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6. Abstracts for the Tenth International Conference on Brain Tumour Research and Therapy: Stalheim Hotel, Voss, Norway, September 6–9, 1993

Author

Abrahamsen, Tore G., Wesenberg, Finn, Mørk, Sverre, Allen, Jeffrey, Hayes, Roberta, DaRosso, Robert, Nirenberg, Anita, Ali-Osman, Francis, Akande, Nike, Amberger, V., Seulberger, H., Paganetti, P. A., Schwab, M. E., Schwab, M. E., Arita N., Ohnishi T., Hiraga S., Yamamoto H., Taki T., Izumoto S., Higuchi M., Hayakawa T., Kusakabe M., Sakakura T., Baldwin, N. G., Rice, C. D., Merchant, R. E., Ashmore, Sally M., Darling, J. L., Bailey, C. C., Balmaceda C., Diez B., Villablanca J., Walker R., Finlay J., Bergenheim, A. Tommy, Hartman, Magdalena, Bergh, Jonas, Ridderheim, PerÅke, Henriksson, Roger, Berens, Michael E., Rief, Monique D., Giese, Alf, Zackrisson, Björn, Elfversson, Jörgen, Bernstein, Mark, Cabantog, Alberto, Glen, Jennifer, Mikulis, David, Bjerkvig, Rolf, Pedersen, Paal-Henning, Mathisen, Berit, Mahesparan, Rupavathana, Haugland, Hans Kristian, Bernstein, Mark, Laperriere, Normand, Thomason, Cindy, Leung, Phil, Bobola M. S., Berger M. S., Silber J. R., Bongcam-Rudloff, Erik, Wang, Jia-Lun, Nistér, Monica, Westermark, Bengt, Brem, Steven, Breslow, Gary, Ho, Jason, Gately, Stephen, Takano, Shingo, Ward, William, Brada, M., Laing, R., Warrington, J., Brem, Steven, Engelhard, Herbert, Takano, Shingo, Gately, Stephen, Brem, Steven, Landau, Barry, Kwaan, Hau, Verrusio, Elaine, Buckner, J. C., Cascino, T. L., Schomberg, P. S., O'Fallon, J. R., Dinapoli, R. P., Burch, P. A., Shaw, E. G., Broaddus, William C., Hager-Loudon, Kathryn, Merchant, Randall E., Loudon, William, Couldwell, William T., Jiang, Jack B., Burns, David, Couldwell, William T., Weiss, Martin H., Apuzzo, Michael L. J., Desbaillets I., Tada M., de Tribolet N., Van Meir, E., Davis, R. L., Onda, K., Prados, M. D., Dolan, M. Eileen, Fleig, Matthew J., Friedman, Henry S., Ekstrand, A. Jonas, Longo, Nicola, James, C. David, Chou, D., Wijnhoven, B., Bellinzona, M., Nakagawa, M., Feuerstein B. G., Basu H. S., Dolan M. E., Bergeron C., Pellarm M., Deen D. F., Marton L. J., Finlay, Jonathan, Fulton D. S., Urtasun R. C., Giese, Alf, Scheck, Adrienne C., Geddes, J., Vowles, G. M., Ashmore, S. M., Gillespie, G. Y., Goldman, C. K., Tucker, M. T., Lyon, E., Tsai, J. -C., Gobbel, G. T., Chan, P. H., Greenberg, Hairy S., Chandler, W. F., Ensminger, W. D., Junck, L., Sandler, H., Bromberg, J., McKeever, P., Gonzalez G. G., Sarkar A., Basu H., Feuerstein B. G., Deen D. F., Haugland, Kr., Tysnes, Ole-Bjørn, Hiraga, Shoju, Arita, Norio, Ohnishi, Takanori, Taki, Takuyu, Yamamoto, Hiroshi, Higuchi, Masahide, Hayakawa, Toru, Isern, Erik, Unsgaard, Geirmund, Marthinsen, Anne Beate Langeland, Strickert, Trond, Helseth, Eirik, Hochberg F., Cosgrove R., Valenzuela R., Pardo F., Zervas N., Jenkins, Robert B., Ritland, Steven R., Hailing, Kevin C., Thibodeau, Stephen N., Juillerat L., Darekar P., Janzer R. C., Hamou M. F., Kato, Tsutomu, Sawamura, Yutaka, Tada, Mitsuhiro, Sakuma, Shirou, Sudo, Masako, Abe, Hiroshi, Kallio M., Leppää J., Nikula T., Nikkinen P., Gylling H., Färkkilä M., Hiltunen J., Jääskeläinen J., Liewendahl K., Keles, G. Evren, Berger, Mitchel S., Deliganis, Anna, Kellie S. J., De Graaf S. S. N., Bloemhof H., Johnston I., Uges D. D. R., Besser M., Chaseling R. W., Ouvrier R. A., Kitchen, N. D., Hughes, S., Beaney, R., Thomas, D. G. T., Kim D. H., Maeda T., Mohapatra G., Park S., Waldman F. W., Gray J. W., Koala, D., Silber, J., Berger, M., Krauseneck P., Müller B., Strik H., Warmuth-Metz M., Kuratsu, Jun-ichi, Takeshima, Hideo, Ushio, Yukitaka, Kretschmar, C., Grodman, H., Linggood, R., Kyritsis, A. P., Bondy, M., Cunningham, J., Xiao, M., Levin, V., Leeds, N., Bruner, J., Yung, W. K. A., Saya, H., Lampson, L. A., Nichols, M. R., Lampson, M. A., Dunne, A. D., Li, Hong, Hamou, Marie-France, Jaufeerally, Rehana, Diserens, Annie-Claire, Van Meir, Erwin, de Tribolet, Nicolas, Levin, V. A., Maor, M., Sawaya, R., Leavens, M., Woo, S., Thall, P., Gleason, M. J., Liang, Bertrand C., Ross, D. A., Meltzer, P. S., Trent, J. M., Greenberg, H. S., Lillehei K. O., Kong Q., DeMasters B. K., Withrow S. J., Macdonald D. R., Cairncross J. G., Ludwin S., Lee D., Cascino T., Buckner J., Dropcho E., Fulton D., Stewart D., Schold C., Wainman N., Eisenhauer E., Kirby S., Fisher B. J., Magrassi, L., Butti, G., Pezzotta, S., Milanesi∘, G., Matsutani, Masao, Marienhagen, Kirsten, Laerum, Ole Didrik, Baldwin, N. G., Merzak, Abderrahim, Koocheckpour, Shahriar, Roxanis, Yannis, Pilktngton, Geoffrey J., Nagai, Masakatsu, Watanabe, Kunihiko, Narita, Jun-ichi, Hagiwara, Hideaki, Noble, Mark, Nomura, K., Oyama, H., Motoo, M., Shibui, S., Tokuue, K., Akine, Y., Ohnishi, T., Arita, N., Hiraga, S., Hayakawa, T., Nygaard, Svein J. Tjoflaat, Tysnes, Ole-Bjørn, Pardo, F. S., Hsu, D. W., Hedley-Whyte, E. T., Efird, J., Schmidt, E. V., Marienhagen, Paal-Henning Pedersenl Kirsten, Pilkington, Geoffrey J., Clarke, Tracey M., Yu, Hui Tian, Rogers, Joan P., Stern, Robert, Phuphanich, Surasak, Greenberg, Harvey, Murtagh, R., Viloria, Jesus, Ransohoff, Joseph, Martin, Kimberly, Hatva, V. Erika, Rao, Jasti S., Mohanam, S., Rempel, Sandra A., Schwechheimer, Karl, Davis, Richard L., Cavenee, Webster K., Rosenblum, Mark L., Reifenberger, Guido, Liu, Lu, Ichimura, Koichi, Schmidt, Esther E., Collins, V. Peter, Revesz T., Scaravilli F., Cockburn H., Thomas D. G. T., Rice, C. D., Biron, R. T., Merchant, R. E., McKerrow, James, Sloane, Bonnie, Mikkelsen, Tom, Roosen, Norbert, Coopersmith, Peter, Smith, Robert, Rooprai, Harcharan Kaur, Maidment, Steven, Rucklidge, Garry, Volovsek, Anton, Rutka J. T., Smith S. L., Matsuzawa K., Sankar, A. A., Darling, J. L., Williams, S. R., Fukuyama K., Marton L. J., Ikeda, Jun, Selker, R. G., Vertosick, F. T., Goldenberg, M. T., Bindal, R., Diez B., Taratuto A., Picco P., Monges J., Martinez M., Pacheco G., Gamboni M., Schultz M., Silber J. R., Mueller B. A., Ewers T. G., Berger M. S., Shiraishi, T., Tabuchi, K., Nakagawa, S., Kihara, S., Stewart, D. J., Eapen, L., Agboola, O., Popovic, P., Goel, R., Raaphorst, P., Wong, P. T. T., Shimokawa, S., Oh-uchida, M., Hori, K., Markert C., Pflughaupt K. -W., Tada M., Diserens A. -C., Jauferrally R., Desbaillets I., Hamou M. -F., de Tribolet N., Takeshima H., Mochizuki H., Clifford J. L., Nishi T., Levin V. A., Lotan R., Saya H., Terzis, A. J. A., Arnold, H., Laerum, O. D., Bjerkvig, R., Taratuto A. L., Sevlever G., Diaz D., Di Tella M., Cuccia V., Pomata H., Gallo G., Dietze, A., Knopp, U., Thomas, R., Brada, M., Carnochan, P., Flux, G., Kitchen, N., Thomas, D., Zalutsky, M., Bigner, D., Tofilon, Philip, Borchardt, Paul, Torp, Sverre H., Dalen, Are, Tohyama, Takashi, Kubo, Osami, Takakura, Kintomo, Lee, Virginia M. -Y., Trojanowski, John Q., Nygaard, Svein, Urtasun, R. C., Parliament, M. B., McEwan, A. J., Mannan, R. H., Weibe, L. I., Unsgårp, G., Sonnewald, U., Gribbestad, I., Isern, E., Petersen, S. B., Wang J., Delgado D. A., Warr, Tracy J., Sheer, Denise, Gorman, Pat, Yamaguchi, F., Westphal, M., Anker, L., Hamel, W., Lücke, M., Shepard, M., Kleihues, P., Herrmann, H. D., Yung, W. K. Alfred, Taylor, Scott, and Steck, Peter A.

