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1. Core Outcome Measures for Perioperative and Anaesthetic Care (COMPAC): a modified Delphi process to develop a core outcome set for trials in perioperative care and anaesthesia

Author

Bartoszko, J., Beattie, W.S., Bellomo, R., Buggy, D., Cabrini, L., Canet, J., Cook, T., Cooper, D.J., Corcoran, T., Devereaux, P.J., Eckenhoff, R., Evered, L., Gan, T.J., Gin, T., Grocott, H., Haller, G., Howell, S., Jayarajah, M., Kalkman, C., Karkouti, K., Kavanagh, B., Klein, A., Landoni, G., Leslie, K., McIlroy, D.R., Mazer, D., Moller, A., Mythen, M., Neuman, M., Pearse, R., Peyton, P., Prowle, J., Richards, T., Scott, D.A., Sessler, D., Shaw, A., Short, T., Shulman, M., Silbert, B., Singer, M., Sneyd, J.R., Story, D., van Dijk, D., van Klei, W., Boney, Oliver, Moonesinghe, S. Ramani, Myles, Paul S., and Grocott, Michael P.W.

Published
2022
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2. Systematic review and consensus definitions for the Standardised Endpoints in Perioperative Medicine initiative: clinical indicators

Author

Myles, P., Grocott, M., Biccard, B., Blazeby, J., Boney, O., Chan, M., Diouf, E., Fleisher, L., Kalkman, C., Kurz, A., Moonesinghe, R., Wijeysundera, D., Gan, T.J., Peyton, P., Sessler, D., Tramèr, M., Cyna, A., De Oliveira, G.S., Jr., Wu, C., Jensen, M., Kehlet, H., Botti, M., Haller, G., Cook, T., Neuman, M., Story, D., Gruen, R., Bampoe, S., Evered, L., Scott, D., Silbert, B., van Dijk, D., Grocott, H., Eckenhoff, R., Rasmussen, L., Eriksson, L., Beattie, S., Landoni, G., Leslie, K., Howell, S., Nagele, P., Richards, T., Lamy, A., Lalu, M., Pearse, R., Mythen, M., Canet, J., Moller, A., Gin, T., Schultz, M., Pelosi, P., Gabreu, M., Futier, E., Creagh-Brown, B., Abbott, T., Klein, A., Corcoran, T., Jamie Cooper, D., Dieleman, S., McIlroy, D., Bellomo, R., Shaw, A., Prowle, J., Karkouti, K., Billings, J., Mazer, D., Jayarajah, M., Murphy, M., Bartoszko, J., Sneyd, R., Morris, S., George, R., Shulman, M., Lane-Fall, M., Nilsson, U., Stevenson, N., Cooper, J.D.J., van Klei, W., Cabrini, L., Miller, T., Pace, N., Jackson, S., Buggy, D., Short, T., Riedel, B., Gottumukkala, V., Alkhaffaf, B., Johnson, M., Haller, Guy, Bampoe, Sohail, Cook, Tim, Fleisher, Lee A., Grocott, Michael P.W., Neuman, Mark, Story, David, and Myles, Paul S.

Published
2019
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3. Systematic review and consensus definitions for standardised endpoints in perioperative medicine: postoperative cancer outcomes

Author

Gan, T.J., Peyton, P., Tramèr, M., Cyna, A., De Oliveira, G.S., Jr., Wu, C., Jensen, M., Kehlet, H., Botti, M., Boney, O., Haller, G., Grocott, M., Cook, T., Fleisher, L., Neuman, M., Story, D., Gruen, R., Bampoe, S., Evered, Lis, Scott, D., Silbert, B., van Dijk, D., Kalkman, C., Chan, M., Grocott, H., Eckenhoff, R., Rasmussen, L., Eriksson, L., Beattie, S., Wijeysundera, D., Landoni, G., Biccard, B., Howell, S., Nagele, P., Richards, T., Lamy, A., Lalu, M., Pearse, R., Mythen, M., Canet, J., Moller, A., Gin, T., Schultz, M., Pelosi, P., Gabreu, M., Futier, E., Creagh-Brown, B., Abbott, T., Klein, A., Corcoran, T., Jamie Cooper, D., Dieleman, S., Diouf, E., McIlroy, D., Bellomo, R., Shaw, A., Prowle, J., Karkouti, K., Billings, J., Mazer, D., Jayarajah, M., Murphy, M., Bartoszko, J., Sneyd, R., Morris, S., George, R., Moonesinghe, R., Shulman, M., Lane-Fall, M., Nilsson, U., Stevenson, N., van Klei, W., Cabrini, L., Miller, T., Jackson, S., Alkhaffaf, B., Buggy, D.J., Freeman, J., Johnson, M.Z., Leslie, K., Riedel, B., Sessler, D.I., Kurz, A., Gottumukkala, V., Short, T., Pace, N., and Myles, P.S.

Published
2018
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4. A systematic review and consensus definitions for standardised end-points in perioperative medicine: pulmonary complications

Author

Myles, P., Gan, T.J., Kurz, A., Peyton, P., Sessler, D., Tramèr, M., Cyna, A., De Oliveira, G.S., Jr., Wu, C., Jensen, M., Kehlet, H., Botti, M., Boney, O., Haller, G., Grocott, M., Cook, T., Fleisher, L., Neuman, M., Story, D., Gruen, R., Bampoe, S., Evered, Lis, Scott, D., Silbert, B., van Dijk, D., Kalkman, C., Chan, M., Grocott, H., Eckenhoff, R., Rasmussen, L., Eriksson, L., Beattie, S., Wijeysundera, D., Landoni, G., Leslie, K., Biccard, B., Howell, S., Nagele, P., Richards, T., Lamy, A., Gabreu, M., Klein, A., Corcoran, T., Jamie Cooper, D., Dieleman, S., Diouf, E., McIlroy, D., Bellomo, R., Shaw, A., Prowle, J., Karkouti, K., Billings, J., Mazer, D., Jayarajah, M., Murphy, M., Bartoszko, J., Sneyd, R., Morris, S., George, R., Moonesinghe, R., Shulman, M., Lane-Fall, M., Nilsson, U., Stevenson, N., van Klei, W., Cabrini, L., Miller, T., Pace, N., Jackson, S., Buggy, D., Short, T., Riedel, B., Gottumukkala, V., Alkhaffaf, B., Johnson, M., Abbott, T.E.F., Fowler, A.J., Pelosi, P., Gama de Abreu, M., Møller, A.M., Canet, J., Creagh-Brown, B., Mythen, M., Gin, T., Lalu, M.M., Futier, E., Grocott, M.P., Schultz, M.J., and Pearse, R.M.

Published
2018
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6. Core Outcome Measures for Perioperative and Anaesthetic Care (COMPAC): a modified Delphi process to develop a core outcome set for trials in perioperative care and anaesthesia

Author

Boney, Oliver, primary, Moonesinghe, S. Ramani, additional, Myles, Paul S., additional, Grocott, Michael P.W., additional, Bartoszko, J., additional, Beattie, W.S., additional, Bellomo, R., additional, Buggy, D., additional, Cabrini, L., additional, Canet, J., additional, Cook, T., additional, Cooper, D.J., additional, Corcoran, T., additional, Devereaux, P.J., additional, Eckenhoff, R., additional, Evered, L., additional, Gan, T.J., additional, Gin, T., additional, Grocott, H., additional, Haller, G., additional, Howell, S., additional, Jayarajah, M., additional, Kalkman, C., additional, Karkouti, K., additional, Kavanagh, B., additional, Klein, A., additional, Landoni, G., additional, Leslie, K., additional, McIlroy, D.R., additional, Mazer, D., additional, Moller, A., additional, Mythen, M., additional, Neuman, M., additional, Pearse, R., additional, Peyton, P., additional, Prowle, J., additional, Richards, T., additional, Scott, D.A., additional, Sessler, D., additional, Shaw, A., additional, Short, T., additional, Shulman, M., additional, Silbert, B., additional, Singer, M., additional, Sneyd, J.R., additional, Story, D., additional, van Dijk, D., additional, and van Klei, W., additional

Published
2022
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7. Standardizing end points in perioperative trials: towards a core and extended outcome set

Author

Myles, P. S., Grocott, M. P. W., Boney, O., Moonesinghe, S. R., Myles, Paul, Grocott, Michael, Biccard, Bruce, Boney, Oliver, Chan, Matthew, Fleisher, Lee, Kalkman, Cor, Kurz, Andrea, Moonesinghe, Ramani, Wijeysundera, Duminda, Bartoszko, J., Beattie, W. S., Bellomo, R., Buggy, D., Cabrini, L., Canet, J., Cook, T., Cooper, D. J., Corcoran, T., Devereaux, P. J., Eckenhoff, R., Evered, L., Gan, T. J., Gin, T., Grocott, H., Haller, G., Howell, S., Jayarajah, M., Kalkman, C., Karkouti, K., Kavanagh, B., Klein, A., Landoni, G., Leslie, K., McIlroy, D. R., Mazer, D., Moller, A., Mythen, M., Neuman, M., Neuman, M., Pearse, R., Peyton, P., Prowle, J., Richards, T., Scott, D. A., Sessler, D., Shaw, A., Short, T., Shulman, M., Silbert, B., Singer, M., Sneyd, J. R., Story, D., van Dijk, D., and van Klei, W.

