental attitudes., Results: Of the participants, 207 parents completed the survey (39% of approached): 75 (36%) were willing, 80 (39%) unsure, and 52 (25%) unwilling to vaccinate their child against COVID-19. Hesitancy toward general childhood and influenza vaccines was highest among the unwilling group (P < 0.001). More highly educated parents more likely to be willing to vaccinate their children, while Black race was associated with being more likely to be unwilling. Rushed COVID-19 vaccine development as well as fear of serious and unknown long-term side effects were themes that differed across the parental groups that were willing, unsure, or unwilling to vaccinate their children. Although doctors and health care teams are trusted sources of vaccine information, perceptions of benefit versus harm and experiences with doctors differed among these 3 groups. The need for additional information on COVID-19 vaccines was greatest among those unwilling or unsure about vaccinating., Limitations: Generalizability may be limited., Conclusions: Two-thirds of parents of children with kidney disease or hypertension were unsure or unwilling to vaccinate their child against COVID-19. Higher hesitancy toward routine childhood and influenza vaccination was associated with hesitancy toward COVID-19 vaccines. Enhanced communication of vaccine information relevant to kidney patients in an accessible manner should be examined as a means to reduce vaccine hesitancy., Plain-Language Summary: Children with kidney disease or hypertension may do worse with COVID-19. As there are now effective vaccines to protect children from COVID-19, we wanted to find out what parents think about COVID-19 vaccines and what influences their attitudes. We surveyed and then interviewed parents of children who had received a kidney transplant, were receiving maintenance dialysis, had chronic kidney disease, or had hypertension. We found that two-thirds of parents were hesitant to vaccinate their children. Their reasons varied, but the key issues included the need for information pertinent to their child and a consistent message from doctors and other health care providers. These findings may inform an effective vaccine campaign to protect children with kidney disease and hypertension., (Copyright © 2022 National Kidney Foundation, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2023

33. Temporal trends and current use of de novo belatacept in kidney transplant recipients in the United States.

Author

Karadkhele G, Duneton C, Garro R, Badell IR, Pearson TC, Larsen CP, and Hogan J

Subjects

Abatacept therapeutic use, Adult, Calcineurin Inhibitors therapeutic use, Graft Rejection drug therapy, Graft Rejection etiology, Graft Rejection prevention & control, Graft Survival, Humans, Immunosuppressive Agents therapeutic use, United States, Kidney Transplantation adverse effects, Transplant Recipients

Abstract

The adoption of de novo belatacept in kidney transplant (kTx) recipients was hampered by an increased risk of acute cellular rejection (ACR) with variation in adopted belatacept based immunosuppressive therapies across centers. We used data from the Scientific Registry of Transplant Recipients (SRTR) to evaluate the temporal trends in belatacept use and describe the associated induction and maintenance regimens in US adult kTx recipients transplanted between June 2011 and December 2018. The number of patients receiving de novo-belatacept based immunosuppressive therapy increased from .74% in 2011 to 3.11% in 2016. In 2016, 66/207 centers used de novo belatacept-based regimen with 3.03% using it in over 50% of their patients. The use of T-cell depleting agents increased with time. Since 2012, the rate of calcineurin inhibitor (CNI) use in combination with belatacept remained stable around 50% and ∼30% remained under belatacept/CNI combination at 1-year post-transplantation. The adoption of belatacept as de novo immunosuppressive regimen has been slow and its use remains low in the United States. Various regimens have been used to modulate the risk of ACR. Further studies evaluating the long-term outcomes of these regimens and assessing their safety especially with regard to the risk of infection are needed., (© 2021 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2022

34. Balloon cell melanoma: an uncommon entity representing a diagnostic pitfall in dermatopathology.

Author

Caltabiano R, Broggi G, Garro R, Terranova M, and Argenziano G

Subjects

Humans, Melanoma diagnosis, Skin Neoplasms diagnosis

Published

2021

35. Re-transplantation in pediatric patients with failure of primary transplant due to recurrent focal segmental glomerulosclerosis: A pediatric nephrology research consortium study.