Published
1993
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8. Reduced adenosine uptake and its contribution to signaling that mediates profibrotic activation in renal tubular epithelial cells: Implication in diabetic nephropathy

Author

Kretschmar C, Oyarzún C, Villablanca C, Jaramillo C, Alarcón S, Perez G, Díaz-Encarnación MM, Pastor-Anglada M, Garrido W, Quezada C, and San Martín R

Subjects
Male, kidney tubule, Adenosine, Sprague Dawley rat, diabetic nephropathy, fibrosis, Epithelial Cells, Rats, Cell Line, Rats, Sprague-Dawley, Kidney Tubules, Animals, Humans, pathology, animal, rat, Diabetic Nephropathies, human, epithelium cell, metabolism, signal transduction
Abstract

Altered nucleoside levels may be linked to pathogenic signaling through adenosine receptors. We hypothesized that adenosine dysregulation contributes to fibrosis in diabetic kidney disease. Our findings indicate that high glucose levels and experimental diabetes decreased uptake activity through the equilibrative nucleoside transporter 1 (ENT1) in proximal tubule cells. In addition, a correlation between increased plasma content of adenosine and a marker of renal fibrosis in diabetic rats was evidenced. At the cellular level, exposure of HK2 cells to high glucose, TGF-ß and the general adenosine receptor agonist NECA, induced the expression of profibrotic cell activation markers a-SMA and fibronectin. These effects can be avoided by using a selective antagonist of the adenosine A3 receptor subtype in vitro. Furthermore, induction of fibrosis marker a-SMA was prevented by the A3 receptor antagonist in diabetic rat kidneys. In conclusion, we evidenced the contribution of purinergic signaling to renal fibrosis in experimental diabetic nephropathy. Copyright: © 2016 Kretschmar et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Published
2016

11. Comparison of pulse-echo-methods for testing concrete

Author

Krause, M., Bärmann, R., Frielinghaus, R., Kretschmar, C., Kroggel, O., Langenberg, K.J., Maierhofer, C., Müller, V., Neisecke, J., Schickert, M., Schmitz, V., Wiggenhauser, H., Wollbold, F., and Publica

Subjects
Radar, ultrasound, Impakt-Puls-Echo, Beton, concrete, impact-puls-echo, Ultraschall
Abstract

Pulse-echo methods (radar, impact-echo, ultrasonic impulse-echo) and simulation of wave propagation are applied for testing concrete specimens with metal ducts. The results of nondestructive testing of the same specimens by nine workgroups are described and compared. The research aims for the experiments are thickness measurement, location of a metal duct and of voided regions inside the duct. The results show the remarkable progress achieved in the past few years: the thickness and location of a duct could be measured for one specimen with great precision. In some cases voided regions in the duct could be located.

Published
1997

12. Schadensanalyse des Dielektrikums - DP5704

Author

Otschik, P., Kretschmar, C., Obenaus, P., and Publica

Subjects
Dielektrikum, reliability, Zuverlässigkeit, dielectric, paste
Abstract

According to some applications of hybrid circuits it can occur that corresponding the long term test of the reliability for a dielectric (85 degree, 85 RH, 1 000 h) is not sufficient Therefore the fired layers of DP 5704 and C 1214D were tested at 30 degree, 95 RH and different voltages (0...15 V) up to 30 days and interimly electrically characterized. The structure of the dielectric was analyzed at fracture surfaces with SEM and EDX This storage conditions lead to following effects The humidity does not penetrate through the planar electrode of the capacitor in the dielectric but about the opening edges only. The insulation resitivity (Riso) and the breakdown voltage decrease and tan delta increases with the time. In the case Riso smaller 10000000 Ohm and tan delta is unchanged small we often observed an increasing of the Riso at a later time. Generally the dielectrics showed at Riso smaller 10000000 Ohm a varistor like behavior. It is shown that the measuring results can be explained by the surface roughness of the dielectrics and by differences in the void distribution. The results suggest ideas for the improvement of the material properties.