Published
2016
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8. Systematic review and consensus definitions for the Standardized Endpoints in Perioperative Medicine (StEP) initiative: cardiovascular outcomes

Author

Beattie, WS, Lalu, M, Bocock, M, Feng, S, Wijeysundera, DN, Nagele, P, Fleisher, LA, Kurz, A, Biccard, B, Leslie, K, Howell, S, Landoni, G, Grocott, H, Lamy, A, Richards, T, Myles, P, Cooper, DJ, Gan, TJ, Peyton, P, Sessler, D, Tramèr, M, Cyna, A, De Oliveira, GS, Wu, C, Jensen, M, Kehlet, H, Botti, Mari, Boney, O, Haller, G, Grocott, M, Cook, T, Fleisher, L, Neuman, M, Story, D, Gruen, R, Bampoe, S, Evered, L, Scott, D, Silbert, B, van Dijk, D, Kalkman, C, Chan, M, Eckenhoff, R, Rasmussen, L, Eriksson, L, Beattie, S, Wijeysundera, D, Bartlett, RJ, McMonnies, R, Gerstl, J, Jay, M, Kishlyansky, D, Machina, M, Bobcock, M, Pearse, R, Mythen, M, Canet, J, Moller, A, Gin, T, Schultz, M, Pelosi, P, Gabreu, M, Futier, E, Creagh-Brown, B, Abbott, T, Klein, A, Corcoran, T, Dieleman, S, Diouf, E, McIlroy, D, Bellomo, R, Shaw, A, Prowle, J, Karkouti, K, Billings, J, Mazer, D, Jayarajah, M, Murphy, M, Bartoszko, J, Sneyd, R, Morris, S, George, R, Moonesinghe, R, Shulman, M, Lane-Fall, M, Nilsson, U, Stevenson, N, Cooper, J, van Klei, W, Cabrini, L, Miller, T, Pace, N, Jackson, S, Buggy, D, Short, T, Riedel, B, Gottumukkala, V, Alkhaffaf, B, Beattie, WS, Lalu, M, Bocock, M, Feng, S, Wijeysundera, DN, Nagele, P, Fleisher, LA, Kurz, A, Biccard, B, Leslie, K, Howell, S, Landoni, G, Grocott, H, Lamy, A, Richards, T, Myles, P, Cooper, DJ, Gan, TJ, Peyton, P, Sessler, D, Tramèr, M, Cyna, A, De Oliveira, GS, Wu, C, Jensen, M, Kehlet, H, Botti, Mari, Boney, O, Haller, G, Grocott, M, Cook, T, Fleisher, L, Neuman, M, Story, D, Gruen, R, Bampoe, S, Evered, L, Scott, D, Silbert, B, van Dijk, D, Kalkman, C, Chan, M, Eckenhoff, R, Rasmussen, L, Eriksson, L, Beattie, S, Wijeysundera, D, Bartlett, RJ, McMonnies, R, Gerstl, J, Jay, M, Kishlyansky, D, Machina, M, Bobcock, M, Pearse, R, Mythen, M, Canet, J, Moller, A, Gin, T, Schultz, M, Pelosi, P, Gabreu, M, Futier, E, Creagh-Brown, B, Abbott, T, Klein, A, Corcoran, T, Dieleman, S, Diouf, E, McIlroy, D, Bellomo, R, Shaw, A, Prowle, J, Karkouti, K, Billings, J, Mazer, D, Jayarajah, M, Murphy, M, Bartoszko, J, Sneyd, R, Morris, S, George, R, Moonesinghe, R, Shulman, M, Lane-Fall, M, Nilsson, U, Stevenson, N, Cooper, J, van Klei, W, Cabrini, L, Miller, T, Pace, N, Jackson, S, Buggy, D, Short, T, Riedel, B, Gottumukkala, V, and Alkhaffaf, B

Published
2021

13. Systematic review and consensus definitions for the Standardised Endpoints in Perioperative Medicine initiative: clinical indicators

Author

Haller, Guy, Bampoe, Sohail, Cook, Tim, Fleisher, Lee A, Grocott, Michael PW, Neuman, Mark, Story, Davd, Myles, Paul S, Myles, P, Grocott, M, Biccard, B, Blazeby, J, Boney, O, Chan, M, Diouf, E, Fleisher, L, Kalkman, C, Kurz, A, Moonesinghe, R, Wijeysundera, D, Gan, TJ, Peyton, P, Sessler, D, Tramèr, M, Cyna, A, De Oliveira, GS, Wu, C, Jensen, M, Kehlet, H, Botti, Mari, Cook, T, Neuman, M, Story, D, Gruen, R, Evered, L, Scott, D, Silbert, B, van Dijk, D, Grocott, H, Eckenhoff, R, Rasmussen, L, Eriksson, L, Beattie, S, Landoni, G, Leslie, K, Howell, S, Nagele, P, Richards, T, Lamy, A, Lalu, M, Pearse, R, Mythen, M, Canet, J, Moller, A, Gin, T, Schultz, M, Pelosi, P, Gabreu, M, Futier, E, Creagh-Brown, B, Abbott, T, Klein, A, Corcoran, T, Jamie Cooper, D, Dieleman, S, McIlroy, D, Bellomo, R, Shaw, A, Prowle, J, Karkouti, K, Billings, J, Mazer, D, Jayarajah, M, Murphy, M, Bartoszko, J, Sneyd, R, Morris, S, George, R, Shulman, M, Lane-Fall, M, Nilsson, U, Stevenson, N, Cooper, JDJ, van Klei, W, Cabrini, L, Miller, T, Pace, N, Jackson, S, Buggy, D, Short, T, Riedel, B, Gottumukkala, V, Alkhaffaf, B, Johnson, M, Haller, Guy, Bampoe, Sohail, Cook, Tim, Fleisher, Lee A, Grocott, Michael PW, Neuman, Mark, Story, Davd, Myles, Paul S, Myles, P, Grocott, M, Biccard, B, Blazeby, J, Boney, O, Chan, M, Diouf, E, Fleisher, L, Kalkman, C, Kurz, A, Moonesinghe, R, Wijeysundera, D, Gan, TJ, Peyton, P, Sessler, D, Tramèr, M, Cyna, A, De Oliveira, GS, Wu, C, Jensen, M, Kehlet, H, Botti, Mari, Cook, T, Neuman, M, Story, D, Gruen, R, Evered, L, Scott, D, Silbert, B, van Dijk, D, Grocott, H, Eckenhoff, R, Rasmussen, L, Eriksson, L, Beattie, S, Landoni, G, Leslie, K, Howell, S, Nagele, P, Richards, T, Lamy, A, Lalu, M, Pearse, R, Mythen, M, Canet, J, Moller, A, Gin, T, Schultz, M, Pelosi, P, Gabreu, M, Futier, E, Creagh-Brown, B, Abbott, T, Klein, A, Corcoran, T, Jamie Cooper, D, Dieleman, S, McIlroy, D, Bellomo, R, Shaw, A, Prowle, J, Karkouti, K, Billings, J, Mazer, D, Jayarajah, M, Murphy, M, Bartoszko, J, Sneyd, R, Morris, S, George, R, Shulman, M, Lane-Fall, M, Nilsson, U, Stevenson, N, Cooper, JDJ, van Klei, W, Cabrini, L, Miller, T, Pace, N, Jackson, S, Buggy, D, Short, T, Riedel, B, Gottumukkala, V, Alkhaffaf, B, and Johnson, M

Published
2019

16. Systematic review and consensus definitions for the Standardised Endpoints in Perioperative Medicine initiative: clinical indicators

Author

Haller, Guy, primary, Bampoe, Sohail, additional, Cook, Tim, additional, Fleisher, Lee A., additional, Grocott, Michael P.W., additional, Neuman, Mark, additional, Story, David, additional, Myles, Paul S., additional, Myles, P., additional, Grocott, M., additional, Biccard, B., additional, Blazeby, J., additional, Boney, O., additional, Chan, M., additional, Diouf, E., additional, Fleisher, L., additional, Kalkman, C., additional, Kurz, A., additional, Moonesinghe, R., additional, Wijeysundera, D., additional, Gan, T.J., additional, Peyton, P., additional, Sessler, D., additional, Tramèr, M., additional, Cyna, A., additional, De Oliveira, G.S., additional, Wu, C., additional, Jensen, M., additional, Kehlet, H., additional, Botti, M., additional, Haller, G., additional, Cook, T., additional, Neuman, M., additional, Story, D., additional, Gruen, R., additional, Bampoe, S., additional, Evered, L., additional, Scott, D., additional, Silbert, B., additional, van Dijk, D., additional, Grocott, H., additional, Eckenhoff, R., additional, Rasmussen, L., additional, Eriksson, L., additional, Beattie, S., additional, Landoni, G., additional, Leslie, K., additional, Howell, S., additional, Nagele, P., additional, Richards, T., additional, Lamy, A., additional, Lalu, M., additional, Pearse, R., additional, Mythen, M., additional, Canet, J., additional, Moller, A., additional, Gin, T., additional, Schultz, M., additional, Pelosi, P., additional, Gabreu, M., additional, Futier, E., additional, Creagh-Brown, B., additional, Abbott, T., additional, Klein, A., additional, Corcoran, T., additional, Jamie Cooper, D., additional, Dieleman, S., additional, McIlroy, D., additional, Bellomo, R., additional, Shaw, A., additional, Prowle, J., additional, Karkouti, K., additional, Billings, J., additional, Mazer, D., additional, Jayarajah, M., additional, Murphy, M., additional, Bartoszko, J., additional, Sneyd, R., additional, Morris, S., additional, George, R., additional, Shulman, M., additional, Lane-Fall, M., additional, Nilsson, U., additional, Stevenson, N., additional, Cooper, J.D.J., additional, van Klei, W., additional, Cabrini, L., additional, Miller, T., additional, Pace, N., additional, Jackson, S., additional, Buggy, D., additional, Short, T., additional, Riedel, B., additional, Gottumukkala, V., additional, Alkhaffaf, B., additional, and Johnson, M., additional