Author

Maniar A, Hooper DK, Sethna CB, Singer P, Traum A, Benoit E, Kotzen E, Verghese P, Garro R, Kamel M, Ranch D, Shih W, Jain NG, and Al-Akash S

Subjects

Child, Child, Preschool, Female, Humans, Male, Plasmapheresis, Retrospective Studies, Surveys and Questionnaires, Glomerulosclerosis, Focal Segmental surgery, Graft Rejection surgery, Kidney Transplantation, Postoperative Complications surgery, Practice Patterns, Physicians' statistics & numerical data, Reoperation statistics & numerical data

Abstract

Introduction: Recurrent focal and segmental glomerulosclerosis (FSGS) in kidney transplant recipients is associated with lower graft survival and increased morbidity. There are limited data to guide the decision to re-transplant patients with transplant failure due to FSGS recurrence. We aimed to evaluate outcomes in patients re-transplanted after having initial graft failure due to recurrent FSGS and to study physician attitudes and practice patterns., Methods: Retrospective data from 10 centers were collected on 20 patients transplanted between January 1997 and September 2018. A survey was sent to nephrologist members of the Pediatric Nephrology Research Consortium., Results: Mean patient age (years) was 9.8 ± 4.8 at first transplant and 15.9 ± 4.9 at re-transplantation. Pre-transplant plasmapheresis was used in 1 (5.3%) primary transplant vs. 7 (38.9%) re-transplants (p = .03). Nephrotic syndrome recurred in 14 patients (70%) after re-transplantation and was severe in 21.1% vs. 64.7% after first transplant (p = .04). Graft survival was significantly higher in the second transplant (p .009) with 70% having functioning grafts at a median of 25.2 months. Thirty-one physicians from 21 centers completed the survey, 94% indicated they would re-transplant such patients, 44.4% preferred a minimum waiting period before re-transplantation, 36.4% preferred living donors, and 22.2% indicated having protocols for re-transplantation at their centers., Conclusions: Consideration for re-transplantation is high among pediatric nephrologists. Pre-transplant plasmapheresis was more frequent in re-transplanted patients. Nephrotic syndrome recurrence was less severe, with better graft survival. More data and a larger population are necessary to further evaluate outcome determinants and best practices in this special population., (© 2021 Wiley Periodicals LLC.)

Published

2021

36. Conversion to permanent vascular access is associated with improved markers of hemodialysis efficacy in children: Pediatric nephrology research consortium study.

Author

Onder AM, Flynn JT, Ansari MAY, Deng F, DeFreitas M, Katsoufis C, Grinsell MM, Patterson L, Jetton J, Fathallah-Shaykh S, Ranch D, Aviles D, Copelovitch L, Ellis E, Chadha V, Elmaghrabi A, Lin JJ, Butani L, Haddad M, Marsenic O, Brakeman P, Quigley R, Shin HS, Garro R, Raina R, Langman CB, and Wood E

Subjects

Child, Female, Humans, Male, Renal Dialysis, Retrospective Studies, Arteriovenous Shunt, Surgical adverse effects, Kidney Failure, Chronic diagnosis, Kidney Failure, Chronic therapy, Nephrology

Abstract

Background and Objectives: Arteriovenous fistulae (AVF) and grafts (AVG) are preferred permanent vascular access (PVA) for chronic hemodialysis (HD) patients. Our objective was to examine the change in markers of HD efficacy after successful establishment of a PVA among children who started HD with a tunneled cuffed catheter (TCC)., Materials and Methods: Retrospective chart reviews were completed on patients from 20 pediatric dialysis centers. All patients used TCC prior to AVF/AVG, and each patient acted as his/her own control. Data on markers of HD efficacy (single-pool Kt/V, urea reduction ratio (URR), serum albumin and hematocrit (Hct)) were collected at the creation of AVF/AVG and for 2 years thereafter. Statistical methods included hypothesis testing and statistical modeling after adjusting for relevant demographic variables., Results: First PVA was created in 98 individual children: 87 (89%) were AVF and 11 (11%) were AVG. The mean TCC vintage prior to AVF/AVG was 10.4 ± 17.3 months. At 1-year follow-up, Kt/V improved by 0.15 ± 0.06 (p = 0.02) and URR improved by 4.54 ± 1.17% (p < 0.0001). Furthermore, PVA was associated with improved serum albumin by 0.31 ± 0.07 g/dL (p < 0.0001) and Hct by 2.80 ± 0.65% (p < 0.0001) at 1 year. These HD efficacy markers remained statistically significant at 2 nd -year follow-up. These observations were further supported by the adjusted models. Conversion to AVF was associated with statistically significant improvement in all four markers of HD efficacy at 1-year follow-up. This trend was not demonstrated for subjects who were converted to AVG., Conclusion: Switching to PVA was associated with improved markers of HD efficacy, single-pool Kt/V, URR, serum albumin, and Hct. This improvement was mostly demonstrated at 1 year and maintained for the 2 nd year. The potential differential impact of the type of PVA on the trajectory of markers of HD efficacy should be further investigated.