Published
1994

13. Entwicklung einer Dünnschichtglaspaste für Aluminiumoxidkeramik

Author

Otschik, P., Kretschmar, C., and Publica

Subjects
Glas, Aluminiumoxid, Glass, paste, alumina
Abstract

A glass paste for alumina was developed to realized a fired thickness smaller than 2 my. The particle size of the glass powder was very small (d(59) equal 0,5 mym) and the thermal expansion coefficient was near to that of alumina.

Published
1994

14. Pediatrics Clinical Research

Author

Wrede, B., primary, Peters, O., additional, Kordes, U., additional, Kutluk, T., additional, Hasselblatt, M., additional, Rytting, M., additional, Rutkowski, S., additional, Mahajan, A., additional, Pietsch, T., additional, Thall, P., additional, Wolff, J. E., additional, Pfister, S., additional, Bingham, R., additional, Vats, T., additional, Rokes, C., additional, Brown, R., additional, Creach, K. M., additional, Rubin, J. B., additional, Leonard, J. R., additional, Limbrick, D. D., additional, Smyth, M. D., additional, Dacey, R. G., additional, Rich, K. M., additional, Dowling, J. L., additional, Linette, G. P., additional, King, A. A., additional, Michalski, J. M., additional, Simpson, J. R., additional, Park, T. S., additional, Perry, A., additional, Mansur, D. B., additional, Gururangan, S., additional, Panandikar, A. P., additional, Broniscer, A., additional, Huang, A., additional, Kellie, S., additional, Ellison, D., additional, Gajjar, A., additional, Aguilera, D., additional, Goldman, S., additional, Tomita, T., additional, Fangusaro, J., additional, Poussaint, T. Y., additional, Onar, A., additional, Gilbertson, R., additional, Packer, R., additional, McClendon, R., additional, Friedman, H., additional, Boyett, J., additional, Baker, J. N., additional, Tagen, M., additional, Onar-Thomas, A., additional, Gilbertson, R. J., additional, Davidoff, A. M., additional, Pai-Panandiker, A., additional, Leung, W., additional, Chin, T. K., additional, Stewart, C. F., additional, Kocak, M., additional, Rowland, C., additional, Merchant, T. E., additional, Kaste, S., additional, Allen, J., additional, Donahue, B., additional, Mathew, J., additional, Kretschmar, C., additional, Pollack, I., additional, Jakacki, R., additional, Massimino, M., additional, Biassoni, V., additional, Gandola, L., additional, Ferroli, P., additional, Bongarzone, I., additional, Spreafico, F., additional, Pecori, E., additional, Schiavello, E., additional, Modena, P., additional, Bach, F., additional, Potepan, P., additional, Slavc, I., additional, Peyrl, A., additional, Czech, T., additional, Haberler, C., additional, Dieckmann, K., additional, Brown, R. J., additional, Dhall, G., additional, Marachelian, A., additional, Gozali, A., additional, Butturini, A., additional, Gilles, F., additional, Thompson, S. J., additional, Gardner, S., additional, Finlay, J. L., additional, Eisenstat, D. D., additional, and Evans, A., additional

Published
2010
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23. Severe ototoxicity following carboplatin-containing conditioning regimen for autologous marrow transplantation for neuroblastoma.

Author

Parsons, S K, Neault, M W, Lehmann, L E, Brennan, L L, Eickhoff, C E, Kretschmar, C S, and Diller, L R

Subjects
OTOTOXIC agents, BONE marrow transplantation, NEUROBLASTOMA
Abstract

Children with neuroblastoma receiving high-dose carboplatin as part of their conditioning regimen for autologous marrow transplantation have a high incidence of speech frequency hearing loss. We evaluated hearing loss in 11 children with advanced stage neuroblastoma who underwent autologous marrow transplantation, following a conditioning regimen containing high-dose carboplatin (2 g/m2, total dose). Audiometric evaluations were obtained at diagnosis, prior to and following transplant. Exposure to other known ototoxins also was assessed. All patients sustained worsening of hearing following high-dose carboplatin. Nine of the 11 children (82%) had evidence of speech frequency hearing loss post transplant for which hearing aids were recommended (grades 3–4). Three of the nine children had speech frequency loss prior to transplant which progressed following transplant. The entire group was heavily pre-treated with platinum-containing chemotherapy pre-BMT and had extensive exposure to other ototoxins, including aminoglycoside antibiotics, diuretics, and noise exposure – all of which could have exacerbated the effects of carboplatin. High-dose carboplatin is ototoxic, particularly in patients who have been primed with previous platinum therapy or other ototoxic agents. We conclude that further efforts are needed to monitor and minimize this complication. In cases where hearing loss is inevitable due to cumulative ototoxic exposures, families need to be adequately prepared for the tradeoffs of potentially curable therapy. [ABSTRACT FROM AUTHOR]

Published
1998
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27. Des wackern Biegleins edler Liebe sey dieses schlechte Blat geweyht Indem Er mit entflammtem Triebe Der Fürstenauin Weyrauch streut

Author

Hamberger, J. E., Manteufel, C. L. von, Alardus, C. N., Brincken, H. B. de, Brock, A. F. von, Carstens, J. J., Eberhardt, M. A. von, Einsidel, C. H. H. von, Erasmus, J. J., Evers, C. D., Fabricius, C. G., Fabricius, J. W., Fick, J. S., Pfeilitzer, F. de, Hartmann, G. S., Hopfensack, P. P., Jeremias, J. E., Koch, J., Koerner, J. E., Kretschmar, C. H., Osten, C. C. von der, Hamberger, J. E., Manteufel, C. L. von, Alardus, C. N., Brincken, H. B. de, Brock, A. F. von, Carstens, J. J., Eberhardt, M. A. von, Einsidel, C. H. H. von, Erasmus, J. J., Evers, C. D., Fabricius, C. G., Fabricius, J. W., Fick, J. S., Pfeilitzer, F. de, Hartmann, G. S., Hopfensack, P. P., Jeremias, J. E., Koch, J., Koerner, J. E., Kretschmar, C. H., and Osten, C. C. von der

Abstract

[Der gesamte Fechtboden. C. C. v. der Osten, genannt Sacken, Curon. J. E. Hamberger, Jensens. C. L. v. Manteufel, Curon. C. N. Alardus, Holsat. H. B. de Brincken, Equ. Curon. A. F. v. Brock, Bremens. J. J. Carstens, Lubecens. M. A. v. Eberhardt, aus Schlesien. C. H. H. v. Einsidel, eq. Misnic. J. J. Erasmus, Argent. C. D. Evers, Lubecens. C. G. Fabricius, Curon. J. W. Fabricius, Palatin. J. S. Fick, Jenens. F. de Pfeilitzer, dit. Frank. Curon. G. S. Hartmann, Curon. P. P. Hopfensack, Palat. J. E. Jeremias, aus Chursachs. J. Koch. Jenens. J. E. Koerner, Coronac. C. H. Kretschmar, siles. ...], Es weren insgesamt 42 Beiträger genannt, Autopsie nach Ex. der ULB Sachsen-Anhalt, Vorlageform des Erscheinungsvermerks: Jena, Gedruckt bey Johann Friedrich Schill, 1746.

