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2. Poster display IV experimental and instrumentation

Author

Masoli, O. Osvaldo, Redruello, M., Ogresta, F., Collaud, C., Koslowski, P., Baliño, N. Perez, Eleta, M., Arce, P., Vidal, L., Kardash, O., Maroz-Vadalajskaya, N. Natalia, Vanhove, C. Christian, Lahoutte, T., Defrise, M., Andreyev, A., Bossuyt, A., Franken, P. R., Franken, P. R. Philippe, Lahoutte, T., Maskali, F., Vanhove, C., Nloga, J., Tran, N., Marie, P. Y., Peix, A. Amalia, Garcia-Barreto, D., Ponce, F., Cabrera, L. O., Valiente, J., Tornes, F., Guerrero, I., Heres, F., Garcia, E. J., Cabale, B., Bindslev, L. Lene, Bisgaard, K. B. Kirsten, Haack-Soerensen, M. H. S. Mandana, Mortensen, S. M. Steen, Kragh, L. K. Linda, Kjaer, A. K. Andreas, Kastrup, J. K. Jens, Hesse, B. H. Birger, Aboul-Enein, F. Fatma, Battah, A., Fattah, A. Abdel, Atty, A. Abdel, Allam, A., Riou, L. Laurent, Broisat, A., Ghezzi, C., Lartizien, C., Berthonneche, C., Toufektsian, M. C., Maitrejean, S., Janier, M., Vanzetto, G., Fagret, D., Rouzet, F. Francois, Daou, D., Lebtahi, R., Frank, R., Leenhardt, A., Slama, M., Guludec, D. Le, Sarda-Mantel, L. Laure, Michel, J. B., Rouzet, F., Martet, G., Meulemans, A., Vrigneaud, J. M., Guludec, D. Le, Daou, D. Doumit, Coaguila, C., Benada, A., Razzouk, M., Idy-Peretti, I., Guludec, D. Le, Vilain, D., Lebtahi, R., Guludec, D. Le, Stegger, L. Lars, Schäfers, K., Flögel, U., Schrader, J., Schober, O., Levkau, B., Schäfers, M., Kies, P. Peter, Wichter, T., Schäfers, K. P., Schäfers, M., Wielepp, J. P. Peter, Baller, D., Pulawski, E., Weise, R., Fricke, E., Horstkotte, D., Burchert, W., Eckert, S., Dongas, A., Horstkotte, D., Burchert, W., Nekolla, S. G. Stephan, Martinez, M. J., Howe, W., Kehren, F., Ziegler, S. I., Vassiliadis, I. Ioannis, Souretis, G., Komporozos, C., Fountos, A., Papademetriou, A., Spanos, A., Antoniou, A., Strembelas, P., Moralidis, E. Efstratios, Arsos, G., Boundas, D., Georga, S., Karatzas, N., Karakatsanis, K., Prassopoulos, V. Vassilios, Parthenakis, F., Patrianakos, A., Koukouraki, S., Velidaki, A., Karkavitsas, N., Vardas, P., Velidaki, A. Antigone, Perisinakis, K., Koukouraki, S., Koutsikos, J., Prassopoulos, V., Vardas, P., Karkavitsas, N., Sundaraiya, S. Sumati, Sumati, S., Sambhasivam, KA., David, S., Zakavi, S. R. Seyed Rasoul, Kakhki, V. R. Dabagh, Jabari, H., Zingerman, B., Bendayan, D., Sagie, A., Solodky, A., Mats, I., Shapira, Y., Kremer, M. R., Zafrir, N. Nili, Rimini, M. L. Maria Luisa De, Catalano, M., Bonzani, G., Scalzone, A., Merenda, R., Monteforte, I., Monda, V., Muto, P., Carboni, G. P. Gian Piero, Miglionico, M., Tavolozza, M., Marcassa, C. Claudio, Campini, R., Calza, P., Giannuzzi, P., Eleuteri, E., Marcassa, C. Claudio, Campini, R., Scapellato, F., Temporelli, P. L., Giannuzzi, P., Pellegrino, T., Storto, G., Sorrentino, A. R., Silvestri, A., Filardi, P. Perrone, Brevetti, G., Cuocolo, A. Alberto, Cho, K. Keiichi, Kumita, S., Seino, K., Nakajo, H., Toba, M., Kumazaki, T., Muramatsu, T. Toshihiro, Yamazaki, T., Seki, K., Kawanami, J., Nakajima, T., Yamada, Y., Suga, T., Matsumoto, K., Nishimura, S., Taki, J. Junichi, Higuchi, T., Kawashima, A., Nakajima, K., Muramori, A., Matsunari, I., Tait, J. F., Vanderheyden, J. L., Strauss, H. W., Tonami, N., Adachi, I. Itaru, Shimomura, H., Kintaka, T., Komori, T., Ogura, Y., Kitaura, Y., Narabayashi, I., Iida, H. Hidehiro, Zeniya, T., Kim, K. M., Watabe, H., Teramoto, N., Yamamichi, Y., Alexanderson, E. Erick, Ricalde, A., Vargas, A., Meave, A., Amigo, M. C., Misko, J., Dziuk, M. Miroslaw, Warczynska, A., Skrobowska, E., Vasconcelos, M. Mariana, Martins, E., Faria, T., Oliveira, A., Pardal, N., Macedo, F., Pereira, J., Rocha-Gonçalves, F., Cantinho, G. Guilhermina, Pena, H., Freire, L., Veiga, A., Gonçalves, P., Godinho, F., Chua, T. Terrance, Lee, C. Y., Keng, F., Ding, Z. P., Koh, T. H., Awamleh, P. Paula, Talavera, P., Torres, V., Balsa, M. A., González, O., Alberca, M. T., Miguel, R., Cosío, F. G., Lomsky, M. Milan, Richter, J., Johansson, L., El-Ali, H., Åström, K., Ljungberg, M., Edenbrandt, L., Hung, G. U. Guang-Uei, Lee, K. W., Chen, C. P., Yang, K. T., Pekindil, G., Sarikaya, A. Ali, Ege, T., Salihoglu, S., Entok, E. Emre, Cavusoglu, Y., Ak, I., Vardareli, E., Timuralp, B., Tout, D. Deborah, Loong, C. Y., Naidoo, V. V., Aswegen, A. Van, Underwood, S. R., Thorley, P. J. Penelope, Goris, M. Michael, ZHU, H. J., Clements, I. P. Ian, Mullan, B. P., O’Connor, M. K., Breen, J. F., McGregor, C. G. A., Liu, Y. H. Yi-Hwa, Li, S., Bourke, B., Weyman, C., Sinusas, A. J., Ramakrishna, G. Gautam, Miller, T. D., O’Connor, M. K., Gibbons, R. J., Tsatkin, V., Wackers, F. J. T. H., Liu, Y. H. Yi-Hwa, Tsatkin, V., Prior, J. O. John, Facta, A. D., Schindler, T. H., Oxilia-Estigarribia, M. A., Hernandez-Pampaloni, M., Campisi, R., Zhang, X., Bischof-Delaloye, A., Nathan, L., Schelbert, H. R., Gullberg, G. T. Grant, Huesman, R. H., Reutter, B. W., Sitek, A., Veress, A. I., Weiss, J. A., Qi, J., Yang, Y., Gordi, T. Toufigh, Olmsted, A., Lieu, H., and Belardinelli, L.

Published
2005
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5. Cardiac manifestations of inherited metabolic disease linked to cellular vitamin B12 uptake: Study in murine model of invalidation of Mtr gene in the heart

Author

Jepchumba Kosgei, Viola, Elkhafifi, F., Lacolley, Patrick, Umoret, R., Maskali, F., Guéant, J.L., Guéant-Rodriguez, R., Nutrition-Génétique et Exposition aux Risques Environnementaux (NGERE), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lorraine (UL), Défaillance Cardiovasculaire Aiguë et Chronique (DCAC), Centre Hospitalier Régional Universitaire de Nancy (CHRU Nancy)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lorraine (UL), Nancyclotep- Experimental Imaging Platform = Plate-forme d'imagerie moléculaire, Faculté de Médecine [Nancy], and Université de Lorraine (UL)

Subjects
[SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], 030204 cardiovascular system & hematology, [SDV.BIBS]Life Sciences [q-bio]/Quantitative Methods [q-bio.QM], 3. Good health, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biomolecules [q-bio.BM], 03 medical and health sciences, 0302 clinical medicine, [SDV.BBM.GTP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Genomics [q-bio.GN], [SDV.MHEP.PHY]Life Sciences [q-bio]/Human health and pathology/Tissues and Organs [q-bio.TO], 030212 general & internal medicine, [INFO.INFO-BI]Computer Science [cs]/Bioinformatics [q-bio.QM], Cardiology and Cardiovascular Medicine, [SDV.AEN]Life Sciences [q-bio]/Food and Nutrition, ComputingMilieux_MISCELLANEOUS
Abstract

International audience

Published
2019
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7. Poster display IV experimental and instrumentation