Published
2019
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17. A systematic review and consensus definitions for standardised end-points in perioperative medicine: pulmonary complications

Author

Abbott, TEF, Fowler, AJ, Pelosi, P, Gama de Abreu, M, Møller, AM, Canet, J, Creagh-Brown, B, Mythen, M, Gin, T, Lalu, MM, Futier, E, Grocott, MP, Schultz, MJ, Pearse, RM, Myles, P, Gan, TJ, Kurz, A, Peyton, P, Sessler, D, Tramèr, M, Cyna, A, De Oliveira, GS, Wu, C, Jensen, M, Kehlet, H, Botti, Mari, Boney, O, Haller, G, Grocott, M, Cook, T, Fleisher, L, Neuman, M, Story, D, Gruen, R, Bampoe, S, Evered, L, Scott, D, Silbert, B, van Dijk, D, Kalkman, C, Chan, M, Grocott, H, Eckenhoff, R, Rasmussen, L, Eriksson, L, Beattie, S, Wijeysundera, D, Landoni, G, Leslie, K, Biccard, B, Howell, S, Nagele, P, Richards, T, Lamy, A, Gabreu, M, Klein, A, Corcoran, T, Jamie Cooper, D, Dieleman, S, Diouf, E, McIlroy, D, Bellomo, R, Shaw, A, Prowle, J, Karkouti, K, Billings, J, Mazer, D, Jayarajah, M, Murphy, M, Bartoszko, J, Sneyd, R, Morris, S, George, R, Moonesinghe, R, Shulman, M, Lane-Fall, M, Nilsson, U, Stevenson, N, van Klei, W, Cabrini, L, Miller, T, Pace, N, Jackson, S, Buggy, D, Short, T, Riedel, B, Gottumukkala, V, Alkhaffaf, B, Johnson, M, Abbott, TEF, Fowler, AJ, Pelosi, P, Gama de Abreu, M, Møller, AM, Canet, J, Creagh-Brown, B, Mythen, M, Gin, T, Lalu, MM, Futier, E, Grocott, MP, Schultz, MJ, Pearse, RM, Myles, P, Gan, TJ, Kurz, A, Peyton, P, Sessler, D, Tramèr, M, Cyna, A, De Oliveira, GS, Wu, C, Jensen, M, Kehlet, H, Botti, Mari, Boney, O, Haller, G, Grocott, M, Cook, T, Fleisher, L, Neuman, M, Story, D, Gruen, R, Bampoe, S, Evered, L, Scott, D, Silbert, B, van Dijk, D, Kalkman, C, Chan, M, Grocott, H, Eckenhoff, R, Rasmussen, L, Eriksson, L, Beattie, S, Wijeysundera, D, Landoni, G, Leslie, K, Biccard, B, Howell, S, Nagele, P, Richards, T, Lamy, A, Gabreu, M, Klein, A, Corcoran, T, Jamie Cooper, D, Dieleman, S, Diouf, E, McIlroy, D, Bellomo, R, Shaw, A, Prowle, J, Karkouti, K, Billings, J, Mazer, D, Jayarajah, M, Murphy, M, Bartoszko, J, Sneyd, R, Morris, S, George, R, Moonesinghe, R, Shulman, M, Lane-Fall, M, Nilsson, U, Stevenson, N, van Klei, W, Cabrini, L, Miller, T, Pace, N, Jackson, S, Buggy, D, Short, T, Riedel, B, Gottumukkala, V, Alkhaffaf, B, and Johnson, M

Published
2018

18. A systematic review and consensus definitions for standardised end-points in perioperative medicine:pulmonary complications

Author

Abbott, T. E.F., Fowler, A. J., Pelosi, P., Gama de Abreu, M., Møller, A. M., Canet, J., Creagh-Brown, B., Mythen, M., Gin, T., Lalu, M. M., Futier, E., Grocott, M. P., Schultz, M. J., Pearse, R. M., Myles, P., Gan, T. J., Kurz, A., Peyton, P., Sessler, D., Tramèr, M., Cyna, A., De Oliveira, G. S., Wu, C., Jensen, M., Kehlet, H., Botti, M., Boney, O., Haller, G., Cook, T., Fleisher, L., Neuman, M., Story, D., Gruen, R., Bampoe, S., Evered, Lis, Scott, D., Silbert, B., van Dijk, D., Kalkman, C., Chan, M., Grocott, H., Eckenhoff, R., Rasmussen, L., Eriksson, L., Beattie, S., Wijeysundera, D., Landoni, G., Leslie, K., Biccard, B., Howell, S., Nagele, P., Richards, T., Lamy, A., Gabreu, M., Klein, A., Corcoran, T., Jamie Cooper, D., Dieleman, S., Diouf, E., McIlroy, D., Bellomo, R., Shaw, A., Prowle, J., Karkouti, K., Billings, J., Mazer, D., Jayarajah, M., Murphy, M., Bartoszko, J., Sneyd, R., Morris, S., George, R., Moonesinghe, R., Shulman, M., Lane-Fall, M., Nilsson, U., Stevenson, N., van Klei, W., Cabrini, L., Miller, T., Pace, N., Jackson, S., Buggy, D., Short, T., Riedel, B., Gottumukkala, V., Alkhaffaf, B., Johnson, M., Abbott, T. E.F., Fowler, A. J., Pelosi, P., Gama de Abreu, M., Møller, A. M., Canet, J., Creagh-Brown, B., Mythen, M., Gin, T., Lalu, M. M., Futier, E., Grocott, M. P., Schultz, M. J., Pearse, R. M., Myles, P., Gan, T. J., Kurz, A., Peyton, P., Sessler, D., Tramèr, M., Cyna, A., De Oliveira, G. S., Wu, C., Jensen, M., Kehlet, H., Botti, M., Boney, O., Haller, G., Cook, T., Fleisher, L., Neuman, M., Story, D., Gruen, R., Bampoe, S., Evered, Lis, Scott, D., Silbert, B., van Dijk, D., Kalkman, C., Chan, M., Grocott, H., Eckenhoff, R., Rasmussen, L., Eriksson, L., Beattie, S., Wijeysundera, D., Landoni, G., Leslie, K., Biccard, B., Howell, S., Nagele, P., Richards, T., Lamy, A., Gabreu, M., Klein, A., Corcoran, T., Jamie Cooper, D., Dieleman, S., Diouf, E., McIlroy, D., Bellomo, R., Shaw, A., Prowle, J., Karkouti, K., Billings, J., Mazer, D., Jayarajah, M., Murphy, M., Bartoszko, J., Sneyd, R., Morris, S., George, R., Moonesinghe, R., Shulman, M., Lane-Fall, M., Nilsson, U., Stevenson, N., van Klei, W., Cabrini, L., Miller, T., Pace, N., Jackson, S., Buggy, D., Short, T., Riedel, B., Gottumukkala, V., Alkhaffaf, B., and Johnson, M.

Abstract

Background: There is a need for robust, clearly defined, patient-relevant outcome measures for use in randomised trials in perioperative medicine. Our objective was to establish standard outcome measures for postoperative pulmonary complications research. Methods: A systematic literature search was conducted using MEDLINE, Web of Science, SciELO, and the Korean Journal Database. Definitions were extracted from included manuscripts. We then conducted a three-stage Delphi consensus process to select the optimal outcome measures in terms of methodological quality and overall suitability for perioperative trials. Results: From 2358 records, the full texts of 81 manuscripts were retrieved, of which 45 met the inclusion criteria. We identified three main categories of outcome measure specific to perioperative pulmonary outcomes: (i) composite outcome measures of multiple pulmonary outcomes (27 definitions); (ii) pneumonia (12 definitions); and (iii) respiratory failure (six definitions). These were rated by the group according to suitability for routine use. The majority of definitions were given a low score, and many were imprecise, difficult to apply consistently, or both, in large patient populations. A small number of highly rated definitions were identified as appropriate for widespread use. The group then recommended four outcome measures for future use, including one new definition. Conclusions: A large number of postoperative pulmonary outcome measures have been used, but most are poorly defined. Our four recommended outcome measures include a new definition of postoperative pulmonary complications, incorporating an assessment of severity. These definitions will meet the needs of most clinical effectiveness trials of treatments to improve postoperative pulmonary outcomes.