28. Des wackern Biegleins edler Liebe sey dieses schlechte Blat geweyht Indem Er mit entflammtem Triebe Der Fürstenauin Weyrauch streut

Author

Hamberger, J. E., Manteufel, C. L. von, Alardus, C. N., Brincken, H. B. de, Brock, A. F. von, Carstens, J. J., Eberhardt, M. A. von, Einsidel, C. H. H. von, Erasmus, J. J., Evers, C. D., Fabricius, C. G., Fabricius, J. W., Fick, J. S., Pfeilitzer, F. de, Hartmann, G. S., Hopfensack, P. P., Jeremias, J. E., Koch, J., Koerner, J. E., Kretschmar, C. H., Osten, C. C. von der, Hamberger, J. E., Manteufel, C. L. von, Alardus, C. N., Brincken, H. B. de, Brock, A. F. von, Carstens, J. J., Eberhardt, M. A. von, Einsidel, C. H. H. von, Erasmus, J. J., Evers, C. D., Fabricius, C. G., Fabricius, J. W., Fick, J. S., Pfeilitzer, F. de, Hartmann, G. S., Hopfensack, P. P., Jeremias, J. E., Koch, J., Koerner, J. E., Kretschmar, C. H., and Osten, C. C. von der

Abstract

[Der gesamte Fechtboden. C. C. v. der Osten, genannt Sacken, Curon. J. E. Hamberger, Jensens. C. L. v. Manteufel, Curon. C. N. Alardus, Holsat. H. B. de Brincken, Equ. Curon. A. F. v. Brock, Bremens. J. J. Carstens, Lubecens. M. A. v. Eberhardt, aus Schlesien. C. H. H. v. Einsidel, eq. Misnic. J. J. Erasmus, Argent. C. D. Evers, Lubecens. C. G. Fabricius, Curon. J. W. Fabricius, Palatin. J. S. Fick, Jenens. F. de Pfeilitzer, dit. Frank. Curon. G. S. Hartmann, Curon. P. P. Hopfensack, Palat. J. E. Jeremias, aus Chursachs. J. Koch. Jenens. J. E. Koerner, Coronac. C. H. Kretschmar, siles. ...], Es weren insgesamt 42 Beiträger genannt, Autopsie nach Ex. der ULB Sachsen-Anhalt, Vorlageform des Erscheinungsvermerks: Jena, Gedruckt bey Johann Friedrich Schill, 1746.

33. PKD2 regulates autophagy and forms a protein complex with BECN1 at the primary cilium of hypothalamic neuronal cells.

Author

García-Navarrete C, Kretschmar C, Toledo J, Gutiérrez K, Hernández-Cáceres MP, Budini M, Parra V, Burgos PV, Lavandero S, Morselli E, Peña-Oyarzún D, and Criollo A

Subjects
Animals, Mice, Autophagy, Beclin-1 metabolism, Cilia metabolism, Hypothalamus metabolism, Hypothalamus cytology, Neurons metabolism, TRPP Cation Channels metabolism, TRPP Cation Channels genetics
Abstract

The primary cilium, hereafter cilium, is an antenna-like organelle that modulates intracellular responses, including autophagy, a lysosomal degradation process essential for cell homeostasis. Dysfunction of the cilium is associated with impairment of autophagy and diseases known as "ciliopathies". The discovery of autophagy-related proteins at the base of the cilium suggests its potential role in coordinating autophagy initiation in response to physiopathological stimuli. One of these proteins, beclin-1 (BECN1), it which is necessary for autophagosome biogenesis. Additionally, polycystin-2 (PKD2), a calcium channel enriched at the cilium, is required and sufficient to induce autophagy in renal and cancer cells. We previously demonstrated that PKD2 and BECN1 form a protein complex at the endoplasmic reticulum in non-ciliated cells, where it initiates autophagy, but whether this protein complex is present at the cilium remains unknown. Anorexigenic pro-opiomelanocortin (POMC) neurons are ciliated cells that require autophagy to maintain intracellular homeostasis. POMC neurons are sensitive to metabolic changes, modulating signaling pathways crucial for controlling food intake. Exposure to the saturated fatty acid palmitic acid (PA) reduces ciliogenesis and inhibits autophagy in these cells. Here, we show that PKD2 and BECN1 form a protein complex in N43/5 cells, an in vitro model of POMC neurons, and that both PKD2 and BECN1 locate at the cilium. In addition, our data show that the cilium is required for PKD2-BECN1 protein complex formation and that PA disrupts the PKD2-BECN1 complex, suppressing autophagy. Our findings provide new insights into the mechanisms by which the cilium controls autophagy in hypothalamic neuronal cells., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published
2024
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34. Calcitriol Treatment Decreases Cell Migration, Viability and β-Catenin Signaling in Oral Dysplasia.

Author

Peña-Oyarzún D, Guzmán C, Kretschmar C, Torres VA, Maturana-Ramirez A, Aitken J, and Reyes M

Abstract

Nearly 90% of oral cancers are characterized as oral squamous cell carcinoma (OSCC), representing the sixth most common type of cancer. OSCC usually evolves from oral potentially malignant disorders that, in some cases, are histologically consistent with a oral dysplasia. The levels of 1α,25 dihydroxyvitamin D3 (1,25-(OH)2D3; calcitriol), the active form of vitamin D3, have been shown to be decreased in patients with oral dysplasia and OSCC. Moreover, treatment with 1,25-(OH)2D3 has been proven beneficial in OSCC by inhibiting the Wnt/β-catenin pathway, a signaling route that promotes cell migration, proliferation, and viability. However, whether this inhibition mechanism occurs in oral dysplasia is unknown. To approach this question, we used dysplastic oral keratinocyte cultures and oral explants (ex vivo model of oral dysplasia) treated with 1,25-(OH)2D3 for 48 h. Following treatment with 1,25-(OH)2D3, both in vitro and ex vivo models of oral dysplasia showed decreased levels of nuclear β-catenin by immunofluorescence (IF) and immunohistochemistry (IHC). Consistently, reduced protein and mRNA levels of the Wnt/β-catenin target gene survivin were observed after treatment with 1,25-(OH)2D3. Moreover, 1,25-(OH)2D3 promoted membranous localization of E-cadherin and nuclear localization of vitamin D receptor (VDR). Functionally, DOK cells treated with 1,25-(OH)2D3 displayed diminished cell migration and viability in vitro.

Published
2024
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35. Inhibition of PORCN Blocks Wnt Signaling to Attenuate Progression of Oral Carcinogenesis.