Author

Masoli, O., Redruello, M., Ogresta, F., Collaud, C., Koslowski, P., Baliño, N., Eleta, M., Arce, P., Vidal, L., Kardash, O., Maroz-Vadalajskaya, N., Vanhove, C., Lahoutte, T., Defrise, M., Andreyev, A., Bossuyt, A., Franken, P., Maskali, F., Nloga, J., Tran, N., Marie, P., Peix, A., Garcia-Barreto, D., Ponce, F., Cabrera, L., Valiente, J., Tornes, F., Guerrero, I., Heres, F., Garcia, E., Cabale, B., Bindslev, L., Bisgaard, K., Haack-Soerensen, M., Mortensen, S., Kragh, L., Kjaer, A., Kastrup, J., Hesse, B., Aboul-Enein, F., Battah, A., Fattah, A., Atty, A., Allam, A., Riou, L., Broisat, A., Ghezzi, C., Lartizien, C., Berthonneche, C., Toufektsian, M., Maitrejean, S., Janier, M., Vanzetto, G., Fagret, D., Rouzet, F., Daou, D., Lebtahi, R., Frank, R., Leenhardt, A., Slama, M., Guludec, D., Sarda-Mantel, L., Michel, J., Martet, G., Meulemans, A., Vrigneaud, J., Coaguila, C., Benada, A., Razzouk, M., Idy-Peretti, I., Vilain, D., Stegger, L., Schäfers, K., Flögel, U., Schrader, J., Schober, O., Levkau, B., Schäfers, M., Kies, P., Wichter, T., Wielepp, J., Baller, D., Pulawski, E., Weise, R., Fricke, E., Horstkotte, D., Burchert, W., Eckert, S., Dongas, A., Nekolla, S., Martinez, M., Howe, W., Kehren, F., Ziegler, S., Vassiliadis, I., Souretis, G., Komporozos, C., Fountos, A., Papademetriou, A., Spanos, A., Antoniou, A., Strembelas, P., Moralidis, E., Arsos, G., Boundas, D., Georga, S., Karatzas, N., Karakatsanis, K., Prassopoulos, V., Parthenakis, F., Patrianakos, A., Koukouraki, S., Velidaki, A., Karkavitsas, N., Vardas, P., Perisinakis, K., Koutsikos, J., Sundaraiya, S., Sumati, S., Sambhasivam, KA, David, S., Zakavi, S., Kakhki, V., Jabari, H., Zingerman, B., Bendayan, D., Sagie, A., Solodky, A., Mats, I., Shapira, Y., Kremer, M., Zafrir, N., Rimini, M., Catalano, M., Bonzani, G., Scalzone, A., Merenda, R., Monteforte, I., Monda, V., Muto, P., Carboni, G., Miglionico, M., Tavolozza, M., Marcassa, C., Campini, R., Calza, P., Giannuzzi, P., Eleuteri, E., Scapellato, F., Temporelli, P., Pellegrino, T., Storto, G., Sorrentino, A., Silvestri, A., Filardi, P., Brevetti, G., Cuocolo, A., Cho, K., Kumita, S., Seino, K., Nakajo, H., Toba, M., Kumazaki, T., Muramatsu, T., Yamazaki, T., Seki, K., Kawanami, J., Nakajima, T., Yamada, Y., Suga, T., Matsumoto, K., Nishimura, S., Taki, J., Higuchi, T., Kawashima, A., Nakajima, K., Muramori, A., Matsunari, I., Tait, J., Vanderheyden, J., Strauss, H., Tonami, N., Adachi, I., Shimomura, H., Kintaka, T., Komori, T., Ogura, Y., Kitaura, Y., Narabayashi, I., Iida, H., Zeniya, T., Kim, K., Watabe, H., Teramoto, N., Yamamichi, Y., Alexanderson, E., Ricalde, A., Vargas, A., Meave, A., Amigo, M., Misko, J., Dziuk, M., Warczynska, A., Skrobowska, E., Vasconcelos, M., Martins, E., Faria, T., Oliveira, A., Pardal, N., Macedo, F., Pereira, J., Rocha-Gonçalves, F., Cantinho, G., Pena, H., Freire, L., Veiga, A., Gonçalves, P., Godinho, F., Chua, T., Lee, C., Keng, F., Ding, Z., Koh, T., Awamleh, P., Talavera, P., Torres, V., Balsa, M., González, O., Alberca, M., Miguel, R., Cosío, F., Lomsky, M., Richter, J., Johansson, L., El-Ali, H., Åström, K., Ljungberg, M., Edenbrandt, L., Hung, G., Lee, K., Chen, C., Yang, K., Pekindil, G., Sarikaya, A., Ege, T., Salihoglu, S., Entok, E., Cavusoglu, Y., Ak, I., Vardareli, E., Timuralp, B., Tout, D., Loong, C., Naidoo, V., Aswegen, A., Underwood, S., Thorley, P., Goris, M., ZHU, H., Clements, I., Mullan, B., O'Connor, M., Breen, J., McGregor, C., Liu, Y., Li, S., Bourke, B., Weyman, C., Sinusas, A., Ramakrishna, G., Miller, T., Gibbons, R., Tsatkin, V., Wackers, F., Prior, J., Facta, A., Schindler, T., Oxilia-Estigarribia, M., Hernandez-Pampaloni, M., Campisi, R., Zhang, X., Bischof-Delaloye, A., Nathan, L., Schelbert, H., Gullberg, G., Huesman, R., Reutter, B., Sitek, A., Veress, A., Weiss, J., Qi, J., Yang, Y., Gordi, T., Olmsted, A., Lieu, H., Belardinelli, L., Masoli, O., Redruello, M., Ogresta, F., Collaud, C., Koslowski, P., Baliño, N., Eleta, M., Arce, P., Vidal, L., Kardash, O., Maroz-Vadalajskaya, N., Vanhove, C., Lahoutte, T., Defrise, M., Andreyev, A., Bossuyt, A., Franken, P., Maskali, F., Nloga, J., Tran, N., Marie, P., Peix, A., Garcia-Barreto, D., Ponce, F., Cabrera, L., Valiente, J., Tornes, F., Guerrero, I., Heres, F., Garcia, E., Cabale, B., Bindslev, L., Bisgaard, K., Haack-Soerensen, M., Mortensen, S., Kragh, L., Kjaer, A., Kastrup, J., Hesse, B., Aboul-Enein, F., Battah, A., Fattah, A., Atty, A., Allam, A., Riou, L., Broisat, A., Ghezzi, C., Lartizien, C., Berthonneche, C., Toufektsian, M., Maitrejean, S., Janier, M., Vanzetto, G., Fagret, D., Rouzet, F., Daou, D., Lebtahi, R., Frank, R., Leenhardt, A., Slama, M., Guludec, D., Sarda-Mantel, L., Michel, J., Martet, G., Meulemans, A., Vrigneaud, J., Coaguila, C., Benada, A., Razzouk, M., Idy-Peretti, I., Vilain, D., Stegger, L., Schäfers, K., Flögel, U., Schrader, J., Schober, O., Levkau, B., Schäfers, M., Kies, P., Wichter, T., Wielepp, J., Baller, D., Pulawski, E., Weise, R., Fricke, E., Horstkotte, D., Burchert, W., Eckert, S., Dongas, A., Nekolla, S., Martinez, M., Howe, W., Kehren, F., Ziegler, S., Vassiliadis, I., Souretis, G., Komporozos, C., Fountos, A., Papademetriou, A., Spanos, A., Antoniou, A., Strembelas, P., Moralidis, E., Arsos, G., Boundas, D., Georga, S., Karatzas, N., Karakatsanis, K., Prassopoulos, V., Parthenakis, F., Patrianakos, A., Koukouraki, S., Velidaki, A., Karkavitsas, N., Vardas, P., Perisinakis, K., Koutsikos, J., Sundaraiya, S., Sumati, S., Sambhasivam, KA, David, S., Zakavi, S., Kakhki, V., Jabari, H., Zingerman, B., Bendayan, D., Sagie, A., Solodky, A., Mats, I., Shapira, Y., Kremer, M., Zafrir, N., Rimini, M., Catalano, M., Bonzani, G., Scalzone, A., Merenda, R., Monteforte, I., Monda, V., Muto, P., Carboni, G., Miglionico, M., Tavolozza, M., Marcassa, C., Campini, R., Calza, P., Giannuzzi, P., Eleuteri, E., Scapellato, F., Temporelli, P., Pellegrino, T., Storto, G., Sorrentino, A., Silvestri, A., Filardi, P., Brevetti, G., Cuocolo, A., Cho, K., Kumita, S., Seino, K., Nakajo, H., Toba, M., Kumazaki, T., Muramatsu, T., Yamazaki, T., Seki, K., Kawanami, J., Nakajima, T., Yamada, Y., Suga, T., Matsumoto, K., Nishimura, S., Taki, J., Higuchi, T., Kawashima, A., Nakajima, K., Muramori, A., Matsunari, I., Tait, J., Vanderheyden, J., Strauss, H., Tonami, N., Adachi, I., Shimomura, H., Kintaka, T., Komori, T., Ogura, Y., Kitaura, Y., Narabayashi, I., Iida, H., Zeniya, T., Kim, K., Watabe, H., Teramoto, N., Yamamichi, Y., Alexanderson, E., Ricalde, A., Vargas, A., Meave, A., Amigo, M., Misko, J., Dziuk, M., Warczynska, A., Skrobowska, E., Vasconcelos, M., Martins, E., Faria, T., Oliveira, A., Pardal, N., Macedo, F., Pereira, J., Rocha-Gonçalves, F., Cantinho, G., Pena, H., Freire, L., Veiga, A., Gonçalves, P., Godinho, F., Chua, T., Lee, C., Keng, F., Ding, Z., Koh, T., Awamleh, P., Talavera, P., Torres, V., Balsa, M., González, O., Alberca, M., Miguel, R., Cosío, F., Lomsky, M., Richter, J., Johansson, L., El-Ali, H., Åström, K., Ljungberg, M., Edenbrandt, L., Hung, G., Lee, K., Chen, C., Yang, K., Pekindil, G., Sarikaya, A., Ege, T., Salihoglu, S., Entok, E., Cavusoglu, Y., Ak, I., Vardareli, E., Timuralp, B., Tout, D., Loong, C., Naidoo, V., Aswegen, A., Underwood, S., Thorley, P., Goris, M., ZHU, H., Clements, I., Mullan, B., O'Connor, M., Breen, J., McGregor, C., Liu, Y., Li, S., Bourke, B., Weyman, C., Sinusas, A., Ramakrishna, G., Miller, T., Gibbons, R., Tsatkin, V., Wackers, F., Prior, J., Facta, A., Schindler, T., Oxilia-Estigarribia, M., Hernandez-Pampaloni, M., Campisi, R., Zhang, X., Bischof-Delaloye, A., Nathan, L., Schelbert, H., Gullberg, G., Huesman, R., Reutter, B., Sitek, A., Veress, A., Weiss, J., Qi, J., Yang, Y., Gordi, T., Olmsted, A., Lieu, H., and Belardinelli, L.