Published
2018

20. Systematic review and consensus definitions for standardised endpoints in perioperative medicine: postoperative cancer outcomes

Author

Buggy, D.J., primary, Freeman, J., additional, Johnson, M.Z., additional, Leslie, K., additional, Riedel, B., additional, Sessler, D.I., additional, Kurz, A., additional, Gottumukkala, V., additional, Short, T., additional, Pace, N., additional, Myles, P.S., additional, Gan, T.J., additional, Peyton, P., additional, Tramèr, M., additional, Cyna, A., additional, De Oliveira, G.S., additional, Wu, C., additional, Jensen, M., additional, Kehlet, H., additional, Botti, M., additional, Boney, O., additional, Haller, G., additional, Grocott, M., additional, Cook, T., additional, Fleisher, L., additional, Neuman, M., additional, Story, D., additional, Gruen, R., additional, Bampoe, S., additional, Evered, Lis, additional, Scott, D., additional, Silbert, B., additional, van Dijk, D., additional, Kalkman, C., additional, Chan, M., additional, Grocott, H., additional, Eckenhoff, R., additional, Rasmussen, L., additional, Eriksson, L., additional, Beattie, S., additional, Wijeysundera, D., additional, Landoni, G., additional, Biccard, B., additional, Howell, S., additional, Nagele, P., additional, Richards, T., additional, Lamy, A., additional, Lalu, M., additional, Pearse, R., additional, Mythen, M., additional, Canet, J., additional, Moller, A., additional, Gin, T., additional, Schultz, M., additional, Pelosi, P., additional, Gabreu, M., additional, Futier, E., additional, Creagh-Brown, B., additional, Abbott, T., additional, Klein, A., additional, Corcoran, T., additional, Jamie Cooper, D., additional, Dieleman, S., additional, Diouf, E., additional, McIlroy, D., additional, Bellomo, R., additional, Shaw, A., additional, Prowle, J., additional, Karkouti, K., additional, Billings, J., additional, Mazer, D., additional, Jayarajah, M., additional, Murphy, M., additional, Bartoszko, J., additional, Sneyd, R., additional, Morris, S., additional, George, R., additional, Moonesinghe, R., additional, Shulman, M., additional, Lane-Fall, M., additional, Nilsson, U., additional, Stevenson, N., additional, van Klei, W., additional, Cabrini, L., additional, Miller, T., additional, Jackson, S., additional, and Alkhaffaf, B., additional

Published
2018
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21. A systematic review and consensus definitions for standardised end-points in perioperative medicine: pulmonary complications

Author

Abbott, T.E.F., primary, Fowler, A.J., additional, Pelosi, P., additional, Gama de Abreu, M., additional, Møller, A.M., additional, Canet, J., additional, Creagh-Brown, B., additional, Mythen, M., additional, Gin, T., additional, Lalu, M.M., additional, Futier, E., additional, Grocott, M.P., additional, Schultz, M.J., additional, Pearse, R.M., additional, Myles, P., additional, Gan, T.J., additional, Kurz, A., additional, Peyton, P., additional, Sessler, D., additional, Tramèr, M., additional, Cyna, A., additional, De Oliveira, G.S., additional, Wu, C., additional, Jensen, M., additional, Kehlet, H., additional, Botti, M., additional, Boney, O., additional, Haller, G., additional, Grocott, M., additional, Cook, T., additional, Fleisher, L., additional, Neuman, M., additional, Story, D., additional, Gruen, R., additional, Bampoe, S., additional, Evered, Lis, additional, Scott, D., additional, Silbert, B., additional, van Dijk, D., additional, Kalkman, C., additional, Chan, M., additional, Grocott, H., additional, Eckenhoff, R., additional, Rasmussen, L., additional, Eriksson, L., additional, Beattie, S., additional, Wijeysundera, D., additional, Landoni, G., additional, Leslie, K., additional, Biccard, B., additional, Howell, S., additional, Nagele, P., additional, Richards, T., additional, Lamy, A., additional, Gabreu, M., additional, Klein, A., additional, Corcoran, T., additional, Jamie Cooper, D., additional, Dieleman, S., additional, Diouf, E., additional, McIlroy, D., additional, Bellomo, R., additional, Shaw, A., additional, Prowle, J., additional, Karkouti, K., additional, Billings, J., additional, Mazer, D., additional, Jayarajah, M., additional, Murphy, M., additional, Bartoszko, J., additional, Sneyd, R., additional, Morris, S., additional, George, R., additional, Moonesinghe, R., additional, Shulman, M., additional, Lane-Fall, M., additional, Nilsson, U., additional, Stevenson, N., additional, van Klei, W., additional, Cabrini, L., additional, Miller, T., additional, Pace, N., additional, Jackson, S., additional, Buggy, D., additional, Short, T., additional, Riedel, B., additional, Gottumukkala, V., additional, Alkhaffaf, B., additional, and Johnson, M., additional

Published
2018
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31. Systematic review and consensus definitions for the Standardized Endpoints in Perioperative Medicine (StEP) initiative: cardiovascular outcomes

Author

W. Scott Beattie, Manoj Lalu, Matthew Bocock, Simon Feng, Duminda N. Wijeysundera, Peter Nagele, Lee A. Fleisher, Andrea Kurz, Bruce Biccard, Kate Leslie, Simon Howell, Giovanni Landoni, Hilary Grocott, Andre Lamy, Toby Richards, Paul Myles, T.J. Gan, Phil Peyton, Dan Sessler, Martin Tramèr, Alan Cyna, Gildasio S. De Oliveira, Christopher Wu, Mark Jensen, Henrik Kehlet, Mari Botti, Oliver Boney, Guy Haller, Mike Grocott, Tim Cook, Lee Fleisher, Mark Neuman, David Story, Russell Gruen, Sam Bampoe, Lis Evered, David Scott, Brendan Silbert, Diederik van Dijk, Cor Kalkman, Matthew Chan, Rod Eckenhoff, Lars Rasmussen, Lars Eriksson, Scott Beattie, Duminda Wijeysundera, Richard J. Bartlett, Robert McMonnies, Jacob Gerstl, Mohammad Jay, David Kishlyansky, Matthew Machina, Matthew Bobcock, Rupert Pearse, Monty Mythen, Jaume Canet, Ann Moller, Tony Gin, Marcus Schultz, Paolo Pelosi, Marcelo Gabreu, Emmanuel Futier, Ben Creagh-Brown, Tom Abbott, Andy Klein, Tomas Corcoran, D. Jamie Cooper, Stefan Dieleman, Elisabeth Diouf, David McIlroy, Rinaldo Bellomo, Andrew Shaw, John Prowle, Keyvan Karkouti, Josh Billings, David Mazer, Mohindas Jayarajah, Michael Murphy, Justyna Bartoszko, Rob Sneyd, Steve Morris, Ron George, Ramani Moonesinghe, Mark Shulman, Meghan Lane-Fall, Ulrica Nilsson, Nathalie Stevenson, Jamie (DJ) Cooper, Wilton van Klei, Luca Cabrini, Tim Miller, Nathan Pace, Sandy Jackson, Donal Buggy, Tim Short, Bernhard Riedel, Vijay Gottumukkala, Bilal Alkhaffaf, Mark Johnson, Beattie, W. S., Lalu, M., Bocock, M., Feng, S., Wijeysundera, D. N., Nagele, P., Fleisher, L. A., Kurz, A., Biccard, B., Leslie, K., Howell, S., Landoni, G., Grocott, H., Lamy, A., Richards, T., Myles, P., Cooper, D. J., Gan, T. J., Peyton, P., Sessler, D., Tramer, M., Cyna, A., De Oliveira, G. S., Wu, C., Jensen, M., Kehlet, H., Botti, M., Boney, O., Haller, G., Grocott, M., Cook, T., Fleisher, L., Neuman, M., Story, D., Gruen, R., Bampoe, S., Evered, L., Scott, D., Silbert, B., van Dijk, D., Kalkman, C., Chan, M., Eckenhoff, R., Rasmussen, L., Eriksson, L., Beattie, S., Wijeysundera, D., Bartlett, R. J., Mcmonnies, R., Gerstl, J., Jay, M., Kishlyansky, D., Machina, M., Bobcock, M., Pearse, R., Mythen, M., Canet, J., Moller, A., Gin, T., Schultz, M., Pelosi, P., Gabreu, M., Futier, E., Creagh-Brown, B., Abbott, T., Klein, A., Corcoran, T., Dieleman, S., Diouf, E., Mcilroy, D., Bellomo, R., Shaw, A., Prowle, J., Karkouti, K., Billings, J., Mazer, D., Jayarajah, M., Murphy, M., Bartoszko, J., Sneyd, R., Morris, S., George, R., Moonesinghe, R., Shulman, M., Lane-Fall, M., Nilsson, U., Stevenson, N., Cooper, J. D., van Klei, W., Cabrini, L., Miller, T., Pace, N., Jackson, S., Buggy, D., Short, T., Riedel, B., Gottumukkala, V., Alkhaffaf, B., Johnson, M., Tramer, Martin, and Haller, Guy Serge Antoine

Subjects
medicine.medical_specialty, Consensus, Heart disease, Delphi Technique, Endpoint Determination, perioperative medicine, MACE, Cochrane Library, Perioperative Care, 03 medical and health sciences, Patient safety, cardiovascular events, outcome measures, 0302 clinical medicine, Postoperative Complications, 030202 anesthesiology, Anesthesiology, medicine, Humans, clinical trials, myocardial infarction, standardised endpoint, Intensive care medicine, Adverse effect, Clinical Trials as Topic, Perioperative medicine, ddc:617, business.industry, Cardiovascular Diseases, Perioperative Medicine, Research Design, Perioperative, medicine.disease, Clinical trial, Anesthesiology and Pain Medicine, business
Abstract

Background: Adverse cardiovascular events are a leading cause of perioperative morbidity and mortality. The definitions of perioperative cardiovascular adverse events are heterogeneous. As part of the international Standardized Endpoints in Perioperative Medicine initiative, this study aimed to find consensus amongst clinical trialists on a set of standardised and valid cardiovascular outcomes for use in future perioperative clinical trials.Methods: We identified currently used perioperative cardiovascular outcomes by a systematic review of the anaesthesia and perioperative medicine literature (PubMed/Ovid, Embase, and Cochrane Library). We performed a three-stage Delphi consensus-gaining process that involved 55 clinician researchers worldwide. Cardiovascular outcomes were first shortlisted and the most suitable definitions determined. These cardiovascular outcomes were then assessed for validity, reliability, feasibility, and clarity.Results: We identified 18 cardiovascular outcomes. Participation in the three Delphi rounds was 100% (n=19), 71% (n=55), and 89% (n=17), respectively. A final list of nine cardiovascular outcomes was elicited from the consensus: myocardial infarction, myocardial injury, cardiovascular death, non-fatal cardiac arrest, coronary revascularisation, major adverse cardiac events, pulmonary embolism, deep vein thrombosis, and atrial fibrillation. These nine cardiovascular outcomes were rated by the majority of experts as valid, reliable, feasible, and clearly defined.Conclusions: These nine consensus cardiovascular outcomes can be confidently used as endpoints in clinical trials designed to evaluate perioperative interventions with the goal of improving perioperative outcomes.