Author

Peña-Oyarzún D, Flores T, Torres VA, Quest AFG, Lobos-González L, Kretschmar C, Contreras P, Maturana-Ramírez A, Criollo A, and Reyes M

Subjects
Humans, Wnt Signaling Pathway, beta Catenin genetics, beta Catenin metabolism, Squamous Cell Carcinoma of Head and Neck, Carcinogenesis genetics, Acyltransferases metabolism, Acyltransferases pharmacology, Membrane Proteins metabolism, Carcinoma, Squamous Cell drug therapy, Carcinoma, Squamous Cell genetics, Mouth Neoplasms drug therapy, Head and Neck Neoplasms
Abstract

Purpose: Oral squamous cell carcinoma (OSCC) is commonly preceded by potentially malignant lesions, referred to as oral dysplasia. We recently reported that oral dysplasia is associated with aberrant activation of the Wnt/β-catenin pathway, due to overexpression of Wnt ligands in a Porcupine (PORCN)-dependent manner. Pharmacologic inhibition of PORCN precludes Wnt secretion and has been proposed as a potential therapeutic approach to treat established cancers. Nevertheless, there are no studies that explore the effects of PORCN inhibition at the different stages of oral carcinogenesis., Experimental Design: We performed a model of tobacco-induced oral cancer in vitro, where dysplastic oral keratinocytes (DOK) were transformed into oral carcinoma cells (DOK-TC), and assessed the effects of inhibiting PORCN with the C59 inhibitor. Similarly, an in vivo model of oral carcinogenesis and ex vivo samples derived from patients diagnosed with oral dysplasia and OSCC were treated with C59., Results: Both in vitro and ex vivo oral carcinogenesis approaches revealed decreased levels of nuclear β-catenin and Wnt3a, as observed by immunofluorescence and IHC analyses. Consistently, reduced protein and mRNA levels of survivin were observed after treatment with C59. Functionally, treatment with C59 in vitro resulted in diminished cell migration, viability, and invasion. Finally, by using an in vivo model of oral carcinogenesis, we found that treatment with C59 prevented the development of OSCC by reducing the size and number of oral tumor lesions., Conclusions: The inhibition of Wnt ligand secretion with C59 represents a feasible treatment to prevent the progression of early oral lesions toward OSCC., (©2023 American Association for Cancer Research.)

Published
2024
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36. Methods for studying primary cilia in heart tissue after ischemia-reperfusion injury.

Author

Kretschmar C, Hernández-Cáceres MP, Reyes M, Peña-Oyarzún D, García-Navarrete C, Troncoso R, Díaz-Castro F, Budini M, Morselli E, Riquelme JA, Hill JA, Lavandero S, and Criollo A

Subjects
Mice, Animals, Cilia metabolism, Heart, Fibrosis, Myocytes, Cardiac metabolism, Myocardium, Myocardial Reperfusion Injury metabolism, Myocardial Reperfusion Injury pathology, Myocardial Infarction
Abstract

Cardiovascular diseases are the leading cause of death and disability worldwide. After heart injury triggered by myocardial ischemia or myocardial infarction, extensive zones of tissue are damaged and some of the tissue dies by necrosis and/or apoptosis. The loss of contractile mass activates a series of biochemical mechanisms that allow, through cardiac remodeling, the replacement of the dysfunctional heart tissue by fibrotic material. Our previous studies have shown that primary cilia, non-motile antenna-like structures at the cell surface required for the activation of specific signaling pathways, are present in cardiac fibroblasts and required for cardiac fibrosis induced by ischemia/reperfusion (I/R) in mice. I/R-induced myocardial fibrosis promotes the enrichment of ciliated cardiac fibroblasts where the myocardial injury occurs. Given discussions about the existence of cilia in specific cardiac cell types, as well as the functional relevance of studying cilia-dependent signaling in cardiac fibrosis after I/R, here we describe our methods to evaluate the presence and roles of primary cilia in cardiac fibrosis after I/R in mice., Competing Interests: Disclosure statement No potential conflict of interest was reported by the authors., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published
2023
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37. Palmitic acid control of ciliogenesis modulates insulin signaling in hypothalamic neurons through an autophagy-dependent mechanism.

Author

Ávalos Y, Hernández-Cáceres MP, Lagos P, Pinto-Nuñez D, Rivera P, Burgos P, Díaz-Castro F, Joy-Immediato M, Venegas-Zamora L, Lopez-Gallardo E, Kretschmar C, Batista-Gonzalez A, Cifuentes-Araneda F, Toledo-Valenzuela L, Rodriguez-Peña M, Espinoza-Caicedo J, Perez-Leighton C, Bertocchi C, Cerda M, Troncoso R, Parra V, Budini M, Burgos PV, Criollo A, and Morselli E

Subjects
Animals, Autophagy, Cilia metabolism, Humans, Hypothalamus metabolism, Insulin metabolism, Mice, Neurons metabolism, Palmitic Acid metabolism, Palmitic Acid pharmacology, Pro-Opiomelanocortin metabolism, Pro-Opiomelanocortin pharmacology, Diabetes Mellitus, Type 2 metabolism, Insulin Resistance genetics
Abstract

Palmitic acid (PA) is significantly increased in the hypothalamus of mice, when fed chronically with a high-fat diet (HFD). PA impairs insulin signaling in hypothalamic neurons, by a mechanism dependent on autophagy, a process of lysosomal-mediated degradation of cytoplasmic material. In addition, previous work shows a crosstalk between autophagy and the primary cilium (hereafter cilium), an antenna-like structure on the cell surface that acts as a signaling platform for the cell. Ciliopathies, human diseases characterized by cilia dysfunction, manifest, type 2 diabetes, among other features, suggesting a role of the cilium in insulin signaling. Cilium depletion in hypothalamic pro-opiomelanocortin (POMC) neurons triggers obesity and insulin resistance in mice, the same phenotype as mice deficient in autophagy in POMC neurons. Here we investigated the effect of chronic consumption of HFD on cilia; and our results indicate that chronic feeding with HFD reduces the percentage of cilia in hypothalamic POMC neurons. This effect may be due to an increased amount of PA, as treatment with this saturated fatty acid in vitro reduces the percentage of ciliated cells and cilia length in hypothalamic neurons. Importantly, the same effect of cilia depletion was obtained following chemical and genetic inhibition of autophagy, indicating autophagy is required for ciliogenesis. We further demonstrate a role for the cilium in insulin sensitivity, as cilium loss in hypothalamic neuronal cells disrupts insulin signaling and insulin-dependent glucose uptake, an effect that correlates with the ciliary localization of the insulin receptor (IR). Consistently, increased percentage of ciliated hypothalamic neuronal cells promotes insulin signaling, even when cells are exposed to PA. Altogether, our results indicate that, in hypothalamic neurons, impairment of autophagy, either by PA exposure, chemical or genetic manipulation, cause cilia loss that impairs insulin sensitivity., (© 2022. The Author(s).)

Published
2022
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38. PKD2/polycystin-2 induces autophagy by forming a complex with BECN1.