Published
2018

13. Intramyocardial implantation of bone marrow-derived stem cells enhances perfusion in chronic myocardial infarction: Dependency on initial perfusion depth and follow-up assessed by gated pinhole SPECT

Author

Tran, N., Franken, Philippe, Maskali, F., Vanhove, C., Marie, P.y., Nuclear Medicine, and Medical Imaging and Physical Sciences

Subjects
myocardial infarction, bone marrow, stem cell therapy, pinhole SPECT, RATS
Abstract

Cell therapy-induced changes in the perfusion of areas of myocardial infarction (MI) remain unclear. This study investigated whether an original pinhole SPECT technique could be applied to a rat Ml model to analyze local improvement in myocardial perfusion relating to engraftment sites of bone marrow-derived stem cells (BMSCs). Methods: Four-month-old MI rats were either untreated (n = 8) or treated (n = 10) by intramyocardial injection of (111)in-labeled BMSCs. Early distribution of In-111-BMSCs within the MI target was evidenced by dual In-111/Tc-99m pinhole SPECT 48 h later. Myocardial perfusion was serially monitored by Tc-99m-sestamibi pinhole gated SPECT up to 3 mo after transplantation. Results: Forty-eight hours after transplantation, In-111-BMSCs were observed in all treated rats and in 18 of their 32 underperfused MI segments (

Published
2007

14. Effect of mesenchymal stem cells on myocardial perfusion and function in a rat model of chronic infarction

Author

Philippe Franken, Maskali, F., Tony Lahoutte, Christian Van Hove, Tran, N., Marie, P. Y., Nuclear Medicine, and Medical Imaging and Physical Sciences

Subjects
rat model, infarction, Stem cells, mesenchypmal, myocardial imaging
Abstract

Background: Despite encouraging preliminar y results of cell-based therapies in patients with ischemic hear t disease there is still a need to develop animal models where abnormalities of myocardial perfusion and left ventricular function can be quantified precisely and followed on a long term basis. Pinhole gated SPECT allows rapid, reproducible and repeatable measurements of myocardial perfusion and function in rats. Aim: To evaluate the effect of bone marrow mesenchymal stem cells (BMSCs) transplantation on myocardial perfusion and function in a rat model of chronic infarction. Methods: 111Indium-oxine labeled autologous BMSCs were injected within the infarct area in 11 male Wistar rats 3 months after the surgical ligature of the left anterior descending coronar y ar ter y. One animal died during the transplantation. The distribution of the implanted cells was determined by dual isotope (111InThe distribution of the implanted cells was determined by dual isotope (111In and 99mTc-sestamibi) pinhole SPECT performed 2 days later. Myocardial perfusion and left ventricular function were calculated by 99mTc-sestamibi pinhole gated SPECT obtained before, and 1 and 3 months after cell transplantation. Polar maps of myocardial perfusion were generated. Perfusion abnormalities with values below 2 SD of a normal database were defined as infarct areas. Left ventricular volumes and ejection fraction were quantified from the gated data using an automatic program (Univ. of Michigan). Results: Transplanted cells were clearly visualized within the infarct area in all animals. Perfusion defect size ranged from 3 to 47% of the left ventricular surface before transplantation. Perfusion normalized in 1 animal, improved in 3 and was unchanged or deteriorated in the remaining 7 animals. No significant changes in left ventricular volumes and ejection fraction were observed except in the animal in whom perfusion was normalized. Conclusion: Pinhole (gated) SPECT is useful to assess the intra-myocardial distribution of transplanted cells and to monitor the effects of cell-based therapies in rats.

Published
2005

23. Poster session 2

Author

Perez-Pomares, J. M., primary, Ruiz-Villalba, A., additional, Ziogas, A., additional, Segovia, J. C., additional, Ehrbar, M., additional, Munoz-Chapuli, R., additional, De La Rosa, A., additional, Dominguez, J. N., additional, Hove-Madsen, L., additional, Sankova, B., additional, Sedmera, D., additional, Franco, D., additional, Aranega Jimenez, A., additional, Babaeva, G., additional, Chizh, N., additional, Galchenko, S., additional, Sandomirsky, B., additional, Schwarzl, M., additional, Seiler, S., additional, Steendijk, P., additional, Huber, S., additional, Maechler, H., additional, Truschnig-Wilders, M., additional, Pieske, B., additional, Post, H., additional, Simrick, S., additional, Kreutzer, R., additional, Rao, C., additional, Terracciano, C. M., additional, Kirchhof, P., additional, Fabritz, L., additional, Brand, T., additional, Theveniau-Ruissy, M., additional, Parisot, P., additional, Francou, A., additional, Saint-Michel, E., additional, Mesbah, K., additional, Kelly, R. G., additional, Wu, H.-T., additional, Sie, S.-S., additional, Chen, C.-Y., additional, Kuan, T.-C., additional, Lin, C. S., additional, Ismailoglu, Z., additional, Guven, M., additional, Yakici, A., additional, Ata, Y., additional, Ozcan, S., additional, Yildirim, E., additional, Ongen, Z., additional, Miroshnikova, V., additional, Demina, E., additional, Rodygina, T., additional, Kurjanov, P., additional, Denisenko, A., additional, Schwarzman, A., additional, Rubanenko, A., additional, Shchukin, Y., additional, Germanov, A., additional, Goldbergova, M., additional, Parenica, J., additional, Lipkova, J., additional, Pavek, N., additional, Kala, P., additional, Poloczek, M., additional, Vasku, A., additional, Parenicova, I., additional, Spinar, J., additional, Gambacciani, C., additional, Chiavacci, E., additional, Evangelista, M., additional, Vesentini, N., additional, Kusmic, C., additional, Pitto, L., additional, Chernova, A., additional, Nikulina, S. U. Y., additional, Arvanitis, D. A., additional, Mourouzis, I., additional, Pantos, C., additional, Kranias, E. G., additional, Cokkinos, D. V., additional, Sanoudou, D., additional, Vladimirskaya, T. E., additional, Shved, I. A., additional, Kryvorot, S. G., additional, Schirmer, I. M., additional, Appukuttan, A., additional, Pott, L., additional, Jaquet, K., additional, Ladilov, Y., additional, Archer, C. R., additional, Bootman, M. D., additional, Roderick, H. L., additional, Fusco, A., additional, Sorriento, D., additional, Santulli, G., additional, Trimarco, B., additional, Iaccarino, G., additional, Hagenmueller, M., additional, Riffel, J., additional, Bernhold, E., additional, Katus, H. A., additional, Hardt, S. 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Published
2012
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29. In vivo location of intramyocardial implanted 111In-oxine labeled mesenchymal stem cells: Assessement with dual energy pinhole 99mTc-Sestamibi SPECT in a rat model of myocardial infarction

Author

Tran, N., primary, Maskali, F., additional, Franken, P., additional, Nloga, J., additional, Lahoutte, T., additional, Maureira, P., additional, Li, Y., additional, Marie, P.Y., additional, Karcher, G., additional, Stoltz, J.F., additional, and Villemot, J.P., additional

Published
2005
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30. Acipimox-enhanced ¹⁸F-fluorodeoxyglucose positron emission tomography for characterizing and predicting early remodeling in the rat infarct model.

Author

Bousquenaud M, Maskali F, Poussier S, Marie PY, Boutley H, Karcher G, Wagner DR, Devaux Y, Bousquenaud, Mélanie, Maskali, Fatiha, Poussier, Sylvain, Marie, Pierre-Yves, Boutley, Henri, Karcher, Gilles, Wagner, Daniel R, and Devaux, Yvan

Abstract

The rat myocardial infarction (MI) model is widely used to study left ventricular (LV) remodeling. In this study, acipimox-enhanced (18)F-Fluorodeoxyglucose (FDG) gated-positron emission tomography (PET) was assessed for characterizing and predicting early remodeling in the rat infarct model. Nineteen Wistar rats had surgical occlusion of the left anterior descending coronary artery and 7 were sham-operated. PET was scheduled 48 h and 2 weeks later for quantifying MI area and LV function. Segments with <50% of FDG uptake had histological evidence of MI (74 ± 9% decrease in parietal thickness, fibrosis development). At 48 h, MI area was large (>35% of LV) in 6 rats, moderate (15-35% of LV) in 8 rats, limited (<15% of LV) in 5 rats and absent in the 7 sham rats. LV remodeling, assessed through the 2 weeks increase in end-diastolic volume, increased between rats with limited, moderate and large MI (+72 ± 25, +109 ± 56, +190 ± 69 μl, respectively, P = 0.007). This 3-groups classification allowed predicting 44% of the 2 weeks increase in end-diastolic volume, and additional 34% were predicted by heart rate at 48 h. The acipimox-enhanced FDG gated-PET technique provides efficient characterization and prediction of early remodeling in the rat infarct model. [ABSTRACT FROM AUTHOR]

Published
2012
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33. 18F-Fluoride PET for quantification of axial and peripheral lesions in adjuvant-induced arthritis in Lewis rats