Published
2021

32. The effect of perioperative benzodiazepine administration on postoperative nausea and vomiting: a systematic review and meta-analysis of randomised controlled trials.

Author

Au E, Zhao K, Belley-Côté E, Song Y, Al-Hazzani W, Sadeghirad B, Wang E, Young J, Kashani H, Kavosh M, Inami T, Beaver C, Kloppenburg S, Mazer D, Jacobsohn E, Um K, and Spence J

Abstract

Background: Despite recent systematic reviews suggesting their benefit for postoperative nausea, vomiting, or both (PONV) prevention, benzodiazepines have not been incorporated into guidelines for PONV prophylaxis because of concerns about possible adverse effects. We conducted an updated meta-analysis to inform future practice guidelines., Methods: We included randomised controlled trials (RCTs) of all languages comparing benzodiazepines with non-benzodiazepine comparators in adults undergoing inpatient surgery. Our outcomes were postoperative nausea, vomiting, or both. We assessed risk of bias for RCTs using the Cochrane Risk of Bias tool. We pooled data using a random-effects model and assessed the quality of evidence for each outcome using the Grading of Recommendations, Assessment, Development and Evaluation (GRADE) approach., Results: We screened 31 413 abstracts and 950 full texts. We included 119 RCTs; 104 were included in quantitative synthesis. Based on moderate certainty evidence, we found that perioperative benzodiazepine administration reduced the incidence of PONV (52 studies, n=5086, relative risk [RR]: 0.77, 95% confidence interval [CI] 0.66-0.89; number needed to treat [NNT] 16; moderate certainty), postoperative nausea (55 studies, n=5916, RR: 0.72, 95% CI 0.62-0.83; NNT 21; moderate certainty), and postoperative vomiting (52 studies, n=5909, RR: 0.74, 95% CI 0.60-0.91; NNT 55; moderate certainty)., Conclusions: Moderate quality evidence shows that perioperative benzodiazepine administration decreases the incidence of PONV. The results of this systematic review and meta-analysis will inform future clinical practice guidelines., Systematic Review Protocol: The protocol for this systematic review was pre-registered with PROSPERO International Prospective Register of Systematic Reviews (CRD42022361088) and published in BMJ Open (PMID 31831540)., (Copyright © 2023 British Journal of Anaesthesia. Published by Elsevier Ltd. All rights reserved.)

Published
2024
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33. Predictors of mitral valve haemodynamics after mitral valve repair for degenerative mitral regurgitation.

Author

Rumman RK, Verma S, Chan V, Mazer D, Quan A, Hibino M, De Varennes B, Chu MWA, Latter D, Teoh H, Yanagawa B, Leong-Poi H, and Connelly KA

Subjects
Humans, Male, Middle Aged, Aged, Female, Mitral Valve diagnostic imaging, Mitral Valve surgery, Canada, Hemodynamics, Treatment Outcome, Mitral Valve Insufficiency diagnostic imaging, Mitral Valve Insufficiency surgery, Mitral Valve Insufficiency etiology, Mitral Valve Annuloplasty adverse effects, Mitral Valve Annuloplasty methods, Mitral Valve Stenosis complications
Abstract

Objective: Intraoperative predictors of functional mitral valve (MV) stenosis after surgical repair of mitral regurgitation (MR) caused by prolapse remain poorly characterised. This study evaluated the effect of annuloplasty size on postoperative MV haemodynamics during exercise and evaluated predictors of MV hemodynamics., Methods: 104 patients were randomly assigned to leaflet resection or preservation for surgical repair of MR in the Canadian Mitral Research Alliance CardioLink-2 study. In this post hoc analysis, we compared MV haemodynamics between the two surgical groups and examined the relationship between annuloplasty size and MV haemodynamics 1 year after repair in the combined groups. Echocardiograms were performed at baseline and intraoperatively. Exercise transthoracic echocardiography was performed 1 year postoperatively. Multivariable linear regression analysis was used to identify predictors of exercise MV gradients at follow-up., Results: Mean age of participants was 65±10 years, and 83% were male. Median annuloplasty size was 34 (IQR 32-36). Dividing by the median, 48 (46%) had annuloplasty size of <34 mm and 56 (54%) had ≥34 mm. Mean and peak exercise gradients at 1 year were 11±5 mm Hg and 22±9 mm Hg in <34, and 6±3 mm Hg and 14±5 mm Hg in ≥34 (p<0.001). Rate of residual MR was similar in both groups. In multivariable analyses, annuloplasty size of ≥34 mm was associated with lower mean and peak exercise gradients at 12 months, after adjustment for repair type, age, sex, heart rate and body surface area (β -4.1, 95% CI -6 to -3, p<0.001, and β -7 95% CI -10 to -4, p<0.001, respectively). Intraoperative mean and peak MV gradients by transesophageal echocardiography independently predicted mean and peak resting and exercise gradients at follow-up (p<0.001). Similar results were obtained in both leaflet resection and preservation., Conclusion: Annuloplasty size of ≥34 mm is associated with a 4 and 7 mm Hg reduction in mean and peak exercise MV gradients, respectively, 1 year post MV repair regardless of the repair strategy used. Intraoperative TEE MV gradients predict exercise MV gradients 1 year post repair., Trial Registration Number: NCT02552771., Competing Interests: Competing interests: SV holds a tier 1 Canada Research chair in Cardiovascular Surgery; and reports receiving research grants and/or speaking honoraria from Amarin, Amgen, AstraZeneca, Bayer, Boehringer Ingelheim, Canadian Medical and Surgical Knowledge Translation Research Group, Eli Lilly, EOCI Pharmacomm, HLS Therapeutics, Janssen, Novartis, Novo Nordisk, Otsuka, Pfizer, PhaseBio, Sanofi, Sun Pharmaceuticals and the Toronto Knowledge Translation Working Group. He is the president of the Canadian Medical and Surgical Knowledge Translation Research Group, a federally incorporated not-for-profit physician organisation. CDM is supported by a merit award from the University of Toronto Department of Anesthesiology and Pain Medicine and reports advisory board honoraria/consulting fees from Amgen, AstraZeneca, BioAge, Boehringer Ingelheim and PhaseBio and DSMB stipends from Beth Israel Deaconess Medical Center, Cerus and Takeda. BDV reports acting as a consultant for Edwards LifeSciences. MC is supported by the Ray and Margaret Elliot Chair in Surgical Innovation and reports speakers’ honoraria from Medtronic, Edwards Lifesciences, Terumo Aortic, Abbott Vascular and Cryolife. HL-P holds the Brazilian Ball Chair in Cardiology and reports receiving honoraria for speaking engagements from Lantheus Medical Imaging and Janssen. KC is listed as an inventor on a patent application by Boehringer Ingelheim on the use of dipeptidyl peptidase-4 inhibitors in heart failure and reports receiving research grants to his institution from AstraZeneca, Servier and Boehringer Ingelheim; support for travel to scientific meetings from Boehringer Ingelheim; and honoraria for speaking engagements and ad hoc participation in advisory boards from Servier, Merck, Eli Lilly, AstraZeneca, Boehringer Ingelheim, Ferring, Novo Nordisk, Novartis and Janssen., (© Author(s) (or their employer(s)) 2023. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2023
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36. Morbidity and mortality in patients managed with high compared with low blood pressure targets during on-pump cardiac surgery: a systematic review and meta-analysis of randomized controlled trials.

Author

McEwen CC, Amir T, Qiu Y, Young J, Kennedy K, Grocott HP, Kashani H, Mazer D, Brudney S, Kavosh M, Jacobsohn E, Vedel A, Wang E, Whitlock RP, Belley-Coté EP, and Spence J

Subjects
Adult, Cardiopulmonary Bypass adverse effects, Humans, Morbidity, Randomized Controlled Trials as Topic, Cardiac Surgical Procedures, Hypotension
Abstract

Purpose: Many believe that blood pressure management during cardiac surgery is associated with postoperative outcomes. We conducted a systematic review and meta-analysis of randomized controlled trials (RCTs) to determine the impact of high compared with low intraoperative blood pressure targets on postoperative morbidity and mortality in adults undergoing cardiac surgery on cardiopulmonary bypass (CPB). Our primary objective was to inform the design of a future large RCT., Source: We searched MEDLINE, EMBASE, Web of Science, CINAHL, and CENTRAL for RCTs comparing high with low intraoperative blood pressure targets in adult patients undergoing any cardiac surgical procedure on CPB. We screened reference lists, grey literature, and conference proceedings., Principal Findings: We included eight RCTs (N =1,116 participants); all examined the effect of blood pressure management only during the CPB. Trial definitions of high compared with low blood pressure varied and, in some, there was a discrepancy between the target and achieved mean arterial pressure. We observed no difference in delirium, cognitive decline, stroke, acute kidney injury, or mortality between high and low blood pressure targets (very-low to low quality evidence). Higher blood pressure targets may have increased the risk of requiring a blood transfusion (three trials; n = 456 participants; relative risk, 1.4; 95% confidence interval, 1.1 to 1.9; P = 0.01; moderate quality evidence) but this finding was based on a small number of trials., Conclusion: Individual trial definitions of high and low blood pressure targets varied, limiting inferences. The effect of high (compared with low) blood pressure targets on other morbidity and mortality after cardiac surgery remains unclear because of limitations with the body of existing evidence. Research to determine the optimal management of blood pressure during cardiac surgery is required., Study Registration: PROSPERO (CRD42020177376); registered: 5 July 2020., (© 2022. Canadian Anesthesiologists' Society.)