Published

2021

37. Predictors for early readmission in patients hospitalized with new onset pediatric lupus nephritis.

Author

Ah Guerra A, Garro R, McCracken C, Rouster-Stevens K, and Prahalad S

Subjects

Adolescent, Albumins administration & dosage, Albumins adverse effects, Child, Female, Humans, Infusions, Intravenous, Lupus Erythematosus, Systemic diagnosis, Lupus Erythematosus, Systemic epidemiology, Lupus Nephritis drug therapy, Lupus Nephritis epidemiology, Male, Retrospective Studies, Risk Factors, Time Factors, Hospitalization statistics & numerical data, Lupus Nephritis diagnosis, Patient Readmission statistics & numerical data

Abstract

Objective: The objective is to determine the 30-day hospital readmission rate following a hospitalization due to pediatric lupus nephritis of recent onset and characterize the risk factors associated with these early readmissions., Methods: The study included 76 children hospitalized from 01/01/2008 to 4/30/2017 due to a new diagnosis of lupus nephritis. We calculated the 30-day hospital readmission rate and compared the characteristics of the patients that were readmitted to patients that were not readmitted using univariable and multivariable analysis., Results: The 30-day readmission rate was 17.1%. Factors that predicted hospital readmission in unavailable analysis were male gender (38.5 vs 14.3%, p = 0.04), not receiving pulse steroids (30.8 vs 3.2%, p = < .001), receiving diuretic treatment (69.2 vs 34.9%, p = .02), receiving albumin infusions (46.2 vs 12.7%, p = .004), stage 2 hypertension on day one of admission (76.9 vs 41.3%, p = .02), a higher white blood cell count on discharge (13.7 × 10 3 /mm 3 vs 8.8 × 10 3 /mm3 , p = .023), need for non-angiotensin converting enzyme (ACE) antihypertensive drugs (76.9 vs 46%, p = .042), and being discharged on nonsteroidal anti-inflammatory drugs (NSAIDs) (23.1 vs 4.8%, p = .025). Multivariable analysis demonstrated an increased risk of readmission for patients not treated with intravenous pulse methylprednisolone (IVMP) (OR = 17.5 (1.81-168.32) p = .013), and for those who required intravenous albumin assisted diuresis for hypervolemia (OR=6.25 (1.29-30.30) p = .022)., Conclusion: In all, 17% of children hospitalized due to new onset lupus nephritis were readmitted within 30 days of discharge. Absence of IVMP and receiving intravenous albumin assisted diuresis during initial hospitalization increase the risk of early readmission in new onset pediatric lupus nephritis.

Published

2021

38. COVID-19 in pediatric kidney transplantation: The Improving Renal Outcomes Collaborative.

Author

Varnell C Jr, Harshman LA, Smith L, Liu C, Chen S, Al-Akash S, Barletta GM, Belsha C, Brakeman P, Chaudhuri A, Fadakar P, Garro R, Gluck C, Goebel J, Kershaw D, Matossian D, Nailescu C, Patel HP, Pruette C, Ranabothu S, Rodig N, Smith J, Sebestyen VanSickle J, Weng P, Danziger-Isakov L, Hooper DK, and Seifert M

Subjects

Child, Humans, Incidence, Prospective Studies, SARS-CoV-2, COVID-19, Kidney Transplantation adverse effects

Abstract

There are limited data on the impact of COVID-19 in children with a kidney transplant (KT). We conducted a prospective cohort study through the Improving Renal Outcomes Collaborative (IROC) to collect clinical outcome data about COVID-19 in pediatric KT patients. Twenty-two IROC centers that care for 2732 patients submitted testing and outcomes data for 281 patients tested for SARS-CoV-2 by PCR. Testing indications included symptoms and/or potential exposures to COVID-19 (N = 134, 47.7%) and/or testing per hospital policy (N = 154, 54.8%). Overall, 24 (8.5%) patients tested positive, of which 15 (63%) were symptomatic. Of the COVID-19-positive patients, 16 were managed as outpatients, six received non-ICU inpatient care and two were admitted to the ICU. There were no episodes of respiratory failure, allograft loss, or death associated with COVID-19. To estimate incidence, subanalysis was performed for 13 centers that care for 1686 patients that submitted all negative and positive COVID-19 results. Of the 229 tested patients at these 13 centers, 10 (5 asymptomatic) patients tested positive, yielding an overall incidence of 0.6% and an incidence among tested patients of 4.4%. Pediatric KT patients in the United States had a low estimated incidence of COVID-19 disease and excellent short-term outcomes., (© 2021 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2021

39. Can Conventional and Diffusion-Weighted MR Enterography Biomarkers Differentiate Inflammatory from Fibrotic Strictures in Crohn's Disease?