Author

Ouichka, R., Derrien, A., Henrionnet, C., Maskali, F., Karcher, G., Pierre GILLET, Damien Loeuille, Astrid Pinzano, Université de Lorraine (UL), Nancyclotep- Experimental Imaging Platform = Plate-forme d'imagerie moléculaire, Centre Hospitalier Régional Universitaire de Nancy (CHRU Nancy)-Université de Lorraine (UL), Ingénierie Moléculaire et Physiopathologie Articulaire (IMoPA), Université de Lorraine (UL)-Centre National de la Recherche Scientifique (CNRS), and Centre Hospitalier Régional Universitaire de Nancy (CHRU Nancy)

Subjects
[SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology
Abstract

Résumé; International audience

34. Poster display IV experimental and instrumentation

Author

Masoli, O., Redruello, M., Ogresta, F., Collaud, C., Koslowski, P., Baliño, N., Eleta, M., Arce, P., Vidal, L., Kardash, O., Maroz-Vadalajskaya, N., Vanhove, C., Lahoutte, T., Defrise, M., Andreyev, A., Bossuyt, A., Franken, P., Maskali, F., Nloga, J., Tran, N., Marie, P., Peix, A., Garcia-Barreto, D., Ponce, F., Cabrera, L., Valiente, J., Tornes, F., Guerrero, I., Heres, F., Garcia, E., Cabale, B., Bindslev, L., Bisgaard, K., Haack-Soerensen, M., Mortensen, S., Kragh, L., Kjaer, A., Kastrup, J., Hesse, B., Aboul-Enein, F., Battah, A., Fattah, A., Atty, A., Allam, A., Riou, L., Broisat, A., Ghezzi, C., Lartizien, C., Berthonneche, C., Toufektsian, M., Maitrejean, S., Janier, M., Vanzetto, G., Fagret, D., Rouzet, F., Daou, D., Lebtahi, R., Frank, R., Leenhardt, A., Slama, M., Guludec, D., Sarda-Mantel, L., Michel, J., Martet, G., Meulemans, A., Vrigneaud, J., Coaguila, C., Benada, A., Razzouk, M., Idy-Peretti, I., Vilain, D., Stegger, L., Schäfers, K., Flögel, U., Schrader, J., Schober, O., Levkau, B., Schäfers, M., Kies, P., Wichter, T., Wielepp, J., Baller, D., Pulawski, E., Weise, R., Fricke, E., Horstkotte, D., Burchert, W., Eckert, S., Dongas, A., Nekolla, S., Martinez, M., Howe, W., Kehren, F., Ziegler, S., Vassiliadis, I., Souretis, G., Komporozos, C., Fountos, A., Papademetriou, A., Spanos, A., Antoniou, A., Strembelas, P., Moralidis, E., Arsos, G., Boundas, D., Georga, S., Karatzas, N., Karakatsanis, K., Prassopoulos, V., Parthenakis, F., Patrianakos, A., Koukouraki, S., Velidaki, A., Karkavitsas, N., Vardas, P., Perisinakis, K., Koutsikos, J., Sundaraiya, S., Sumati, S., Sambhasivam, KA, David, S., Zakavi, S., Kakhki, V., Jabari, H., Zingerman, B., Bendayan, D., Sagie, A., Solodky, A., Mats, I., Shapira, Y., Kremer, M., Zafrir, N., Rimini, M., Catalano, M., Bonzani, G., Scalzone, A., Merenda, R., Monteforte, I., Monda, V., Muto, P., Carboni, G., Miglionico, M., Tavolozza, M., Marcassa, C., Campini, R., Calza, P., Giannuzzi, P., Eleuteri, E., Scapellato, F., Temporelli, P., Pellegrino, T., Storto, G., Sorrentino, A., Silvestri, A., Filardi, P., Brevetti, G., Cuocolo, A., Cho, K., Kumita, S., Seino, K., Nakajo, H., Toba, M., Kumazaki, T., Muramatsu, T., Yamazaki, T., Seki, K., Kawanami, J., Nakajima, T., Yamada, Y., Suga, T., Matsumoto, K., Nishimura, S., Taki, J., Higuchi, T., Kawashima, A., Nakajima, K., Muramori, A., Matsunari, I., Tait, J., Vanderheyden, J., Strauss, H., Tonami, N., Adachi, I., Shimomura, H., Kintaka, T., Komori, T., Ogura, Y., Kitaura, Y., Narabayashi, I., Iida, H., Zeniya, T., Kim, K., Watabe, H., Teramoto, N., Yamamichi, Y., Alexanderson, E., Ricalde, A., Vargas, A., Meave, A., Amigo, M., Misko, J., Dziuk, M., Warczynska, A., Skrobowska, E., Vasconcelos, M., Martins, E., Faria, T., Oliveira, A., Pardal, N., Macedo, F., Pereira, J., Rocha-Gonçalves, F., Cantinho, G., Pena, H., Freire, L., Veiga, A., Gonçalves, P., Godinho, F., Chua, T., Lee, C., Keng, F., Ding, Z., Koh, T., Awamleh, P., Talavera, P., Torres, V., Balsa, M., González, O., Alberca, M., Miguel, R., Cosío, F., Lomsky, M., Richter, J., Johansson, L., El-Ali, H., Åström, K., Ljungberg, M., Edenbrandt, L., Hung, G., Lee, K., Chen, C., Yang, K., Pekindil, G., Sarikaya, A., Ege, T., Salihoglu, S., Entok, E., Cavusoglu, Y., Ak, I., Vardareli, E., Timuralp, B., Tout, D., Loong, C., Naidoo, V., Aswegen, A., Underwood, S., Thorley, P., Goris, M., ZHU, H., Clements, I., Mullan, B., O'Connor, M., Breen, J., McGregor, C., Liu, Y., Li, S., Bourke, B., Weyman, C., Sinusas, A., Ramakrishna, G., Miller, T., Gibbons, R., Tsatkin, V., Wackers, F., Prior, J., Facta, A., Schindler, T., Oxilia-Estigarribia, M., Hernandez-Pampaloni, M., Campisi, R., Zhang, X., Bischof-Delaloye, A., Nathan, L., Schelbert, H., Gullberg, G., Huesman, R., Reutter, B., Sitek, A., Veress, A., Weiss, J., Qi, J., Yang, Y., Gordi, T., Olmsted, A., Lieu, H., Belardinelli, L., Masoli, O., Redruello, M., Ogresta, F., Collaud, C., Koslowski, P., Baliño, N., Eleta, M., Arce, P., Vidal, L., Kardash, O., Maroz-Vadalajskaya, N., Vanhove, C., Lahoutte, T., Defrise, M., Andreyev, A., Bossuyt, A., Franken, P., Maskali, F., Nloga, J., Tran, N., Marie, P., Peix, A., Garcia-Barreto, D., Ponce, F., Cabrera, L., Valiente, J., Tornes, F., Guerrero, I., Heres, F., Garcia, E., Cabale, B., Bindslev, L., Bisgaard, K., Haack-Soerensen, M., Mortensen, S., Kragh, L., Kjaer, A., Kastrup, J., Hesse, B., Aboul-Enein, F., Battah, A., Fattah, A., Atty, A., Allam, A., Riou, L., Broisat, A., Ghezzi, C., Lartizien, C., Berthonneche, C., Toufektsian, M., Maitrejean, S., Janier, M., Vanzetto, G., Fagret, D., Rouzet, F., Daou, D., Lebtahi, R., Frank, R., Leenhardt, A., Slama, M., Guludec, D., Sarda-Mantel, L., Michel, J., Martet, G., Meulemans, A., Vrigneaud, J., Coaguila, C., Benada, A., Razzouk, M., Idy-Peretti, I., Vilain, D., Stegger, L., Schäfers, K., Flögel, U., Schrader, J., Schober, O., Levkau, B., Schäfers, M., Kies, P., Wichter, T., Wielepp, J., Baller, D., Pulawski, E., Weise, R., Fricke, E., Horstkotte, D., Burchert, W., Eckert, S., Dongas, A., Nekolla, S., Martinez, M., Howe, W., Kehren, F., Ziegler, S., Vassiliadis, I., Souretis, G., Komporozos, C., Fountos, A., Papademetriou, A., Spanos, A., Antoniou, A., Strembelas, P., Moralidis, E., Arsos, G., Boundas, D., Georga, S., Karatzas, N., Karakatsanis, K., Prassopoulos, V., Parthenakis, F., Patrianakos, A., Koukouraki, S., Velidaki, A., Karkavitsas, N., Vardas, P., Perisinakis, K., Koutsikos, J., Sundaraiya, S., Sumati, S., Sambhasivam, KA, David, S., Zakavi, S., Kakhki, V., Jabari, H., Zingerman, B., Bendayan, D., Sagie, A., Solodky, A., Mats, I., Shapira, Y., Kremer, M., Zafrir, N., Rimini, M., Catalano, M., Bonzani, G., Scalzone, A., Merenda, R., Monteforte, I., Monda, V., Muto, P., Carboni, G., Miglionico, M., Tavolozza, M., Marcassa, C., Campini, R., Calza, P., Giannuzzi, P., Eleuteri, E., Scapellato, F., Temporelli, P., Pellegrino, T., Storto, G., Sorrentino, A., Silvestri, A., Filardi, P., Brevetti, G., Cuocolo, A., Cho, K., Kumita, S., Seino, K., Nakajo, H., Toba, M., Kumazaki, T., Muramatsu, T., Yamazaki, T., Seki, K., Kawanami, J., Nakajima, T., Yamada, Y., Suga, T., Matsumoto, K., Nishimura, S., Taki, J., Higuchi, T., Kawashima, A., Nakajima, K., Muramori, A., Matsunari, I., Tait, J., Vanderheyden, J., Strauss, H., Tonami, N., Adachi, I., Shimomura, H., Kintaka, T., Komori, T., Ogura, Y., Kitaura, Y., Narabayashi, I., Iida, H., Zeniya, T., Kim, K., Watabe, H., Teramoto, N., Yamamichi, Y., Alexanderson, E., Ricalde, A., Vargas, A., Meave, A., Amigo, M., Misko, J., Dziuk, M., Warczynska, A., Skrobowska, E., Vasconcelos, M., Martins, E., Faria, T., Oliveira, A., Pardal, N., Macedo, F., Pereira, J., Rocha-Gonçalves, F., Cantinho, G., Pena, H., Freire, L., Veiga, A., Gonçalves, P., Godinho, F., Chua, T., Lee, C., Keng, F., Ding, Z., Koh, T., Awamleh, P., Talavera, P., Torres, V., Balsa, M., González, O., Alberca, M., Miguel, R., Cosío, F., Lomsky, M., Richter, J., Johansson, L., El-Ali, H., Åström, K., Ljungberg, M., Edenbrandt, L., Hung, G., Lee, K., Chen, C., Yang, K., Pekindil, G., Sarikaya, A., Ege, T., Salihoglu, S., Entok, E., Cavusoglu, Y., Ak, I., Vardareli, E., Timuralp, B., Tout, D., Loong, C., Naidoo, V., Aswegen, A., Underwood, S., Thorley, P., Goris, M., ZHU, H., Clements, I., Mullan, B., O'Connor, M., Breen, J., McGregor, C., Liu, Y., Li, S., Bourke, B., Weyman, C., Sinusas, A., Ramakrishna, G., Miller, T., Gibbons, R., Tsatkin, V., Wackers, F., Prior, J., Facta, A., Schindler, T., Oxilia-Estigarribia, M., Hernandez-Pampaloni, M., Campisi, R., Zhang, X., Bischof-Delaloye, A., Nathan, L., Schelbert, H., Gullberg, G., Huesman, R., Reutter, B., Sitek, A., Veress, A., Weiss, J., Qi, J., Yang, Y., Gordi, T., Olmsted, A., Lieu, H., and Belardinelli, L.