Published
2022
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37. Safety and efficacy of perioperative benzodiazepine administration: study protocol for a systematic review and meta-analysis.

Author

Spence J, Young J, Alhazzani W, Whitlock R, D'Aragon F, Um K, Mazer D, Beaver C, Jacobsohn E, and Belley-Cote E

Subjects
Anti-Anxiety Agents pharmacology, Humans, Meta-Analysis as Topic, Research Design, Systematic Reviews as Topic, Benzodiazepines pharmacology, Perioperative Care methods, Postoperative Cognitive Complications chemically induced, Postoperative Cognitive Complications diagnosis, Surgical Procedures, Operative psychology
Abstract

Introduction: Perioperative benzodiazepines are used because of their anxiolytic, sedative and amnestic effects. Evidence has demonstrated an association of benzodiazepines with adverse neuropsychiatric effects. Nonetheless, because of their potential benefits, perioperative benzodiazepines continue to be used routinely. We seek to evaluate the body of evidence of the risks and benefits of benzodiazepine use during the perioperative period., Methods and Analysis: We will search Cochrane CENTRAL, MEDLINE, EMBASE, PsychINFO, CINAHL and Web of Science from inception to March 2019 for randomised controlled trials (RCTs) and observational studies evaluating the administration of benzodiazepine medications as compared with all other medications (or nothing) in patients undergoing cardiac and non-cardiac surgery. We will exclude studies assessing the use of benzodiazepines for procedural sedation or day surgery. We will examine the impact of giving these medications before, during and after surgery. Outcomes of interest include the incidence of delirium, duration of delirium, postprocedure cognitive change, the incidence of intraoperative awareness, patient satisfaction/quality of life/quality of recovery, length-of-stay (LOS) in the intensive care unit (ICU), hospital LOS and in-hospital mortality.Reviewers will screen references and assess eligibility using predefined criteria independently and in duplicate. Two reviewers will independently collect data using prepiloted forms. We will present results separately for RCTs and observational studies. We will pool data using a random effect model and present results as relative risk with 95% CIs for dichotomous outcomes and mean difference with 95% CI for continuous outcomes. We will pool adjusted ORs for observational studies. We will assess risk of bias for individual studies using the Cochrane Collaboration tool for RCTs. For observational studies, we will use tools designed by the Clinical Advances through Research and Information Translation group. Quality of evidence for each outcome will be assessed using the Grading of Recommendations Assessment, Development and Evaluation approach., Ethics and Dissemination: This systematic review involves no patient contact and no interaction with healthcare providers or systems. As such, we did not seek ethics board approval. We will disseminate the findings of our systematic review through the presentation at peer-reviewed conferences and by seeking publication in a peer-reviewed journal., Prospero Registration Number: CRD42019128144., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2019. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2019
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38. Reporting preclinical anesthesia study (REPEAT): Evaluating the quality of reporting in the preclinical anesthesiology literature.

Author

Fergusson DA, Avey MT, Barron CC, Bocock M, Biefer KE, Boet S, Bourque SL, Conic I, Chen K, Dong YY, Fox GM, George RB, Goldenberg NM, Gragasin FS, Harsha P, Hong PJ, James TE, Larrigan SM, MacNeil JL, Manuel CA, Maximos S, Mazer D, Mittal R, McGinn R, Nguyen LH, Patel A, Richebé P, Saha TK, Steinberg BE, Sampson SD, Stewart DJ, Syed S, Vella K, Wesch NL, and Lalu MM

Subjects
Analgesics therapeutic use, Animals, Databases, Factual, Guidelines as Topic, Pain drug therapy, Drug Evaluation, Preclinical standards, Research Report standards
Abstract

Poor reporting quality may contribute to irreproducibility of results and failed 'bench-to-bedside' translation. Consequently, guidelines have been developed to improve the complete and transparent reporting of in vivo preclinical studies. To examine the impact of such guidelines on core methodological and analytical reporting items in the preclinical anesthesiology literature, we sampled a cohort of studies. Preclinical in vivo studies published in Anesthesiology, Anesthesia & Analgesia, Anaesthesia, and the British Journal of Anaesthesia (2008-2009, 2014-2016) were identified. Data was extracted independently and in duplicate. Reporting completeness was assessed using the National Institutes of Health Principles and Guidelines for Reporting Preclinical Research. Risk ratios were used for comparative analyses. Of 7615 screened articles, 604 met our inclusion criteria and included experiments reporting on 52 490 animals. The most common topic of investigation was pain and analgesia (30%), rodents were most frequently used (77%), and studies were most commonly conducted in the United States (36%). Use of preclinical reporting guidelines was listed in 10% of applicable articles. A minority of studies fully reported on replicates (0.3%), randomization (10%), blinding (12%), sample-size estimation (3%), and inclusion/exclusion criteria (5%). Statistics were well reported (81%). Comparative analysis demonstrated few differences in reporting rigor between journals, including those that endorsed reporting guidelines. Principal items of study design were infrequently reported, with few differences between journals. Methods to improve implementation and adherence to community-based reporting guidelines may be necessary to increase transparent and consistent reporting in the preclinical anesthesiology literature., Competing Interests: The authors have declared that no competing interests exist.

Published
2019
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39. Assessment of safety and efficacy of mesenchymal stromal cell therapy in preclinical models of acute myocardial infarction: a systematic review protocol.

Author

Barron CC, Lalu MM, Stewart DJ, Fergusson D, Yang H, Moher D, Liu P, Mazer D, Devereaux PJ, and McIntyre L

Subjects
Animals, Humans, Myocardial Infarction physiopathology, Research Design, Systematic Reviews as Topic, Ventricular Function, Left, Mesenchymal Stem Cell Transplantation, Mesenchymal Stem Cells, Myocardial Infarction surgery
Abstract

Background: Despite advances in treatment, acute myocardial infarction (MI) is still associated with significant morbidity and mortality, especially in patients with extensive damage and scar formation. Based on some promising preclinical studies, there is interest in the use of mesenchymal stromal cells (MSCs) to promote cardiac repair after acute MI. However, there is a need for a systematic review of this evidence to summarize the efficacy and safety of MSCs in preclinical models of MI. This will better inform the translation of MSC therapy for acute MI and guide the design of a future clinical trial., Methods/design: A systematic literature search of MEDLINE, Embase, and BIOSIS Previews will be conducted. We will identify comparative preclinical studies (randomized and non-randomized) of myocardial infarction that include animals given MSC therapy versus a vehicle/placebo. The primary outcome will be left ventricular ejection fraction. Secondary and tertiary outcomes will include death, infarct size, measures of cardiac function, biochemical outcomes, and MSC retention and differentiation. Risk of bias will be assessed using the Cochrane Risk of Bias Tool. Subgroup analyses will be performed to measure how various sources of preclinical study heterogeneity affect the direction and magnitude of the primary outcome. We will meta-analyze data using inverse variance random effects modeling., Discussion: This systematic review of preclinical evidence will provide a summary of the efficacy and safety of MSCs in animal models of MI. The results will help determine whether sufficient evidence exists to conduct a clinical trial in humans and inform its design.

Published
2017
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40. Cerebral Oximetry Monitoring to Maintain Normal Cerebral Oxygen Saturation during High-risk Cardiac Surgery: A Randomized Controlled Feasibility Trial.

Author

Deschamps A, Hall R, Grocott H, Mazer CD, Choi PT, Turgeon AF, de Medicis E, Bussières JS, Hudson C, Syed S, Seal D, Herd S, Lambert J, Denault A, Deschamps A, Mutch A, Turgeon A, Denault A, Todd A, Jerath A, Fayad A, Finnegan B, Kent B, Kennedy B, Cuthbertson BH, Kavanagh B, Warriner B, MacAdams C, Lehmann C, Fudorow C, Hudson C, McCartney C, McIsaac D, Dubois D, Campbell D, Mazer D, Neilpovitz D, Rosen D, Cheng D, Drapeau D, Dillane D, Tran D, Mckeen D, Wijeysundera D, Jacobsohn E, Couture E, de Medicis E, Alam F, Abdallah F, Ralley FE, Chung F, Lellouche F, Dobson G, Germain G, Djaiani G, Gilron I, Hare G, Bryson G, Clarke H, McDonald H, Roman-Smith H, Grocott H, Yang H, Douketis J, Paul J, Beaubien J, Bussières J, Pridham J, Armstrong JN, Parlow J, Murkin J, Gamble J, Duttchen K, Karkouti K, Turner K, Baghirzada L, Szabo L, Lalu M, Wasowicz M, Bautista M, Jacka M, Murphy M, Schmidt M, Verret M, Perrault MA, Beaudet N, Buckley N, Choi P, MacDougall P, Jones P, Drolet P, Beaulieu P, Taneja R, Martin R, Hall R, George R, Chun R, McMullen S, Beattie S, Sampson S, Choi S, Kowalski S, McCluskey S, Syed S, Boet S, Ramsay T, Saha T, Mutter T, Chowdhury T, Uppal V, and Mckay W

Subjects
Aged, Algorithms, Feasibility Studies, Female, Follow-Up Studies, Humans, Male, Oxygen Consumption physiology, Prospective Studies, Risk, Cardiac Surgical Procedures, Cerebrovascular Circulation physiology, Monitoring, Intraoperative methods, Oximetry methods, Oxygen blood
Abstract

Background: Cerebral oxygen desaturation during cardiac surgery has been associated with adverse perioperative outcomes. Before a large multicenter randomized controlled trial (RCT) on the impact of preventing desaturations on perioperative outcomes, the authors undertook a randomized prospective, parallel-arm, multicenter feasibility RCT to determine whether an intervention algorithm could prevent desaturations., Methods: Eight Canadian sites randomized 201 patients between April 2012 and October 2013. The primary outcome was the success rate of reversing cerebral desaturations below 10% relative to baseline in the intervention group. Anesthesiologists were blinded to the cerebral saturation values in the control group. Intensive care unit personnel were blinded to cerebral saturation values for both groups. Secondary outcomes included the area under the curve of cerebral desaturation load, enrolment rates, and a 30-day follow-up for adverse events., Results: Cerebral desaturations occurred in 71 (70%) of the 102 intervention group patients and 56 (57%) of the 99 control group patients (P = 0.04). Reversal was successful in 69 (97%) of the intervention group patients. The mean cerebral desaturation load (SD) in the operating room was smaller for intervention group patients compared with control group patients (104 [217] %.min vs. 398 [869] %.min, mean difference, -294; 95% CI, -562 to -26; P = 0.03). This was also true in the intensive care unit (P = 0.02). There were no differences in adverse events between the groups., Conclusions: Study sites were successful in reversal of desaturation, patient recruitment, randomization, and follow-up in cardiac surgery, supporting the feasibility of conducting a large multicenter RCT.