Author

Foti PV, Travali M, Farina R, Palmucci S, Coronella M, Spatola C, Puzzo L, Garro R, Inserra G, Riguccio G, Zanoli L, and Basile A

Subjects

Adult, Biomarkers, Constriction, Pathologic diagnostic imaging, Fibrosis, Humans, Magnetic Resonance Imaging, Retrospective Studies, Crohn Disease complications, Crohn Disease diagnostic imaging

Abstract

Background and Objectives: To retrospectively assess the value of magnetic resonance enterography (MRE) parameters derived from conventional and diffusion weighted imaging (DWI) sequences to differentiate fibrotic strictures from inflammatory ones in adult patients with Crohn's disease (CD), using surgical specimens as the histopathological reference standard. Material and Methods : Twenty-three patients with CD who had undergone surgical resection of ileal strictures with full-thickness histopathologic analysis within 3 months from preoperative MRE were included. Two radiologists blinded to histopathology in consensus evaluated the following biomarkers on MRE images matched to resected pathological specimens: T1 ratio, T2 ratio, enhancement pattern, mural thickness, pre-stenotic luminal diameter, and apparent diffusion coefficient (ADC). A blinded pathologist graded stricture histological specimens with acute inflammation score (AIS) and fibrosis score (FS). MRE measurements were correlated with the reference standard. Results: Inflammation and fibrosis coexisted in 78.3% of patients. T2 ratio was reduced in patients with severe fibrosis ( p = 0.01). Pre-stenotic bowel dilatation positively correlated with FS ( p = 0.002). The ADC value negatively correlated with FS ( p < 0.001) and was different between FS grades ( p < 0.05). The area under the receiver operating characteristic curve for discriminating between none and mild/moderate-severe bowel wall fibrosis was 0.75 for pre-stenotic bowel dilatation (sensitivity 100%, specificity 44.4%) and 0.97 for ADC (sensitivity 80%, specificity 100%). Conclusions: Inflammation and fibrosis often coexist in CD bowel strictures needing surgery. The combination of parameters derived from conventional MR sequences (T2 ratio, pre-stenotic dilatation) and from DWI (ADC) may provide a contribution to detect and grade bowel fibrosis in adult CD patients.

Published

2021

40. Brincidofovir for the treatment of human adenovirus infection in pediatric solid organ transplant recipients: A case series.

Author

Londeree J, Winterberg PD, Garro R, George RP, Shin S, Liverman R, Serluco A, Romero R, and Yildirim I

Subjects

Adenovirus Infections, Human etiology, Adolescent, Antiviral Agents therapeutic use, Cytosine therapeutic use, Female, Follow-Up Studies, Humans, Infant, Male, Retrospective Studies, Transplantation, Homologous, Young Adult, Adenovirus Infections, Human drug therapy, Cytosine analogs & derivatives, Kidney Transplantation, Liver Transplantation, Organophosphonates therapeutic use, Postoperative Complications, Transplant Recipients

Abstract

HAdV viremia can cause significant morbidity among pediatric recipients of SOT with variability in incidence and severity of disease based on the type of allograft. Currently, there are no US FDA-approved treatments for HAdV infections, and historically, the mainstay of treatment has been decreasing immunosuppression, with antiviral therapies reserved for those with severe disease. We describe the treatment of four pediatric SOT recipients (two kidney, one combined kidney-liver, and one liver) presenting with HAdV disease at our institution using brincidofovir. Our case series highlights the variability in presentation and the potential for severe disease in pediatric SOT recipients as we review disease presentation, disease course, complications, and treatment with brincidofovir., (© 2020 Wiley Periodicals LLC.)

Published

2020

41. The Improving Renal Outcomes Collaborative: Blood Pressure Measurement in Transplant Recipients.

Author

Seifert ME, Dahale DS, Kamel M, Winterberg PD, Barletta GM, Belsha CW, Chaudhuri A, Flynn JT, Garro R, George RP, Goebel JW, Kershaw DB, Matossian D, Misurac J, Nailescu C, Nguyen CR, Pearl M, Pollack A, Pruette CS, Singer P, VanSickle JS, Verghese P, Warady BA, Warmin A, Weng PL, Wickman L, Wilson AC, and Hooper DK

Subjects

Humans, Hypertension physiopathology, Prospective Studies, Blood Pressure physiology, Blood Pressure Determination methods, Hypertension diagnosis, Kidney Transplantation, Quality Improvement, Transplant Recipients