35. P67 Long non-coding RNAs in the infarcted heart.

Author

Zangrando, J, Zhang, L, Vausort, M, Maskali, F, Marie, PY, Wagner, DR, and Devaux, Y

Subjects
MYOCARDIAL infarction, NON-coding RNA, GENE expression, EXTRACELLULAR matrix proteins, VENTRICULAR remodeling, IN situ hybridization
Abstract

Purpose: Long non-coding RNAs (lncRNAs) constitute a novel class of non-coding RNAs. LncRNAs regulate gene expression, thus having the possibility to modulate disease progression. In this study, we investigated the expression of lncRNAs in the heart after myocardial infarction (MI).Methods: Adult male C57/BL6 mice were subjected to coronary ligation or sham operation. Cardiac gene expression was investigated using whole-genome microarrays with an in-house analytical pipeline dedicated to lncRNAs. Cardiac function was evaluated by 18F-fluorodesoxyglucose positron emission tomography (18F-FDG PET).Results: In a derivation group of 4 MI and 4 sham-operated mice sacrificed 24 hours after surgery, microarray analysis showed that MI significantly affected the cardiac transcriptome. 20 lncRNAs were up-regulated in the MI group, and 10 lncRNAs were down-regulated in the MI group (fold-change >2, false discovery rate <5%). Among these, 2 lncRNAs (called lncRNA1 and lncRNA2) showed robust up-regulation in the MI group: lncRNA1 (5-fold) and lncRNA2 (13-fold). This was confirmed using quantitative PCR, in which lncRNA1 and lncRNA2 displayed 6- and 12-fold up-regulation in the MI group, respectively (both P<0.05). Up-regulation of these 2 lncRNAs after MI was further confirmed in an independent validation group of 8 MI and 8 sham-operated mice (9-fold and 16-fold for lncRNA1 and lncRNA2, P<0.001). In a time-course analysis involving 21 additional MI mice, the expression of both lncRNAs peaked 24 hours after induction of MI and returned to basal levels after 2 days. In situ hybridization revealed an increase of lncRNA1 expression in the left ventricle of MI mice. Both lncRNAs were robustly correlated with left ventricular ejection fraction determined 24 hours after MI by 18F-FDG PET (r>0.8). Bioinformatic analyses of microarray data revealed that lncRNA1 expression displayed strong association with genes coding for proteins involved in angiogenesis, fibrosis, hypertrophy, inflammation, and extracellular matrix remodeling, all pathways involved in the development of left ventricular remodeling and heart failure post MI. Among the genes most highly correlated with lncRNA1 (r>0.80), MMP9, TNFalpha, CXCR4, and BNP were all up-regulated in the heart of MI mice.Conclusion: We show for the first time that expression of lncRNAs is regulated in the infarcted heart. This study provides the basis for future investigations of the role of lncRNAs in the diseased heart. [ABSTRACT FROM PUBLISHER]

Published
2014
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36. Assessment of a one-week ketogenic diet on brain glycolytic metabolism and on the status epilepticus stage of a lithium-pilocarpine rat model.

Author

Doyen M, Lambert C, Roeder E, Boutley H, Chen B, Pierson J, Verger A, Raffo E, Karcher G, Marie PY, and Maskali F

Subjects
Rats, Animals, Pilocarpine pharmacology, Lithium pharmacology, Rats, Wistar, Fluorodeoxyglucose F18 pharmacology, Brain diagnostic imaging, Hippocampus, Disease Models, Animal, Diet, Ketogenic, Status Epilepticus chemically induced, Status Epilepticus diagnostic imaging
Abstract

The ketogenic diet (KD) has been shown to be effective in refractory epilepsy after long-term administration. However, its interference with short-term brain metabolism and its involvement in the early process leading to epilepsy remain poorly understood. This study aimed to assess the effect of a short-term ketogenic diet on cerebral glucose metabolic changes, before and after status epilepticus (SE) in rats, by using [ 18 F]-FDG PET. Thirty-nine rats were subjected to a one-week KD (KD-rats, n = 24) or to a standard diet (SD-rats, n = 15) before the induction of a status epilepticus (SE) by lithium-pilocarpine administrations. Brain [ 18 F]-FDG PET scans were performed before and 4 h after this induction. Morphological MRIs were acquired and used to spatially normalize the PET images which were then analyzed voxel-wisely using a statistical parametric-based method. Twenty-six rats were analyzed (KD-rats, n = 15; SD-rats, n = 11). The 7 days of the KD were associated with significant increases in the plasma β-hydroxybutyrate level, but with an unchanged glycemia. The PET images, recorded after the KD and before SE induction, showed an increased metabolism within sites involved in the appetitive behaviors: hypothalamic areas and periaqueductal gray, whereas no area of decreased metabolism was observed. At the 4th hour following the SE induction, large metabolism increases were observed in the KD- and SD-rats in areas known to be involved in the epileptogenesis process late-i.e., the hippocampus, parahippocampic, thalamic and hypothalamic areas, the periaqueductal gray, and the limbic structures (and in the motor cortex for the KD-rats only). However, no statistically significant difference was observed when comparing SD and KD groups at the 4th hour following the SE induction. A one-week ketogenic diet does not prevent the status epilepticus (SE) and associated metabolic brain abnormalities in the lithium-pilocarpine rat model. Further explorations are needed to determine whether a significant prevention could be achieved by more prolonged ketogenic diets and by testing this diet in less severe experimental models, and moreover, to analyze the diet effects on the later and chronic stages leading to epileptogenesis., (© 2024. The Author(s).)

Published
2024
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37. Multi-tracer and multiparametric PET imaging to detect the IDH mutation in glioma: a preclinical translational in vitro, in vivo, and ex vivo study.

Author

Clément A, Zaragori T, Filosa R, Ovdiichuk O, Beaumont M, Collet C, Roeder E, Martin B, Maskali F, Barberi-Heyob M, Pouget C, Doyen M, and Verger A

Subjects
Animals, Fluorodeoxyglucose F18, Humans, Mutation, Positron-Emission Tomography methods, Rats, Receptors, GABA genetics, Glioma diagnostic imaging, Glioma genetics, Glioma metabolism
Abstract

Background: This translational study explores multi-tracer PET imaging for the non-invasive detection of the IDH1 mutation which is a positive prognostic factor in glioma., Methods: U87 human high-grade glioma (HGG) isogenic cell lines with or without the IDH1 mutation (CRISP/Cas9 method) were stereotactically grafted into rat brains, and examined, in vitro, in vivo and ex vivo. PET imaging sessions, with radiotracers specific for glycolytic metabolism ([ 18 F]FDG), amino acid metabolism ([ 18 F]FDopa), and inflammation ([ 18 F]DPA-714), were performed sequentially during 3-4 days. The in vitro radiotracer uptake was expressed as percent per million cells. For each radiotracer examined in vivo, static analyses included the maximal and mean tumor-to-background ratio (TBR max and TBR mean ) and metabolic tumor volume (MTV). Dynamic analyses included the distribution volume ratio (DVR) and the relative residence time (RRT) extracted from a reference Logan model. Ex vivo analyses consisted of immunological analyses., Results: In vitro, IDH1+ cells (i.e. cells expressing the IDH1 mutation) showed lower levels of [ 18 F]DPA-714 uptake compared to IDH1- cells (p < 0.01). These results were confirmed in vivo with lower [ 18 F]DPA-714 uptake in IDH+ tumors (3.90 versus 5.52 for TBR max , p = 0.03). Different values of [ 18 F]DPA-714 and [ 18 F] FDopa RRT (respectively 11.07 versus 22.33 and 2.69 versus - 1.81 for IDH+ and IDH- tumors, p < 0.02) were also observed between the two types of tumors. RRT [ 18 F]DPA-714 provided the best diagnostic performance to discriminate between the two cell lines (AUC of 100%, p < 0.01). Immuno-histological analyses revealed lower expression of Iba-1 and TSPO antibodies in IDH1+ tumors., Conclusions: [18F]DPA-714 and [18F] FDopa both correlate with the presence of the IDH1 mutation in HGG. These radiotracers are therefore good candidates for translational studies investigating their clinical applications in patients., (© 2022. The Author(s).)