Published
2016
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41. From concept to publication: celebrating mentorship and knowledge generation through research during postgraduate residency training.

Author

Beattie WS, Donati F, Cheng D, Mazer D, and Miller DR

Subjects
Female, Humans, Male, Ambulatory Surgical Procedures statistics & numerical data, Aorta physiology, Brain metabolism, Cardiac Surgical Procedures statistics & numerical data, Diastole physiology, Echocardiography, Transesophageal methods, Hemodynamics physiology, One-Lung Ventilation methods, Oxygen Consumption physiology, Patient Admission statistics & numerical data, Sternotomy statistics & numerical data, Surgical Wound Infection epidemiology, Tracheostomy statistics & numerical data
Published
2013
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42. Effect of pneumoperitoneum on renal tissue oxygenation and blood flow in a rat model.

Author

Wiesenthal JD, Fazio LM, Perks AE, Blew BD, Mazer D, Hare G, Honey RJ, and Pace KT

Subjects
Animals, Carbon Dioxide chemistry, Disease Models, Animal, Gases, Humans, Hydrogen-Ion Concentration, Hypoxia metabolism, Laparoscopy methods, Oxygen chemistry, Oxygen metabolism, Pneumoperitoneum metabolism, Pressure, Rats, Rats, Sprague-Dawley, Renal Circulation, Kidney blood supply, Kidney metabolism, Pneumoperitoneum pathology
Abstract

Objectives: To determine the correlation between the renal blood flow (RBF) and tissue oxygenation (PO(2)) at varying intra-abdominal pressures (IAPs) and to compare the effects on renal blood flow from carbon dioxide-induced pneumoperitoneum., Methods: Carbon dioxide pneumoperitoneum was established in Sprague-Dawley rats (n = 6). Licox oxygen/temperature tissue probes were laparoscopically inserted into the renal parenchyma, with the renal PO(2) and RBF recorded every 30 seconds while the IAP was gradually increased. Microprobes measuring the RBF, mean arterial pressures and serum pH were placed into the parenchyma to compare the effects of carbon dioxide pneumoperitoneum (n = 7) with that of open surgery (n = 6) and medical air pneumoperitoneum (n = 6)., Results: Renal PO(2) was inversely related to the IAP (P < .001). Despite the reduction in IAP, the renal PO(2) in the recovery phase was lower than at baseline (P = .045). The renal PO(2) and RBF changed in a virtually identical pattern at varying levels of IAP (P > .05). The RBF significantly declined with a pneumoperitoneal pressure of 15 and 20 mm Hg (P = .022), regardless of the gas used to create the pneumoperitoneum. A partial reversal of the RBF occurred with a decrease of the IAP. The RBF in the open surgical arm remained unchanged. Although both the serum pH and the mean arterial pressure were inversely proportional to the IAP (P < .001), the mean arterial pressure was depressed to the greatest extent in the medical air group (P = .02)., Conclusions: These results have demonstrated that elevated IAP secondary to pneumoperitoneum causes significant renal hypoxia and decreased RBF. Additionally, this experiment has demonstrated the use of the Licox probes in monitoring the renal PO(2) and established a novel method for evaluating the effects of IAP on the kidney., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published
2011
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45. Dual antiplatelet therapy in patients requiring urgent coronary artery bypass grafting surgery: a position statement of the Canadian Cardiovascular Society.

Author

Fitchett D, Eikelboom J, Fremes S, Mazer D, Singh S, Bittira B, Brister S, Graham J, Gupta M, Karkouti K, Lee A, Love M, McArthur R, Peterson M, Verma S, and Yau T

Subjects
Acute Coronary Syndrome surgery, Aspirin therapeutic use, Canada, Clopidogrel, Drug Therapy, Combination, Health Planning Guidelines, Hemorrhage prevention & control, Humans, Risk Factors, Societies, Medical, Ticlopidine analogs & derivatives, Ticlopidine therapeutic use, Treatment Outcome, Acute Coronary Syndrome drug therapy, Coronary Artery Bypass adverse effects, Hemorrhage chemically induced, Platelet Aggregation Inhibitors therapeutic use
Abstract

Unlabelled: Acute coronary syndrome (ACS) guidelines recommend that most patients receive dual antiplatelet therapy with clopidogrel and acetylsalicylic acid (ASA) at the time of presentation to prevent recurrent ischemic events. Approximately 10% of ACS patients require coronary artery bypass grafting surgery (CABG) during the index admission. Most studies show that patients who receive ASA and clopidogrel within five days of CABG have an increase in operative bleeding. Current consensus guidelines recommend discontinuation of clopidogrel therapy at least five days before planned CABG to reduce bleeding-related events. However, high-risk individuals may require urgent surgery without delay, to reduce the risk of potentially fatal ischemic events. The present multidisciplinary position statement provides evidence- based recommendations for the optimal use of dual antiplatelet therapy to balance ischemic and bleeding risks in patients with recent ACS who may require urgent CABG., Recommendations: 1. All ACS patients should be considered for dual antiplatelet therapy with ASA and clopidogrel at the earliest opportunity, despite the possibility of a need for urgent CABG. 2. For patients who have received clopidogrel and ASA, and require CABG: * Those at high risk of an early fatal event (eg, with refractory ischemia despite optimal medical treatment, and with high-risk coronary anatomy (eg, severe left main stenosis with severe right coronary artery disease), should be considered for early surgery without discontinuation of clopidogrel. * In patients with a high bleeding risk (eg, previous surgery, complex surgery) who are also at high risk for an ischemic event, consideration should be given to discontinuing clopidogrel for three to five days before surgery. * Patients at a lower risk for ischemic events (most patients) should have clopidogrel discontinued five days before surgery. 3. For patients who have CABG within five days of receiving clopidogrel and ASA, the risk of major bleeding and transfusion can be minimized by applying multiple strategies before and during surgery. 4. Patients who receive clopidogrel pre-CABG for a recent ACS indication should have clopidogrel restarted after surgery to decrease the risk of recurrent ACS. 5. For patients with a recent coronary stent, the decision to continue clopidogrel until the time of surgery or to discontinue will depend on the risk and potential impact of stent thrombosis. Restarting clopidogrel after CABG will depend on whether the stented vessel was revascularized, the type of stent and the time from stent implantation. Clopidogrel should be restarted when hemostasis is assured to prevent recurrent acute ischemic events.

Published
2009
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46. Physical exercise attenuates the cardiac autonomic deficit induced by nitric oxide synthesis blockade.

Author

Rossi BR, Mazer D, Silveira LC, Jacinto CP, Di Sacco TH, Blanco JH, Cesarino EJ, and Souza HC

Subjects
Adrenergic beta-Antagonists pharmacology, Analysis of Variance, Animals, Atropine Derivatives pharmacology, Autonomic Nervous System drug effects, Blood Pressure drug effects, Blood Pressure physiology, Disease Models, Animal, Enzyme Inhibitors pharmacology, Heart Rate drug effects, Heart Rate physiology, Hypertension chemically induced, Male, NG-Nitroarginine Methyl Ester pharmacology, Propranolol pharmacology, Rats, Rats, Wistar, Autonomic Nervous System physiopathology, Hypertension physiopathology, Nitric Oxide Synthase antagonists & inhibitors, Physical Conditioning, Animal physiology
Abstract

Background: The nitric oxide (NO) synthesis blockade is characterized by an increase in the cardiac sympathetic activity and the physical training promotes the decrease in the sympathetic activity., Objective: We investigated the effect of the NO synthesis blockade on the autonomic cardiovascular control in rats submitted to aerobic exercises during a 10-week period., Methods: Male Wistar rats were divided in four groups: control rats, treated with chow food and water ad libitum for 10 weeks (CR); control rats, treated with N G-nitro-L-arginine methyl ester (L-NAME) during the last week (CRL); rats trained during 10 weeks on an electrical treadmill (TR); rats trained for 10 weeks and treated with L-NAME during the last week (TRL). The autonomic cardiovascular control was investigated in all groups with the use of a double blockade with methylatropine and propranolol and analysis of variability., Results: The CRL and TRL groups presented hypertension. The CRL group presented tachycardia and predominance of the sympathetic tonus in heat rate (HR) measurement after the pharmacological autonomic blockade. The TR group presented bradycardia and lower intrinsic HR when compared to the others. The evaluation of the HR variability showed lower absolute and normalized values in the low frequency (LF) band in the CRL group. On the other hand, the TRL presented an increase in the LF band in absolute values. The analysis of variability of the systemic arterial pressure (SAP) showed that the CRL and TRL groups presented higher values in the LF band., Conclusion: The previous physical exercise prevented the deficit in the autonomic cardiac control induced by the treatment with L-NAME, but did not prevent the increase in the SAP variability.