Abstract

Background and Objectives: Hypertension is highly prevalent in pediatric kidney transplant recipients and contributes to cardiovascular death and graft loss. Improper blood pressure (BP) measurement limits the ability to control hypertension in this population. Here, we report multicenter efforts from the Improving Renal Outcomes Collaborative (IROC) to standardize and improve appropriate BP measurement in transplant patients., Methods: Seventeen centers participated in structured quality improvement activities facilitated by IROC, including formal training in quality improvement methods. The primary outcome measure was the proportion of transplant clinic visits with appropriate BP measurement according to published guidelines. Prospective data were analyzed over a 12-week pre-intervention period and a 20-week active intervention period for each center and then aggregated as of the program-specific start date. We used control charts to quantify improvements across IROC centers. We applied thematic analysis to identify patterns and common themes of successful interventions., Results: We analyzed data from 5392 clinic visits. At baseline, BP was measured and documented appropriately at 11% of visits. Center-specific interventions for improving BP measurement included educating clinic staff, assigning specific team member roles, and creating BP tracking tools and alerts. Appropriate BP measurement improved throughout the 20-week active intervention period to 78% of visits., Conclusions: We standardized appropriate BP measurement across 17 pediatric transplant centers using the infrastructure of the IROC learning health system and substantially improved the rate of appropriate measurement over 20 weeks. Accurate BP assessment will allow further interventions to reduce complications of hypertension in pediatric kidney transplant recipients., Competing Interests: POTENTIAL CONFLICT OF INTEREST: The authors have indicated they have no potential conflicts of interest to disclose., (Copyright © 2020 by the American Academy of Pediatrics.)

Published

2020

42. Predictors of time to first cannulation for arteriovenous fistula in pediatric hemodialysis patients: Midwest Pediatric Nephrology Consortium study.

Author

Onder AM, Flynn JT, Billings AA, Deng F, DeFreitas M, Katsoufis C, Grinsell MM, Patterson L, Jetton J, Fathallah-Shaykh S, Ranch D, Aviles D, Copelovitch L, Ellis E, Chadha V, Elmaghrabi A, Lin JJ, Butani L, Haddad M, Marsenic O, Brakeman P, Quigley R, Shin HS, Garro R, Liu H, Rahimikollu J, Raina R, Langman CB, and Wood E

Subjects

Adolescent, Child, Female, Humans, Male, Retrospective Studies, Arteriovenous Shunt, Surgical, Continuous Renal Replacement Therapy, Kidney Failure, Chronic therapy, Time-to-Treatment

Abstract

Background: Permanent vascular access (PVA) is preferred for long-term hemodialysis. Arteriovenous fistulae (AVF) have the best patency and the lowest complication rates compared to arteriovenous grafts (AVG) and tunneled cuffed catheters (TCC). However, AVF need time to mature. This study aimed to investigate predictors of time to first cannulation for AVF in pediatric hemodialysis patients., Methods: Data on first AVF and AVG of patients at 20 pediatric dialysis centers were collected retrospectively, including demographics, clinical information, dialysis markers, and surgical data. Statistical modeling was used to investigate predictors of outcome., Results: First PVA was created in 117 children: 103 (88%) AVF and 14 (12%) AVG. Mean age at AVF creation was 15.0 ± 3.3 years. AVF successfully matured in 89 children (86.4%), and mean time to first cannulation was 3.6 ± 2.5 months. In a multivariable regression model, study center, age, duration of non-permanent vascular access (NPVA), and Kt/V at AVF creation predicted time to first cannulation, with study center as the strongest predictor (p < 0.01). Time to first cannulation decreased with increasing age (p = 0.03) and with increasing Kt/V (p = 0.01), and increased with duration of NPVA (p = 0.03). Secondary failure occurred in 10 AVF (11.8%). Time to first cannulation did not predict secondary failure (p = 0.29), but longer time to first cannulation tended towards longer secondary patency (p = 0.06)., Conclusions: Study center is the strongest predictor of time to first cannulation for AVF and deserves further investigation. Time to first cannulation is significantly shorter in older children, with more efficient dialysis treatments, and increases with longer NPVA duration.

Published

2020

43. Renal allograft loss due to renal vascular thrombosis in the US pediatric renal transplantation.

Author

Wang CS, Greenbaum LA, Patzer RE, Garro R, Warshaw B, George RP, Winterberg PD, Patel K, and Hogan J

Subjects

Centers for Medicare and Medicaid Services, U.S. statistics & numerical data, Child, Child, Preschool, Cold Ischemia adverse effects, Cold Ischemia statistics & numerical data, Female, Follow-Up Studies, Graft Rejection etiology, Graft Survival, Humans, Incidence, Kidney Transplantation methods, Male, Registries statistics & numerical data, Risk Factors, Thrombosis etiology, Time Factors, Transplantation, Homologous adverse effects, Transplantation, Homologous methods, United States epidemiology, Young Adult, Graft Rejection epidemiology, Kidney blood supply, Kidney Failure, Chronic surgery, Kidney Transplantation adverse effects, Thrombosis epidemiology