Published
2022
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38. Preliminary Study of New Gallium-68 Radiolabeled Peptide Targeting NRP-1 to Detect Brain Metastases by Positron Emission Tomography.

Author

Moussaron A, Jouan-Hureaux V, Collet C, Pierson J, Thomas N, Choulier L, Veran N, Doyen M, Arnoux P, Maskali F, Dumas D, Acherar S, Barberi-Heyob M, and Frochot C

Subjects
Animals, Cell Line, Tumor, Cell Proliferation, Cell Tracking, Cerebellum diagnostic imaging, Cerebellum pathology, Female, Human Umbilical Vein Endothelial Cells metabolism, Humans, Peptides chemical synthesis, Protein Binding, Radiopharmaceuticals chemical synthesis, Rats, Nude, Recombinant Proteins metabolism, Surface Plasmon Resonance, Water chemistry, Rats, Brain Neoplasms diagnosis, Brain Neoplasms diagnostic imaging, Gallium Radioisotopes chemistry, Neuropilin-1 metabolism, Peptides chemistry, Positron-Emission Tomography, Radiopharmaceuticals chemistry
Abstract

Due to their very poor prognosis and a fatal outcome, secondary brain tumors are one of the biggest challenges in oncology today. From the point of view of the early diagnosis of these brain micro- and macro-tumors, the sensitivity and specificity of the diagnostic tools constitute an obstacle. Molecular imaging, such as Positron Emission Tomography (PET), is a promising technique but remains limited in the search for cerebral localizations, given the commercially available radiotracers. Indeed, the [ 18 F]FDG PET remains constrained by the physiological fixation of the cerebral cortex, which hinders the visualization of cerebral metastases. Tumor angiogenesis is recognized as a crucial phenomenon in the progression of malignant tumors and is correlated with overexpression of the neuropilin-1 (NRP-1) receptor. Here, we describe the synthesis and the photophysical properties of the new gallium-68 radiolabeled peptide to target NRP-1. The KDKPPR peptide was coupled with gallium-68 anchored into a bifunctional NODAGA chelating agent, as well as Cy5 for fluorescence detection. The Cy5 absorbance spectra did not change, whereas the molar extinction coefficient (ε) decreased drastically. An enhancement of the fluorescence quantum yield (φ F ) could be observed due to the better water solubility of Cy5. [ 68 Ga]Ga-NODAGA-K(Cy5)DKPPR was radiosynthesized efficiently, presented hydrophilic properties (log D = -1.86), and had high in vitro stability (>120 min). The molecular affinity and the cytotoxicity of this new chelated radiotracer were evaluated in vitro on endothelial cells (HUVEC) and MDA-MB-231 cancer cells (hormone-independent and triple-negative line) and in vivo on a brain model of metastasis in a nude rat using the MDA-MB-231 cell line. No in vitro toxicity has been observed. The in vivo preliminary experiments showed promising results, with a high contrast between the healthy brain and metastatic foci for [ 68 Ga]Ga-NODAGA-K(Cy5)DKPPR.

Published
2021
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39. Programming by Methyl Donor Deficiency during Pregnancy and Lactation Produces Cardiomyopathy in Adult Rats Subjected to High Fat Diet.

Author

Li Z, Kosgei VJ, Bison A, Alberto JM, Umoret R, Maskali F, Brunaud L, Guéant JL, and Guéant-Rodriguez RM

Subjects
Animals, Diet, High-Fat adverse effects, Energy Metabolism, Female, Fetal Development, Folic Acid, Lactation, Lipid Metabolism, Male, Myocardium pathology, Pregnancy, Rats, Rats, Wistar, Receptor, Angiotensin, Type 2, Transforming Growth Factor beta1, Ventricular Function, Left, Vitamin B 12, Cardiomyopathies chemically induced, Folic Acid Deficiency, Maternal Nutritional Physiological Phenomena, Vitamin B 12 Deficiency
Abstract

Scope: Vitamin B12 and folate (methyl donors) deficiency is frequent during pregnancy. Experimental rat models with methyl donor deficit during pregnancy and lactation (Initial methyl donor deficit (iMDD)) produce impaired myocardium fatty acid oxidation and mitochondrial energy metabolism at weaning., Methods and Results: The consequences of iMDD on heart of rat pups under normal diet after weaning and high fat diet (HF) between day (D) 50 and D185 are investigated. iMDD/HF induces increased histological fibrosis and increased B-type natriuretic peptide blood level. Inflammation is evidenced by increased protein expression of NFkB, Caspase1, and IL1β and fibrosis by increased expression of αSMA, col1a1, and col1a2 in females, but not in males. Fibrosis is related to increased angiotensin at D50 and D185 and increased protein expression of TGFB1 and AT1 angiotensin receptors at D185. The limited fibrosis in males is consistent with increased expression of AT2, the antagonist receptor of AT1. The increased expression of GLUT4 and decreased expression of PGC1α and PPARα reflect a shift from fatty acid oxidation to glycolysis., Conclusion: Developmental programming by iMDD produces cardiomyopathy in female offspring exposed to HF. The cardiomyopathy is linked to inflammation and fibrosis through angiotensin-AT2 and TGFB1 pathways and alteration of energy metabolism., (© 2021 Wiley-VCH GmbH.)

Published
2021
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40. Implementation of iMiDEV™, a new fully automated microfluidic platform for radiopharmaceutical production.

Author

Ovdiichuk O, Mallapura H, Pineda F, Hourtané V, Långström B, Halldin C, Nag S, Maskali F, Karcher G, and Collet C

Subjects
Fluorine Radioisotopes, Quality Control, Radiochemistry, Microfluidics, Radiopharmaceuticals
Abstract

iMiDEV™ microfluidic system is a new automated tool for a small-scale production of radiopharmaceuticals. This new radiochemistry module utilizes microfluidic cassettes capable of producing diversified radiopharmaceuticals in liquid phase reactions in an automated synthesizer. The user interface is intuitive and designed to give the operator all the information required and to allow driving the synthesis either manually or fully automatically. In this work, we have demonstrated liquid phase reaction and presented the first results of an efficient fully automated [18F]NaF radiosynthesis on the iMiDEV™ platform. Different parameters such as a type of cyclotron targets, initial activity, concentration and volume of the fluoride-18 targetry have been investigated in order to elaborate the optimised radiolabelling of the ligand. Single and double sodium [18F]fluoride synthesis procedures have been successfully developed using two chambers of the cassette. A single-dose of radiotracer was produced in an average radiochemical yield of 87% (decay corrected) within 8 min and quality control tests were performed as per European Pharmacopoeia.

Published
2021
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41. Synthesis of a DOTA- C -glyco bifunctional chelating agent and preliminary in vitro and in vivo study of [ 68 Ga]Ga-DOTA- C -glyco-RGD.

Author

Mangin F, Collet C, Jouan-Hureaux V, Maskali F, Roeder E, Pierson J, Selmeczi K, Marie PY, Boura C, Pellegrini-Moïse N, and Lamandé-Langle S

Abstract

The design of bifunctional chelating agents (BFCA) allowing straightforward radiometal labelling of biomolecules is a current challenge. We report herein the development of a bifunctional chelating agent based on a DOTA chelator linked to a C -glycosyl compound, taking advantage of the robustness and hydrophilicity of this type of carbohydrate derivative. This new BFCA was coupled with success by CuAAC with c(RGDfK) for α v β 3 integrin targeting. As attested by in vitro evaluation, the conjugate DOTA- C -glyco-c(RGDfC) demonstrated high affinity for α v β 3 integrins (IC 50 of 42 nM). [ 68 Ga]Ga-DOTA- C -glyco-c(RGDfK) was radiosynthesized straightforwardly and showed high hydrophilic property (log  D 7.4 = -3.71) and in vitro stability (>120 min). Preliminary in vivo PET study of U87MG engrafted mice gave evidence of an interesting tumor-to-non-target area ratio. All these data indicate that [ 68 Ga]Ga-DOTA- C -glyco-c(RGDfK) allows monitoring of α v β 3 expression and could thus be used for cancer diagnosis. The DOTA- C -glycoside BFCA reported here could also be used with various ligands and chelating other (radio)metals opening a broad scope of applications in imaging modalities and therapy., Competing Interests: There are no conflicts to declare., (This journal is © The Royal Society of Chemistry.)

Published
2021
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42. A 1-week extension of a ketogenic diet provides a further decrease in myocardial 18 F-FDG uptake and a high detectability of myocarditis with FDG-PET.