Published
2009
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47. Impact of arterial and arteriovenous renal clamping with and without intrarenal cooling on renal oxygenation and temperature in a porcine model.

Author

Schuler TD, Perks AE, Fazio LM, Blew BD, Mazer D, Hare G, D'A Honey RJ, and Pace KT

Subjects
Animals, Constriction, Models, Animal, Swine, Time Factors, Body Temperature, Hypothermia, Induced, Kidney physiology, Oxygen physiology, Renal Artery surgery, Renal Veins surgery
Abstract

Background: As laparoscopic partial nephrectomy increases in prominence, more needs to be understood about the combined effect of the pneumoperitoneum and renal ischemia during tumor resection. The purpose of this study is to investigate the effect of combined renal hilar clamping (arterial only versus arteriovenous) and retrograde intrarenal cooling on renal temperature and oxygenation in a porcine laparoscopic partial nephrectomy model., Materials and Methods: Under general anesthesia, laparoscopic access with intra-abdominal pressure of 15 mm Hg to the left renal hilum was obtained. Licox tissue oxygenation and temperature probes were placed into the kidney transcutaneously; measurements were taken every 30 seconds. After establishing baseline readings, either the artery alone (n=18) or the artery and vein (n=18) were clamped for 30, 60 or 90 minutes (n=12 each). During vascular clamping, retrograde, intrarenal cooling was performed with ice cold saline infused via a percutaneously placed ureteric catheter in 18 pigs. Changes in renal pO2 and temperature were analyzed with repeated measures ANCOVA in SPSS 16., Results: Retrograde cooling decreased renal parenchyma to 75.8% of baseline temperature (27.9 degrees C) within 15 minutes. There were no differences in cooling whether arterial or arteriovenous clamping was used (p=0.79). In uncooled animals, there was no significant difference in the decrease in renal pO2 during the clamp phase (p=0.18) or during the recovery phase (p=0.52). During the recovery phase, renal pO2 in uncooled animals was significantly higher than in those who received cooling (p=0.01). Animals who underwent hilar clamping for extended periods (60 and 90 min) had a slower recovery of renal pO2 to baseline than those with hilar clamping for 30 minutes (p=0.04), Conclusion: Retrograde intrarenal cooling can reliably cool the porcine kidney to 28 degrees C, regardless of whether arterial or arteriovenous clamping is used. Renal pO2 is not significantly different between animals that undergo artery only versus en bloc hilar clamping. Pigs that were provided with retrograde cooling had a slower return of pO2 to baseline following release of hilar clamps, possibly due to hypothermic vasospasm. Clamp durations greater than 60 minutes were also associated with slower return of renal oxygenation to baseline.

Published
2008
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48. Variability and predictability of large-volume red blood cell transfusion in cardiac surgery: a multicenter study.

Author

Karkouti K, Wijeysundera DN, Beattie WS, Callum JL, Cheng D, Dupuis JY, Kent B, Mazer D, Rubens FD, Sawchuk C, and Yau TM

Subjects
Aged, Female, Humans, Male, Middle Aged, Odds Ratio, Regression Analysis, Reproducibility of Results, Retrospective Studies, Blood Loss, Surgical statistics & numerical data, Cardiac Surgical Procedures methods, Erythrocyte Transfusion statistics & numerical data, Predictive Value of Tests
Abstract

Background: In cardiac surgery, excessive blood loss requiring large-volume red blood cell (RBC) transfusion is a common occurrence that is associated with significant morbidity and mortality. The objectives of this study were to measure the interinstitution variation and predictability of large-volume RBC transfusion., Study Design and Methods: Data were retrospectively collected on 3500 consecutive cardiac surgical patients at seven Canadian hospitals during 2004. The crude and risk-adjusted institutional odds ratios (ORs) for large-volume (>or=5 U) RBC transfusion were calculated with logistic regression. The predictive accuracy of an existing prediction rule for large-volume RBC transfusion was calculated for each institution., Results: Large-volume RBC transfusion occurred in 538 (15%) patients. When compared to the reference hospital (median crude rate), the institutional unadjusted and adjusted ORs for large-volume RBC transfusion ranged from 0.29 to 1.26 and 0.14 to 1.15, respectively (p<0.0001 for interinstitution variation). The variation was lower, but still considerable, for excessive blood loss, defined as at least 5-U RBC transfusion or reexploration; the ORs ranged from 0.42 to 1.22 (p<0.0001). The prediction rule performed well at most sites; its pooled positive predictive value for excessive blood loss was 71 percent (range, 63%-89%), and its negative predictive value was 90 percent (range, 87%-93%)., Conclusions: There is marked interinstitution variation in large-volume RBC transfusion in cardiac surgery that is not explained by patient- or surgery-related factors. Despite this variation, patients at high or low risk for large-volume RBC transfusion can be accurately identified by a prediction rule composed of readily available clinical variables.

Published
2007
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49. Hemolink, an o-raffinose cross-linked haemoglobin-based oxygen carrier, does not affect activation and function of human platelets in whole blood in vitro.

Author

Leytin V, Mazer D, Mody M, Garvey B, and Freedman J

Subjects
Blood Platelets physiology, Flow Cytometry, Hemostasis drug effects, Humans, In Vitro Techniques, Platelet Function Tests, Blood Platelets drug effects, Blood Substitutes pharmacology, Hemoglobins pharmacology, Platelet Activation drug effects, Raffinose analogs & derivatives, Raffinose pharmacology
Abstract

Haemoglobin-based oxygen carriers (HBOCs) are anticipated to be safe and efficient alternatives to RBC transfusions. Haemoglobin (Hb) raffimer (Hemolink; Hemosol, Toronto, ON, Canada) is polymerized human Hb, cross-linked with o-raffinose. As administration of cell-free Hb may affect blood cells and tissues, this study was focused on evaluating effects of Hb raffimer on human platelets in whole blood in vitro. Citrated blood from healthy donors was incubated with Hb raffimer to achieve raffimer concentrations of 2-50 vol percentage (2-50 g/l). Platelet activation, phosphatidylserine exposure and microparticle generation were measured by flow cytometry. Aperture closure time on collagen/ADP- and collagen/epinephrine-coated membranes was determined by a platelet function analyser (PFA-100). We found that addition of Hb raffimer to blood samples up to 50 vol % did not affect human platelets as measured by various markers of platelet activation (CD42b, CD41, PAC-1, CD62, CD63), procoagulant activity (annexin V) and microparticle formation; differences between Hb raffimer- and lactated Ringer's-diluted blood were not significant. Similarly, no adverse effect of Hb raffimer on closure time was observed at concentrations up to 50 vol %, in comparison with Ringer's solution. These data indicate that exposure of human blood to high concentrations of Hb raffimer in vitro did not cause platelet activation nor affect platelet function.

Published
2003
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50. Nutritional supplementation with MyoVive repletes essential cardiac myocyte nutrients and reduces left ventricular size in patients with left ventricular dysfunction.

Author

Jeejeebhoy F, Keith M, Freeman M, Barr A, McCall M, Kurian R, Mazer D, and Errett L

Subjects
Aged, Carnitine administration & dosage, Carnitine analysis, Coenzymes, Double-Blind Method, Female, Humans, Male, Middle Aged, Radionuclide Ventriculography methods, Taurine administration & dosage, Taurine analysis, Ubiquinone administration & dosage, Ubiquinone analysis, Ventricular Dysfunction, Left metabolism, Carnitine metabolism, Dietary Supplements, Heart Failure metabolism, Myocardium metabolism, Taurine metabolism, Ubiquinone analogs & derivatives, Ubiquinone metabolism, Ventricular Dysfunction, Left therapy
Abstract

Background: Congestive heart failure depletes the myocardium of carnitine, coenzyme Q10 (CoQ10), and taurine--substances known to influence mitochondrial function and cell calcium. We hypothesized that feeding patients a nutritional supplement that contained carnitine, CoQ10, and taurine would result in higher myocardial levels of these nutrients and improve left ventricular function., Methods: Forty-one patients who underwent aortocoronary artery bypass with an ejection fraction < or =40% at referral were randomly assigned to a double-blind trial of supplement or placebo. Radionuclide ventriculography was performed at randomization and before surgery. Surgical myocardial biopsies, adjusted for protein content, were analyzed for carnitine, CoQ10, and taurine levels., Results: The groups were well matched. Minor exceptions were supplement group versus placebo group for digoxin use (7 vs 0, respectively; P =.009) and age (62 +/- 11 years vs 69 +/- 5 years, respectively; P =.04). There were significantly higher levels in the treated group compared with the placebo group for myocardial levels of CoQ10 (138.17 +/- 39.87 nmol/g wet weight and 56.67 +/- 23.08 nmol/g wet weight; P =.0006), taurine (13.12 +/- 4.00 micromol/g wet weight and 7.91 +/- 2.81 micromol/g wet weight; P =.003), and carnitine (1735.4 +/- 798.5 nmol/g wet weight and 1237.6 +/- 343.1 nmol/g wet weight; P =.06). The left ventricular end-diastolic volume fell by -7.5 +/- 21.7 mL in the supplement group and increased by 10.0 +/- 19.8 mL in the placebo group (P =.037)., Conclusions: Supplementation results in higher myocardial CoQ10, taurine, and carnitine levels and is associated with a reduction in left ventricular end-diastolic volume in patients with left ventricular dysfunction before revascularization. Because the risk of death for surgical revascularization is related to preoperative left ventricular end-diastolic volume, supplementation could improve outcomes.

Published
2002
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