Author

Peña-Oyarzun D, Rodriguez-Peña M, Burgos-Bravo F, Vergara A, Kretschmar C, Sotomayor-Flores C, Ramirez-Sarmiento CA, De Smedt H, Reyes M, Perez W, Torres VA, Morselli E, Altamirano F, Wilson CAM, Hill JA, Lavandero S, and Criollo A

Subjects
Beclin-1 metabolism, Blotting, Western, Fluorescent Antibody Technique, HEK293 Cells, HeLa Cells, Humans, Immunoprecipitation, TRPP Cation Channels metabolism, Autophagy, Beclin-1 physiology, TRPP Cation Channels physiology
Abstract

Macroautophagy/autophagy is an intracellular process involved in the breakdown of macromolecules and organelles. Recent studies have shown that PKD2/PC2/TRPP2 (polycystin 2, transient receptor potential cation channel), a nonselective cation channel permeable to Ca 2+ that belongs to the family of transient receptor potential channels, is required for autophagy in multiple cell types by a mechanism that remains unclear. Here, we report that PKD2 forms a protein complex with BECN1 (beclin 1), a key protein required for the formation of autophagic vacuoles, by acting as a scaffold that interacts with several co-modulators via its coiled-coil domain (CCD). Our data identified a physical and functional interaction between PKD2 and BECN1, which depends on one out of two CCD domains (CC1), located in the carboxy-terminal tail of PKD2. In addition, depletion of intracellular Ca 2+ with BAPTA-AM not only blunted starvation-induced autophagy but also disrupted the PKD2-BECN1 complex. Consistently, PKD2 overexpression triggered autophagy by increasing its interaction with BECN1, while overexpression of PKD2 D509V , a Ca 2+ channel activity-deficient mutant, did not induce autophagy and manifested diminished interaction with BECN1. Our findings show that the PKD2-BECN1 complex is required for the induction of autophagy, and its formation depends on the presence of the CC1 domain of PKD2 and on intracellular Ca 2+ mobilization by PKD2. These results provide new insights regarding the molecular mechanisms by which PKD2 controls autophagy. Abbreviations : ADPKD: autosomal dominant polycystic kidney disease; ATG: autophagy-related; ATG14/ATG14L: autophagy related 14; Baf A1: bafilomycin A 1 ; BCL2/Bcl-2: BCL2 apoptosis regulator; BCL2L1/BCL-XL: BCL2 like 1; BECN1: beclin 1; CCD: coiled-coil domain; EBSS: Earle's balanced salt solution; ER: endoplasmic reticulum; GAPDH: glyceraldehyde-3-phosphate dehydrogenase; GFP: green fluorescent protein; GOLGA2/GM130: golgin A2; GST: glutathione s-transferase; LAMP1: lysosomal associated membrane protein 1; MAP1LC3/LC3: microtubule associated protein 1 light chain 3; MTORC1: mechanistic target of rapamycin kinase complex 1; NBR1: NBR1 autophagy cargo receptor; PIK3C3/VPS34: phosphatidylinositol 3-kinase catalytic subunit type 3; PKD2/PC2: polycystin 2, transient receptor potential cation channel; RTN4/NOGO: reticulon 4; RUBCN/RUBICON: rubicon autophagy regulator; SQSTM1/p62: sequestosome 1; UVRAG: UV radiation resistance associated; WIPI2: WD repeat domain, phosphoinositide interacting 2.

Published
2021
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39. Role of Autophagy in the Microenvironment of Oral Squamous Cell Carcinoma.

Author

Peña-Oyarzún D, Reyes M, Hernández-Cáceres MP, Kretschmar C, Morselli E, Ramirez-Sarmiento CA, Lavandero S, Torres VA, and Criollo A

Abstract

Oral squamous cell carcinoma, the most common type of oral cancer, affects more than 275,000 people per year worldwide. Oral squamous cell carcinoma is very aggressive, as most patients die after 3 to 5 years post-diagnosis. The initiation and progression of oral squamous cell carcinoma are multifactorial: smoking, alcohol consumption, and human papilloma virus infection are among the causes that promote its development. Although oral squamous cell carcinoma involves abnormal growth and migration of oral epithelial cells, other cell types such as fibroblasts and immune cells form the carcinoma niche. An underlying inflammatory state within the oral tissue promotes differential stress-related responses that favor oral squamous cell carcinoma. Autophagy is an intracellular degradation process that allows cancer cells to survive under stress conditions. Autophagy degrades cellular components by sequestering them in vesicles called autophagosomes, which ultimately fuse with lysosomes. Although several autophagy markers have been associated with oral squamous cell carcinoma, it remains unclear whether up- or down-regulation of autophagy favors its progression. Autophagy levels during oral squamous cell carcinoma are both timing- and cell-specific. Here we discuss how autophagy is required to establish a new cellular microenvironment in oral squamous cell carcinoma and how autophagy drives the phenotypic change of oral squamous cell carcinoma cells by promoting crosstalk between carcinoma cells, fibroblasts, and immune cells., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2020 Peña-Oyarzún, Reyes, Hernández-Cáceres, Kretschmar, Morselli, Ramirez-Sarmiento, Lavandero, Torres and Criollo.)

Published
2020
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40. New emerging roles of Polycystin-2 in the regulation of autophagy.

Author

Peña-Oyarzun D, Batista-Gonzalez A, Kretschmar C, Burgos P, Lavandero S, Morselli E, and Criollo A

Subjects
Animals, Humans, Protein Processing, Post-Translational, TRPP Cation Channels chemistry, Autophagy, TRPP Cation Channels metabolism
Abstract

Polycystin-2 (PC2) is a calcium channel that can be found in the endoplasmic reticulum, the plasmatic membrane, and the primary cilium. The structure of PC2 is characterized by a highly ordered C-terminal tail with an EF-motif (calcium-binding domain) and a canonical coiled-coil domain (CCD; interaction domain), and its activity is regulated by interacting partners and post-translational modifications. Calcium mobilization into the cytosol by PC2 has been mainly associated with cell growth and differentiation, and therefore mutations or dysfunction of PC2 lead to renal and cardiac consequences. Interestingly, PC2-related pathologies are usually treated with rapamycin, an autophagy stimulator. Autophagy is an intracellular degradation process where recycling material is sequestered into autophagosomes and then hydrolyzed by fusion with a lysosome. Interestingly, several studies have provided evidence that PC2 may be required for autophagy, suggesting that PC2 maintains a physiologic catabolic state., (© 2020 Elsevier Inc. All rights reserved.)

Published
2020
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41. Polycystin-2 Is Required for Starvation- and Rapamycin-Induced Atrophy in Myotubes.

Author

Kretschmar C, Peña-Oyarzun D, Hernando C, Hernández-Moya N, Molina-Berríos A, Hernández-Cáceres MP, Lavandero S, Budini M, Morselli E, Parra V, Troncoso R, and Criollo A

Abstract

Muscle atrophy involves a massive catabolism of intracellular components leading to a significant reduction in cellular and tissue volume. In this regard, autophagy, an intracellular mechanism that degrades proteins and organelles, has been implicated with muscle breakdown. Recently, it has shown that polycystin-2 (PC2), a membrane protein that belongs to the transient receptor potential (TRP) family, is required for the maintenance of cellular proteostasis, by regulating autophagy in several cell types. The role of PC2 in the control of atrophy and autophagy in skeletal muscle remains unknown. Here, we show that PC2 is required for the induction of atrophy in C2C12 myotubes caused by nutrient deprivation or rapamycin exposure. Consistently, overexpression of PC2 induces atrophy in C2C12 myotubes as indicated by decreasing of the myogenic proteins myogenin and caveolin-3. In addition, we show that inhibition of mTORC1, by starvation or rapamycin is inhibited in cells when PC2 is silenced. Importantly, even if PC2 regulates mTORC1, our results show that the regulation of atrophy by PC2 is independent of autophagy. This study provides novel evidence regarding the role of PC2 in skeletal muscle cell atrophy.