Author

Clément A, Boutley H, Poussier S, Pierson J, Lhuillier M, Kolodziej A, Olivier JL, Karcher G, Marie PY, and Maskali F

Subjects
Animal Feed, Animals, Diet, Carbohydrate-Restricted, Dietary Carbohydrates, Fasting, Heart, Inflammation, Male, Myocardium metabolism, Myosins metabolism, Radiopharmaceuticals, Rats, Rats, Wistar, Swine, Diet, Ketogenic, Fluorodeoxyglucose F18, Heart Diseases diagnostic imaging, Myocarditis diagnostic imaging, Positron-Emission Tomography methods
Abstract

Background: Short periods of fasting and/or low-carbohydrate diet have been proven beneficial for decreasing the myocardial uptake of 18 F-fluorodeoxyglucose ( 18 F-FDG) and enhancing the detection of inflammatory heart diseases by 18 F-FDG positron emission tomography (PET). This study aimed at determining whether this benefit is increased when a low-carbohydrate ketogenic diet is prolonged up to 7 days., Methods: Wistar rats underwent serial 18 F-FDG-PET imaging after an 18-hour fasting period and after 2, 4 and 7 days of a ketogenic diet (3% carbohydrate) and they were compared to rats submitted to the same protocol but with normal diet (44% carbohydrate). The 18 F-FDG-PET/ketogenic protocol was also applied in rats with immune myocarditis (injection of porcine cardiac myosin)., Results: The 7-day ketogenic diet was associated with (1) a sustained increase in circulating ketone bodies at an equivalent level to that reached after 18-hour fasting, (2) a gradual decrease in 18 F-FDG uptake within normal myocardium reaching a lower level compared to fasting at the 7th day (myocardium-to-blood ratios: 1.68 ± 1.02 vs 3.25 ± 1.40, P < .05) and (3) a high 18 F-FDG-PET detectability of myocarditis areas., Conclusion: One-week extension of a ketogenic diet provides a further decrease in the 18 F-FDG uptake of normal myocardium and a high detectability of inflammatory areas.

Published
2020
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43. PET imaging of 68 Ga-NODAGA-RGD, as compared with 18 F-fluorodeoxyglucose, in experimental rodent models of engrafted glioblastoma.

Author

Isal S, Pierson J, Imbert L, Clement A, Collet C, Pinel S, Veran N, Reinhard A, Poussier S, Gauchotte G, Frezier S, Karcher G, Marie PY, and Maskali F

Abstract

Background: Tracers triggering αvβ3 integrins, such as certain RGD-containing peptides, were found promising in previous pilot studies characterizing high-grade gliomas. However, only limited comparisons have been performed with current PET tracers. This study aimed at comparing the biodistribution of 18 F-fluorodeoxyglucose ( 18 F-FDG) with that of 68 Ga-NODAGA-RGD, an easily synthesized monomeric RGD compound with rapid kinetics, in two different rodent models of engrafted human glioblastoma., Methods: Nude rodents bearing human U87-MG glioblastoma tumor xenografts in the flank (34 tumors in mice) or in the brain (5 tumors in rats) were analyzed. Kinetics of 68 Ga-NODAGA-RGD and of 18 F-FDG were compared with PET imaging in the same animals, along with additional autohistoradiographic analyses and blocking tests for 68 Ga-NODAGA-RGD., Results: Both tracers showed a primary renal route of clearance, although with faster clearance for 68 Ga-NODAGA-RGD resulting in higher activities in the kidneys and bladder. The tumor activity from 68 Ga-NODAGA-RGD, likely corresponding to true integrin binding (i.e., suppressed by co-injection of a saturating excess of unlabeled RGD), was found relatively high, but only at the 2 nd hour following injection, corresponding on average to 53% of total tumor activity. Tumor uptake of 68 Ga-NODAGA-RGD decreased progressively with time, contrary to that of 18 F-FDG, although 68 Ga-NODAGA-RGD exhibited 3.4 and 3.7-fold higher tumor-to-normal brain ratios on average compared to 18 F-FDG in mice and rat models, respectively. Finally, ex-vivo analyses revealed that the tumor areas with high 68 Ga-NODAGA-RGD uptake also exhibited the highest rates of cell proliferation and αv integrin expression, irrespective of cell density., Conclusions: 68 Ga-NODAGA-RGD has a high potential for PET imaging of glioblastomas, especially for areas with high integrin expression and cell proliferation, although PET recording needs to be delayed until the 2 nd hour following injection in order to provide sufficiently high integrin specificity.

Published
2018
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44. Synthesis and preliminary in vivo evaluation of new [ 18 F]fluoro-inositols as Positron Emission Tomography radiotracers.

Author

Collet C, Schmitt S, Maskali F, Clément A, Chrétien F, Karcher G, Marie PY, Poussier S, and Lamandé-Langle S

Subjects
Animals, Breast Neoplasms diagnostic imaging, Breast Neoplasms pathology, Disease Models, Animal, Female, Humans, Inositol analogs & derivatives, Inositol chemical synthesis, Mice, Molecular Structure, Fluorine Radioisotopes standards, Inositol chemistry, Positron-Emission Tomography, Radiopharmaceuticals
Abstract

This study describes the synthesis and radiosynthesis of eight new [ 18 F]fluoro-inositol-based radiotracers in myo- and scyllo-inositol configuration. These radiotracers are equipped with a propyl linker bearing fluorine-18. This fluorinated arm is either on a hydroxyl group, i.e. O-alkylated inositols, or on the cyclohexyl backbone, i.e. C-branched derivatives. To modulate lipophilicity, inositols were synthesized in acetylated or hydroxylated form. Automated radiosynthesis was performed on the AllInOne module and the radiotracers were produced in good radiochemical yields (15-31.5% dc). Preliminary in vivo preclinical evaluation of these eight [ 18 F]fluoro-inositols as Positron Emission Tomography (PET) imaging agents in a breast tumour-bearing mouse model was performed and compared with [ 18 F]-2-fluoro-2-deoxy-d-glucose ([ 18 F]FDG). Amongst the different inositols, [ 18 F]myo-2 showed the highest tumour uptake 2.34±0.39%ID/g, revealing the potential of this tracer for monitoring breast cancer., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published
2017
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45. Quantitative SPM Analysis Involving an Adaptive Template May Be Easily Applied to [ 18 F]FDG PET Images of the Rat Brain.

Author

Poussier S, Maskali F, Vexiau G, Verger A, Boutley H, Karcher G, Raffo E, and Marie PY

Subjects
Animals, Imaging, Three-Dimensional, Male, Rats, Sprague-Dawley, Brain diagnostic imaging, Fluorodeoxyglucose F18 chemistry, Positron-Emission Tomography, Statistics as Topic
Abstract

Purpose: The Statistical Parametric Mapping (SPM) software is frequently used for the quantitative analysis of patients' brain images obtained from 2-deoxy-2-[ 18 F]fluoro-D-glucose positron emission tomography ([ 18 F]FDG PET). However, its adaptation to small animals is difficult, particularly for the initial step of spatial normalization which requires a specific brain anatomical template. This study was aimed at determining whether SPM analysis can be applied to rat, and more specifically to the lithium-pilocarpine model of epilepsy, by using an adaptive template. This template developed for PET clinical imaging is constructed from a block matching algorithm., Procedures: SPM analysis of brain [ 18 F]FDG PET images from Sprague-Dawley rats was used with the block matching (BM) adaptive template for the detection of brain abnormalities (1) artificially inserted within the initially normal brain images of 10 rats (50 % decrease in signal intensity within 40 spheres of 0.5 to 1.0 mm in diameter) and (2) occurring at 4 h (n = 16), 48 h (n = 15), and 8 days (n = 13) after lithium-pilocarpine treatment., Results: Concordant positive clusters were documented for all inserted abnormalities, whereas no aberrant clusters were documented in remote brain areas. Positive clusters were also detected on sites known to be involved in the epileptogenesis process of the lithium-pilocarpine model (piriform and entorhinal cortex, hippocampus), with the expected time-specific changes involving an early hypermetabolism followed by a severe hypometabolism and a subsequent partial recovery., Conclusion: A quantitative SPM analysis of brain [ 18 F]FDG PET images may be applied to the monitoring of rat brain function when using an adaptive BM template.

Published
2017
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46. Development of 6-[(18) F]fluoro-carbohydrate-based prosthetic groups and their conjugation to peptides via click chemistry.

Author

Collet C, Maskali F, Clément A, Chrétien F, Poussier S, Karcher G, Marie PY, Chapleur Y, and Lamandé-Langle S

Subjects
Animals, Click Chemistry methods, Positron-Emission Tomography, Radiopharmaceuticals pharmacokinetics, Rats, Tissue Distribution, Fluorine Radioisotopes chemistry, Glycopeptides chemistry, Radiopharmaceuticals chemical synthesis
Abstract

This work describes the development of new 6-[(18) F]fluoro-carbohydrate-based prosthetic groups equipped with an azido arm that are able to participate in copper(I)-catalyzed cycloadditions for (18) F labeling of biomolecules under mild conditions. The radiolabeling in high radiochemical yields (up to 68 ± 6%) of these different prosthetic groups is presented. The flexibility of the azido arm introduced on the carbohydrate moieties allows efficient click reactions with different alkyne functionalized peptides such as gluthation or Arg-Gly-Asp derivatives in order to prepare glycopeptides. The radiosyntheses of (18) F-labeled glycopeptides proceed in high radiochemical yields (up to 76%) in an automated process with excellent radiochemical purity. The addition of a sugar moiety on peptides should enhance the bioavailability, pharmacokinetic, and in vivo clearance properties of these glycopeptides, compared with the unlabeled native peptide, and these properties are highly favorable for positron emission tomography imaging. A high uptake of (18) F-β-gluco-c(RGDfC) is shown by positron emission tomography imaging in a subcutaneous abscess model in the rat, revealing the potential of this tracer to monitor integrin expression as a part of inflammation and/or angiogenesis processes., (Copyright © 2015 John Wiley & Sons, Ltd.)

Published
2016
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47. TREM-1 Mediates Inflammatory Injury and Cardiac Remodeling Following Myocardial Infarction.