Abstract

Background: Renal vascular thrombosis (RVT) is a major cause of early allograft loss in the first year following pediatric kidney transplantation. We examined recent trends in allograft loss due to RVT and identified associated risk factors., Methods: We identified 14,640 kidney-only transplants performed between 1995 and 2014 with follow-up until June 30, 2016, in 13,758 pediatric patients aged < 19 years from the US Renal Data System. We examined the 1-year incidence of allograft loss due to RVT by year of transplant, and plotted the trend over time. Cox proportional hazards models were used to investigate the relationship between year of transplant as well as recipient, donor, and transplant characteristics with allograft loss due to RVT., Results: The incidence of allograft loss due to RVT consistently declined among pediatric kidney transplant performed between 1995 and 2014. Among transplants performed between 1995 and 2004, 128/7542 (1.7%) allografts were lost due to RVT compared to 53/7098 (0.8%) among transplants performed between 2005 and 2014; average 1-year cumulative incidence was 1.5% (95% CI, 1.3-1.9%) and 0.6% (95% CI, 0.5-0.8%), respectively. Increased risk for allograft loss due to RVT was associated with en bloc kidney transplantation (HR, 3.42; 95% CI 1.38-8.43) and cold ischemia time ≥ 12 h (HR, 1.78; 95% CI, 1.15-2.76). Interestingly, these risk factors were more prevalent in the latter decade., Conclusions: The incidence of allograft loss due to RVT significantly and continuously declined among pediatric kidney transplants performed between 1995 and 2014. The causes for this improvement are unclear in the present analysis.

Published

2019

44. Correction to: Predictors of patency for arteriovenous fistulae and grafts in pediatric hemodialysis patients.

Author

Onder AM, Flynn JT, Billings AA, Deng F, DeFreitas M, Katsoufis C, Grinsell MM, Patterson LT, Jetton J, Fathallah-Shaykh S, Ranch D, Aviles D, Copelovitch L, Ellis E, Chadha V, Elmaghrabi A, Lin JJ, Butani L, Haddad M, Couloures OM, Brakeman P, Quigley R, Shin HS, Garro R, Liu H, Rahimikollu J, Raina R, Langman CB, and Wood EG

Abstract

The original version of this article unfortunately contained a mistake. The name of Vimal Chadha was presented incorrectly. The corrected author list is given above.

Published

2019

45. Acute cellular rejection treatment outcomes stratified by Banff grade in pediatric kidney transplant.

Author

Chen J, Liverman R, Garro R, Jernigan S, Travers C, and Winterberg PD

Subjects

Acute Disease, Administration, Oral, Adolescent, Child, Child, Preschool, Drug Administration Schedule, Female, Follow-Up Studies, Graft Rejection diagnosis, Humans, Infant, Infant, Newborn, Injections, Intravenous, Male, Retrospective Studies, Severity of Illness Index, Treatment Outcome, Young Adult, Anti-Inflammatory Agents therapeutic use, Antilymphocyte Serum therapeutic use, Graft Rejection drug therapy, Immunosuppressive Agents therapeutic use, Kidney Transplantation, Methylprednisolone therapeutic use, Prednisone therapeutic use

Abstract

Introduction: There are limited data to guide optimal treatment strategies for acute cellular rejection (ACR) based on Banff grade for pediatric kidney transplant recipients. This report reviews a large pediatric transplant center's experience with ACR., Materials and Methods: A retrospective analysis of pediatric kidney transplant recipients at our center from 2007 to 2014 was performed. Primary outcomes were incidence of graft failure and graft function one year following ACR based on Banff grade and treatment received., Results: A total of 204 patients were reviewed, of which 65 received rejection treatment with either an oral steroid cycle (n = 16), intravenous steroid pulse (n = 28), or anti-thymocyte globulin (rATG, n = 21). Overall, patients received rATG for treatment of more severe rejection associated with impaired graft function and as a group experienced statistically significant improvements in eGFR over the year following treatment, though most did not regain baseline graft function., Discussion: Our data suggest that rATG is partially effective in treating ACR, but our study was underpowered to determine the effect of different treatments based on Banff grade. Since there is limited literature to guide clinical treatment of ACR in children, large transplant centers should collaborate to evaluate outcomes and establish evidence-based practice., (© 2018 Wiley Periodicals, Inc.)