Published
2019
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42. Hyperosmotic stress stimulates autophagy via polycystin-2.

Author

Peña-Oyarzun D, Troncoso R, Kretschmar C, Hernando C, Budini M, Morselli E, Lavandero S, and Criollo A

Abstract

Various intracellular mechanisms are activated in response to stress, leading to adaptation or death. Autophagy, an intracellular process that promotes lysosomal degradation of proteins, is an adaptive response to several types of stress. Osmotic stress occurs under both physiological and pathological conditions, provoking mechanical stress and activating various osmoadaptive mechanisms. Polycystin-2 (PC2), a membrane protein of the polycystin family, is a mechanical sensor capable of activating the cell signaling pathways required for cell adaptation and survival. Here we show that hyperosmotic stress provoked by treatment with hyperosmolar concentrations of sorbitol or mannitol induces autophagy in HeLa and HCT116 cell lines. In addition, we show that mTOR and AMPK, two stress sensor proteins involved modulating autophagy, are downregulated and upregulated, respectively, when cells are subjected to hyperosmotic stress. Finally, our findings show that PC2 is required to promote hyperosmotic stress-induced autophagy. Downregulation of PC2 prevents inhibition of hyperosmotic stress-induced mTOR pathway activation. In conclusion, our data provide new insight into the role of PC2 as a mechanosensor that modulates autophagy under hyperosmotic stress conditions., Competing Interests: CONFLICTS OF INTEREST The authors declare that no competing interests exist.

Published
2017
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43. [Pilot study of psychiatric and social aspects of children and adolescents with fragile X syndrome].

Author

Häßler F, Gaese F, Colla M, Huss M, Kretschmar C, Brinkman M, Peters H, Elstner S, Weirich S, and Pittrow D

Subjects
Adolescent, Child, Combined Modality Therapy, Comorbidity, Cost of Illness, Female, Fragile X Syndrome epidemiology, Fragile X Syndrome therapy, Germany, Humans, Male, Mental Disorders diagnosis, Mental Disorders epidemiology, Mental Disorders therapy, Neurologic Examination, Pilot Projects, Prospective Studies, Risk Factors, Emotional Adjustment, Emotional Intelligence, Fragile X Syndrome diagnosis, Fragile X Syndrome psychology, Mental Disorders psychology
Abstract

Objective: The study describes the burden of psychosocial risks of mental illnesses and the ways in which children and adolescents with fragile X syndrome (FRX) can be treated., Method: Data from a sample of 34 patients with FRX younger than 18 years stemming from a prospective multicenter (n = 11) registry study (EXPLAIN) were analyzed with regard to psychosocial burden and Treatment., Results: One third of all participants reported having relatives who suffer from FRX. The majority of participants were suffering themselves from one kind or another mental or neurological problems. Younger participants (< 14 years) tended to suffer from atactic disorders, epileptic seizures, and autistic symptoms. These disorders were usually treated by psychotropic drugs supplemented by logopedic therapies and occupational therapies (more than once a month). In our sample, 96.3 % of the younger patients and more than 57.1 % of the older patients were still living with their parents., Conclusions: Patients with FRX often suffer from additional neurological and mental disorders. For that reason, they should be diagnosed and treated early on.

Published
2017
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44. Characterization, treatment patterns, and patient-related outcomes of patients with Fragile X syndrome in Germany: final results of the observational EXPLAIN-FXS study.

Author

Haessler F, Gaese F, Huss M, Kretschmar C, Brinkman M, Peters H, Elstner S, Colla M, and Pittrow D

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Europe, Female, Follow-Up Studies, Fragile X Syndrome complications, Germany, Humans, Male, Mental Disorders complications, Mental Disorders psychology, Middle Aged, Phenotype, Prospective Studies, Registries, Seizures complications, Seizures psychology, Young Adult, Cost of Illness, Fragile X Syndrome psychology, Fragile X Syndrome therapy, Patient Outcome Assessment
Abstract

Background: As data on the phenotype, characteristics and management of patients with Fragile X Syndrome (FXS) are limited, we aimed to collect such data in Germany in experienced centres involved in the treatment of such patients., Methods: EXPLAIN-FXS is a prospective observational (non-interventional) study (registry) performed between April 2013 and January 2016 at 18 sites in Germany. Requirements for patient participation included confirmed diagnosis of FXS by genetic testing (>200 CGG repeats) and written informed consent. Patients were followed for up to 2 years., Results: Seventy-five patients (84.0 % males, mean age 16.7 ± 14.5 years, ranging from 2 - 82 years) were analysed. The mean 6-item score, determined according to Giangreco (J Pediatr 129:611-614, 1996), was 6.9 ± 2.5 points. At least one neurological finding each was noted in 53 patients (69.7 %). Specifically, ataxia was noted in 5 patients (6.6 %), lack of fine motor skills in 40 patients, (52.6 %), muscle tonus disorder in 4 patients (5.3 %), and other neurological disorders in 39 patients (51.3 %). Spasticity was not noted in any patient. Seizures were reported in 6 patients (8.1 %), anxiety disorders in 22 patients (30.1 %), depression in 7 patients (9.6 %), ADHD/ADD in 36 patients (49.3 %), impairment of social behavior in 39 patients (53.4 %), and other comorbidities in 23 patients (31.5 %). The mean Aberrant Behaviour Checklist Community Edition (ABC-C) score on behavioral symptoms, obtained in 71 patients at first documentation, was 48.4 ± 27.8 (median 45.0, range 5-115). The mean visual analogue scale (VAS) score, obtained in 59 patients at first documentation, was 84.9 ± 14.6 points (median 90; range 50 - 100)., Conclusions: This report describes the largest cohort of patients with FXS in Europe. The reported observations indicate a substantial burden of disease for patients and their caregivers. Based on these observations, an early expert psychiatric diagnosis is recommended for suspected FXS patients. Further recommendations include multimodal and multi-professional management that is tailored to the individual patient's needs., Trial Registration: The ClinTrials.gov identifier is NCT01711606 . Registered on 18 October 2012.

Published
2016
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45. [Psychiatric and Social Aspects of Patients with Fragile X Syndrome].