Author

Boufenzer A, Lemarié J, Simon T, Derive M, Bouazza Y, Tran N, Maskali F, Groubatch F, Bonnin P, Bastien C, Bruneval P, Marie PY, Cohen R, Danchin N, Silvestre JS, Ait-Oufella H, and Gibot S

Subjects
Acute Disease, Amino Acid Sequence, Animals, Blotting, Western, Coronary Disease blood, Gene Expression, Humans, Inflammation genetics, Inflammation physiopathology, Leukocytes metabolism, Leukocytes pathology, Male, Membrane Glycoproteins antagonists & inhibitors, Membrane Glycoproteins blood, Membrane Glycoproteins genetics, Mice, Inbred C57BL, Mice, Knockout, Myocardial Infarction genetics, Myocardial Infarction physiopathology, Peptides pharmacology, Rats, Wistar, Receptors, Immunologic antagonists & inhibitors, Receptors, Immunologic blood, Receptors, Immunologic genetics, Reverse Transcriptase Polymerase Chain Reaction, Survival Analysis, Triggering Receptor Expressed on Myeloid Cells-1, Ventricular Function, Left drug effects, Ventricular Function, Left genetics, Ventricular Function, Left physiology, Ventricular Remodeling drug effects, Ventricular Remodeling genetics, Ventricular Remodeling physiology, Inflammation metabolism, Membrane Glycoproteins metabolism, Myocardial Infarction metabolism, Receptors, Immunologic metabolism
Abstract

Rationale: Optimal outcome after myocardial infarction (MI) depends on a coordinated healing response in which both debris removal and repair of the myocardial extracellular matrix play a major role. However, adverse remodeling and excessive inflammation can promote heart failure, positioning leucocytes as central protagonists and potential therapeutic targets in tissue repair and wound healing after MI., Objective: In this study, we examined the role of triggering receptor expressed on myeloid cells-1(TREM-1) in orchestrating the inflammatory response that follows MI. TREM-1, expressed by neutrophils and mature monocytes, is an amplifier of the innate immune response., Methods and Results: After infarction, TREM-1 expression is upregulated in ischemic myocardium in mice and humans. Trem-1 genetic invalidation or pharmacological inhibition using a synthetic peptide (LR12) dampens myocardial inflammation, limits neutrophils recruitment and monocyte chemoattractant protein-1 production, thus reducing classical monocytes mobilization to the heart. It also improves left ventricular function and survival in mice (n=20-22 per group). During both permanent and transient myocardial ischemia, Trem-1 blockade also ameliorates cardiac function and limits ventricular remodeling as assessed by fluorodeoxyglucose-positron emission tomographic imaging and conductance catheter studies (n=9-18 per group). The soluble form of TREM-1 (sTREM-1), a marker of TREM-1 activation, is detectable in the plasma of patients having an acute MI (n=1015), and its concentration is an independent predictor of death., Conclusions: These data suggest that TREM-1 could constitute a new therapeutic target during acute MI., (© 2015 American Heart Association, Inc.)

Published
2015
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48. Identification of candidate long non-coding RNAs in response to myocardial infarction.

Author

Zangrando J, Zhang L, Vausort M, Maskali F, Marie PY, Wagner DR, and Devaux Y

Subjects
Animals, Disease Models, Animal, Gene Expression Regulation, Male, Mice, Mice, Inbred C57BL, Myocardial Infarction pathology, Oligonucleotide Array Sequence Analysis, Stroke Volume, Ventricular Remodeling, Heart Ventricles metabolism, Myocardial Infarction genetics, RNA, Long Noncoding genetics
Abstract

Background: Long non-coding RNAs (lncRNAs) constitute a novel class of non-coding RNAs. LncRNAs regulate gene expression, thus having the possibility to modulate disease progression. In this study, we investigated the changes of lncRNAs expression in the heart after myocardial infarction (MI)., Results: Adult male C57/BL6 mice were subjected to coronary ligation or sham operation. In a derivation group of 4 MI and 4 sham-operated mice sacrificed 24 hours after surgery, microarray analysis showed that MI was associated with up-regulation of 20 lncRNAs and down-regulation of 10 lncRNAs (fold-change >2). Among these, 2 lncRNAs, called myocardial infarction-associated transcript 1 (MIRT1) and 2 (MIRT2), showed robust up-regulation in the MI group: 5-fold and 13-fold, respectively. Up-regulation of these 2 lncRNAs after MI was confirmed by quantitative PCR in an independent validation group of 8 MI and 8 sham-operated mice (9-fold and 16-fold for MIRT1 and MIRT2, P < 0.001). In a time-course analysis involving 21 additional MI mice, the expression of both lncRNAs peaked 24 hours after MI and returned to baseline after 2 days. In situ hybridization revealed an up-regulation of MIRT1 expression in the left ventricle of MI mice. Expression of MIRT1 and MIRT2 correlated with the expression of multiple genes known to be involved in left ventricular remodeling. Mice with high level of expression of MIRT1 and MIRT2 had a preserved ejection fraction., Conclusion: Myocardial infarction induces important changes in the expression of lncRNAs in the heart. This study motivates further investigation of the role of lncRNAs in left ventricular remodeling.

Published
2014
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49. Assessment of the early stage of cardiac remodeling of spontaneously hypertensive heart failure rats using the quantitative 3-dimensional analysis provided by acipimox-enhanced FDG-PET.

Author

Maskali F, Poussier S, Louis H, Boutley H, Lhuillier M, Thornton SN, Karcher G, Lacolley P, and Marie PY

Subjects
Animals, Arterial Pressure, Cardiac Catheterization, Disease Models, Animal, Fibrosis, Heart Failure etiology, Heart Failure metabolism, Heart Failure physiopathology, Heart Ventricles metabolism, Heart Ventricles physiopathology, Lipid Metabolism, Male, Predictive Value of Tests, Rats, Rats, Inbred SHR, Rats, Inbred WKY, Stroke Volume, Time Factors, Ventricular Function, Left, Fluorodeoxyglucose F18, Heart Failure diagnostic imaging, Heart Ventricles diagnostic imaging, Hypertension complications, Imaging, Three-Dimensional, Positron-Emission Tomography methods, Pyrazines, Radiographic Image Interpretation, Computer-Assisted, Radiopharmaceuticals, Ventricular Remodeling
Abstract

Spontaneously hypertensive heart failure rats (SHHF) appear to constitute an original model for analyzing the evolution of the metabolic syndrome towards heart failure. This study aimed to characterize early cardiac dysfunction and remodeling in SHHF rats: (1) as compared with spontaneously hypertensive rats (SHR) and with a control group of Kyoto rats (WKY), and (2) by using the 3-dimensional quantitative analysis provided by acipimox-enhanced positron emission tomography (PET) with (18)F-fluorodesoxyglucose (FDG). Left ventricular (LV) ejection fraction (EF) and volume were quantified by automatic software on the FDG-PET images recorded in SHR (n = 20), SHHF (n = 18) and WKY-rats (n = 19) at ages 3 or 10 months old. Arterial blood pressure was determined by cardiac catheterization and cardiac fibrosis was quantified after sacrifice. Blood pressure was similarly elevated in SHR and SHHF rats (respective systolic blood pressures at 10-months: 199 ± 39 vs. 205 ± 2 mmHg), but SHHF rats had higher body mass than SHR rats (at 10-months, 630 ± 36 vs. 413 ± 27 g, p < 0.05) and higher blood levels of cholesterol and of triglycerides. At 3 months, cardiac parameters did not show significant differences between groups but at 10-months, SHHF and SHR rats exhibited an enhancement in myocardial mass and fibrosis associated with a clear decline in LV-EF (SHHF: 46 ± 6 %; SHR: 47 ± 5 %) as compared with WKY (56 ± 6 %, p < 0.01 for both comparisons). Cardiac remodeling of SHHF rats was clearly observable by FDG-PET from the age of 10-months, but in a similar way to that observed for SHR rats, suggesting a predominant role of hypertension.

Published
2014
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50. Cardioprotective effects of adenosine within the border and remote areas of myocardial infarction.

Author

Bousquenaud M, Maskali F, Poussier S, Zangrando J, Marie PY, Boutley H, Fay R, Karcher G, Wagner DR, and Devaux Y

Abstract

Background: Adenosine may have beneficial effects on left ventricular function after myocardial infarction (MI), but the magnitude of this effect on remote and MI areas is controversial. We assessed the long-term effects of adenosine after MI using electrocardiogram-triggered 18 F-fluorodeoxyglucose positron emission tomography., Methods: Wistar rats were subjected to coronary ligation and randomized into three groups treated daily for 2 months by NaCl (control; n = 7), 2-chloroadenosine (CADO; n = 8) or CADO with 8-sulfophenyltheophilline, an antagonist of adenosine receptors (8-SPT; n = 8)., Results: After 2 months, control rats exhibited left ventricular remodelling, with increased end-diastolic volume and decreased ejection fraction. Left ventricular remodelling was not significantly inhibited by CADO. Segmental contractility, as assessed by the change in myocardial thickening after 2 months, was improved in CADO rats compared to control rats (+1.6% ± 0.8% vs. -2.3% ± 0.8%, p < 0.001). This improvement was significant in border (+5.6% ± 0.8% vs. +1.5% ± 0.8%, p < 0.001) and remote (-4.0% ± 1.0% vs. -10.4% ± 1.3%, p < 0.001) segments, but absent in MI segments. Histological analyses revealed that CADO reduced fibrosis, cardiomyocyte hypertrophy and apoptosis. Protective effects of CADO were blunted by 8-SPT., Conclusion: Long-term administration of adenosine protects the left ventricle from contractile dysfunction following MI.

Published
2013
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