Published

2019

46. Predictors of patency for arteriovenous fistulae and grafts in pediatric hemodialysis patients.

Author

Onder AM, Flynn JT, Billings AA, Deng F, DeFreitas M, Katsoufis C, Grinsell MM, Patterson LT, Jetton J, Fathallah-Shaykh S, Ranch D, Aviles D, Copelovitch L, Ellis E, Chanda V, Elmaghrabi A, Lin JJ, Butani L, Haddad M, Couloures OM, Brakeman P, Quigley R, Stella Shin H, Garro R, Liu H, Rahimikollu J, Raina R, Langman CB, and Wood EG

Subjects

Adolescent, Canada, Child, Female, Humans, Male, Renal Dialysis adverse effects, Retrospective Studies, Risk Factors, Time Factors, Treatment Failure, United States, Arteriovenous Shunt, Surgical adverse effects, Kidney Failure, Chronic therapy, Renal Dialysis methods, Vascular Grafting adverse effects, Vascular Patency

Abstract

Background: Hemodialysis (HD) guidelines recommend permanent vascular access (PVA) in children unlikely to receive kidney transplant within 1 year of starting HD. We aimed to determine predictors of primary and secondary patency of PVA in pediatric HD patients., Methods: Retrospective chart reviews were performed for first PVAs in 20 participating centers. Variables collected included patient demographics, complications, interventions, and final outcome., Results: There were 103 arterio-venous fistulae (AVF) and 14 AV grafts (AVG). AVF demonstrated superior primary (p = 0.0391) and secondary patency (p = 0.0227) compared to AVG. Primary failure occurred in 16 PVA (13.6%) and secondary failure in 14 PVA (12.2%). AVF were more likely to have primary failure (odds ratio (OR) = 2.10) and AVG had more secondary failure (OR = 3.33). No demographic, clinical, or laboratory variable predicted primary failure of PVA. Anatomical location of PVA was predictive of secondary failure, with radial having the lowest risk compared to brachial (OR = 12.425) or femoral PVA (OR = 118.618). Intervention-free survival was predictive of secondary patency for all PVA (p = 0.0252) and directly correlated with overall survival of AVF (p = 0.0197) but not AVG. Study center demonstrated statistically significant effect only on intervention-free AVF survival (p = 0.0082), but not number of complications or interventions, or outcomes., Conclusions: In this multi-center pediatric HD cohort, AVF demonstrated primary and secondary patency advantages over AVG. Radial PVA was least likely to develop secondary failure. Intervention-free survival was the only predictor of secondary patency for AVF and directly correlated with overall access survival. The study center effect on intervention-free survival of AVF deserves further investigation.

Published

2019

47. Long-Term Outcomes of Kidney Transplantation in Children.

Author

Winterberg PD and Garro R

Subjects

Adolescent, Child, Graft Rejection, Humans, Immunosuppressive Agents therapeutic use, Young Adult, Kidney Failure, Chronic surgery, Kidney Transplantation, Quality of Life

Abstract

Kidney transplantation is the preferred treatment for end-stage renal disease (ESRD) in children and confers improved survival, skeletal growth, heath-related quality of life, and neuropsychological development compared with dialysis. Kidney transplantation in children with ESRD results in 10-year patient survival exceeding 90%. Therefore, the long-term management of these patients is focused on maintaining quality of life and minimizing long-term side effects of immunosuppression. Optimal management of pediatric kidney transplant recipients includes preventing rejection and infection, identifying and reducing the cardiovascular and metabolic effects of long-term immunosuppressive therapy, supporting normal growth and development, and managing a smooth transition into adulthood., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2019

48. Multimethod Assessment of Medication Nonadherence and Barriers in Adolescents and Young Adults With Solid Organ Transplants.

Author

Eaton CK, Gutierrez-Colina AM, Quast LF, Liverman R, Lee JL, Mee LL, Reed-Knight B, Cushman G, Chiang G, Romero R, Mao C, Garro R, and Blount RL

Subjects

Adolescent, Adult, Caregivers psychology, Female, Humans, Male, Southeastern United States, Young Adult, Health Services Accessibility statistics & numerical data, Medication Adherence psychology, Medication Adherence statistics & numerical data, Transplant Recipients psychology, Transplant Recipients statistics & numerical data

Abstract

Objective: To (a) examine levels of medication nonadherence in adolescent and young adult (AYA) solid organ transplant recipients based on AYA- and caregiver proxy-reported nonadherence to different medication types and the medication-level variability index (MLVI) for tacrolimus, and (b) examine associations of adherence barriers and AYA and caregiver emotional distress symptoms with reported nonadherence and the MLVI., Method: The sample included 47 AYAs (M age = 16.67 years, SD = 1.74; transplant types: 25% kidney, 47% liver, 28% heart) and their caregivers (94 total participants). AYAs and caregivers reported on AYAs' adherence barriers and their own emotional functioning. Nonadherence was measured with AYA self- and caregiver proxy-report and the MLVI for tacrolimus., Results: The majority of AYAs and caregivers denied nonadherence, with lower rates of nonadherence reported for antirejection medications. In contrast, 40% of AYAs' MLVI values indicated nonadherence to tacrolimus. AYAs and caregivers who verbally acknowledged nonadherence had more AYA barriers and greater caregiver emotional distress symptoms compared with those who denied nonadherence. AYAs with MLVIs indicating nonadherence had more barriers than AYAs with MLVIs indicating adherence., Conclusions: Multimethod nonadherence evaluations for AYA transplant recipients should assess objective nonadherence using the MLVI, particularly in light of low reported nonadherence rates for antirejection medications. Assessments should include adherence barriers measures, given associations with the MLVI, and potentially prioritize assessing barriers over gauging nonadherence via self- or proxy-reports. Caregiver emotional distress symptoms may also be considered to provide insight into family or environmental barriers to adherence.

Published

2018

49. Ofatumumab for the treatment of childhood nephrotic syndrome.

Author

Wang CS, Liverman RS, Garro R, George RP, Glumova A, Karp A, Jernigan S, and Warshaw B

Subjects

Adolescent, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal, Humanized, Drug Hypersensitivity, Glomerulosclerosis, Focal Segmental drug therapy, Glomerulosclerosis, Focal Segmental etiology, Humans, Kidney pathology, Kidney Transplantation adverse effects, Male, Postoperative Complications drug therapy, Remission Induction, Treatment Outcome, Antibodies, Monoclonal therapeutic use, Nephrotic Syndrome drug therapy

Abstract

Background: Ofatumumab is a humanized anti-CD20 monoclonal antibody that has recently garnered interest as a potential therapeutic agent for nephrotic syndrome. We report our center's experience in administering ofatumumab to five pediatric patients with idiopathic nephrotic syndrome., Methods: Between March 2015 and November 2016, five patients were treated with ofatumumab. One patient had post-transplant recurrent focal segmental glomerulosclerosis (FSGS) which had been resistant to plasmapheresis and numerous immunosuppressive agents. Four patients had nephrotic syndrome in their native kidneys, one with initial steroid-resistant disease and the others with subsequent development of steroid resistance. Two of the patients were treated with a desensitization protocol after experiencing hypersensitivity reactions to ofatumumab., Results: One patient did not complete ofatumumab treatment due to infusion reactions. Of the four remaining patients, three achieved complete remission after treatment, and one achieved partial remission. One of the patients achieving complete remission represents the first reported case of successful treatment of post-transplant recurrent FSGS using ofatumumab. Two patients who received ofatumumab with our desensitization protocol were able to complete their treatments after initially experiencing hypersensitivity reactions., Conclusions: Ofatumumab may be an effective treatment for refractory childhood nephrotic syndrome and post-transplant recurrent FSGS. A desensitization protocol may be helpful to address hypersensitivity reactions.

Published

2017

50. CRIT-LINE: a noninvasive tool to monitor hemoglobin levels in pediatric hemodialysis patients.

Author

Garro R, Sutherland S, Bayes L, Alexander S, and Wong C

Subjects

Adolescent, Age Factors, Anemia blood, Anemia drug therapy, Anemia etiology, Biomarkers blood, Child, Child, Preschool, Equipment Design, Female, Hematinics therapeutic use, Hematocrit, Humans, Male, Predictive Value of Tests, Renal Insufficiency, Chronic blood, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic diagnosis, Reproducibility of Results, Time Factors, Treatment Outcome, Young Adult, Anemia diagnosis, Hemoglobins metabolism, Monitoring, Physiologic instrumentation, Renal Dialysis adverse effects, Renal Insufficiency, Chronic therapy

Abstract

Background: The national average for achieving the KDOQI-recommended hemoglobin (Hgb) target level of 11-12 g/dL is low with the current anemia management protocol of measuring Hgb levels every 2-4 weeks to guide intervention. The objective of this study was to correlate initial Hgb readings from the CRIT-LINE monitor with actual serum Hgb levels in pediatric patients on hemodialysis (HD)., Methods: Data were collected from pediatric HD patients who had Hgb tests ordered for routine and/or clinical reasons. Hgb concentrations were read with the CRIT-LINE after 0.5 or 1 L of blood had been processed by HD in patients with a body weight of ≤20 or >20 kg, respectively. Ultrafiltration was kept at a minimum until the CRIT-LINE Hgb was read., Results: In total, 217 Hgb readings from 23 HD patients were analyzed. Results showed a statistically significant correlation between CRIT-LINE readings and laboratory Hgb measurements (r = 0.94, p < 0.0001) using Pearson correlation coefficients for well-distributed data. The mean Hgb levels measured by CRIT-LINE and the laboratory were 11.12 ± 1.63 and 11.31 ± 1.69 g/dL, respectively., Conclusions: The CRIT-LINE monitor is an accurate instrument for monitoring Hgb levels in HD patients. Further studies will be needed to evaluate whether using CRIT-LINE Hgb levels to guide anemia management will improve the percentage of children with Hgb levels within target.

Published

2015