Author

Pittrow D, Gaese F, Colla M, Huss M, Kretschmar C, Brinkman M, Peters H, Elstner S, Weirich S, and Häßler F

Subjects
Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Combined Modality Therapy, Cost of Illness, Female, Fragile X Syndrome diagnosis, Fragile X Syndrome genetics, Fragile X Syndrome therapy, Genetic Predisposition to Disease genetics, Germany, Humans, Intellectual Disability diagnosis, Intellectual Disability genetics, Intellectual Disability therapy, Male, Mental Disorders diagnosis, Mental Disorders genetics, Mental Disorders therapy, Middle Aged, Prospective Studies, Registries, Young Adult, Fragile X Syndrome psychology, Intellectual Disability psychology, Mental Disorders psychology
Abstract

Objective: The goal of the study was to describe the burden of psychosocial risks, of mental illnesses and the ways of treatment of patients with fragile X syndrome (FRX)., Method: Data from a sample of 46 FRX-patients stemming from a prospective multicenter (N = 12) registry study (EXPLAIN) were analyzed with regard to psychosocial burden and treatment., Results: More than 50 % of all participants reported about relatives suffering from FRX, too. The majority of participants did not finish school and was suffering from one or another kind of mental problems. Younger participants (< 18 yrs.) tended to suffer from expansive disorders. Older participants were rather burdened by internalizing symptoms and disorders. Disorders were usually treated by psychotropic drugs added by logopedic therapies and occupational therapies (more than once a month). In our sample 90.6 % of younger and more than 64.3 % of older patients were still living with their parents., Conclusions: Patients with FRX often suffer from additional mental disorders and should be diagnosed and treated early., (© Georg Thieme Verlag KG Stuttgart · New York.)

Published
2016
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46. EXPLAIN Fragile-X: an explorative, longitudinal study on the characterization, treatment pathways, and patient-related outcomes of Fragile X Syndrome.

Author

Haessler F, Gaese F, Colla M, Huss M, Kretschmar C, Brinkman M, Schieb H, Peters H, Elstner S, and Pittrow D

Subjects
Disease Progression, Female, Germany, Humans, Longitudinal Studies, Male, Prospective Studies, Research Design, Treatment Outcome, Fragile X Syndrome diagnosis, Fragile X Syndrome therapy
Abstract

Background: Fragile X syndrome (FXS), caused by a mutation of the FMR1 gene on the X chromosome, is the most common inherited form of intellectual disability and autism spectrum disorders. Comprehensive data are lacking, however, on the characteristics and management patients with FXS in Germany., Methods/design: EXPLAIN is a prospective, observational, longitudinal registry with a non-probability sampling approach. It collects data on patient characteristics, therapeutic interventions, psychosocial parameters (including those of family members and caregivers), quality of life of caregiver and patient, caregiver burden, and health economic parameters, such as hospitalisation time. It is designed to include data from 300 patients in ambulatory care from about 50 centres that employ psychiatrists, paediatricians, neurologists, and other relevant specialists, in Germany. The study was initiated in March, 2013. Patients will be followed for at least two years., Discussion: The registry is expected to provide much-needed data on the characteristics and management of patients with FXS in Germany. It will also allow comparisons with other countries, and will enable gap analyses based on current guidelines for management of these patients., Trial Registration: The ClinicalTrials.gov identifier is NCT01711606.

Published
2013
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47. Diagnostic sensitivity of serum and lumbar CSF bHCG in newly diagnosed CNS germinoma.

Author

Allen J, Chacko J, Donahue B, Dhall G, Kretschmar C, Jakacki R, Holmes E, and Pollack I

Subjects
Adolescent, Adult, Central Nervous System Neoplasms blood, Central Nervous System Neoplasms cerebrospinal fluid, Child, Child, Preschool, Female, Germinoma blood, Germinoma cerebrospinal fluid, Humans, Male, Sensitivity and Specificity, Young Adult, alpha-Fetoproteins analysis, Biomarkers, Tumor analysis, Central Nervous System Neoplasms diagnosis, Chorionic Gonadotropin, beta Subunit, Human cerebrospinal fluid, Germinoma diagnosis
Abstract

Background: Marked elevations of AFP and bHCG in serum or CSF may serve as surrogate diagnostic markers in lieu of histology for primary CNS mixed, malignant germ cell tumors. There is less information on the diagnostic sensitivity of bHCG assays in germinoma., Procedure: We report baseline serum and lumbar CSF bHCG values in 58 newly diagnosed, histologically confirmed germinoma patients gathered from two prospective clinical trials which required that patients have a normal AFP and bHCG ≤50 mIU/ml in serum and lumbar CSF., Results: The location of the primary tumors was: suprasellar(23); pineal(20); suprasellar/pineal(9); and other sites(6). The mean age of the study population was 13.5 (4.3-25.9) years. A total of 23(40%) patients had elevations of bHCG in either serum or CSF, 20(34.5%) of whom had only bHCG elevations in CSF. The patients' bHCG profiles were divided into four categories: I (normal serum and lumbar CSF bHCG), 35(60%); II (normal serum and elevated CSF bHCG), 20(34.5%); III (elevated serum and CSF bHCG), 2(3.5%); and IV (elevated serum and normal CSF bHCG), 1(2%). The median CSF bHCG level was 7.7(2.5-16) in the 22 patients with abnormal CSF values and the lumbar value was higher than the serum value in 20 of 23(87%) patients with bHCG elevations., Conclusions: Lumbar CSF was a more informative screen for bHCG than serum but the majority of patients (60%) had normal bHCG values at diagnosis. Until a more sensitive tumor marker for germinoma is devised, histologic confirmation remains the standard of care. Pediatr Blood Cancer 2012; 59: 1180-1182. © 2012 Wiley Periodicals, Inc., (Copyright © 2012 Wiley Periodicals, Inc.)

Published
2012
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48. Feasibility of a tandem autologous peripheral blood stem cell transplant regimen for high risk neuroblastoma in a cooperative group setting: a Pediatric Oncology Group study: a report from the Children's Oncology Group.

Author

Granger M, Grupp SA, Kletzel M, Kretschmar C, Naranjo A, London WB, and Diller L

Subjects
Antineoplastic Combined Chemotherapy Protocols adverse effects, Child, Child, Preschool, Disease-Free Survival, Humans, Infant, Male, Survival Rate, Transplantation, Autologous, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Neuroblastoma mortality, Neuroblastoma therapy, Peripheral Blood Stem Cell Transplantation
Abstract

Background: The Pediatric Oncology Group performed a pilot study to assess the feasibility of tandem high dose chemotherapy (HDC) with stem cell rescue (HDC/SCR). We report here the results of this single arm trial of induction chemotherapy, local control measures (surgery and local radiation), and tandem HDC/SCR., Procedure: Patients with high risk neuroblastoma (NBL) underwent five cycles of induction chemotherapy and resection of primary tumors. Peripheral blood stem cells (PBSC) were collected after Course 3 without exvivo manipulation. Myeloablative chemotherapy was performed in rapid sequence after induction chemotherapy and surgery. The ability of patients to complete both cycles of HDC/SCR was a primary endpoint. Transplant-related toxicity, progression-free survival (PFS) and overall survival (OS) were recorded., Results: A total of 33 patients were enrolled. Twenty-two patients completed at least one HDC/SCR procedure and 17 patients completed both. Only one patient had insufficient stem cells collected for both transplants. There was one transplant-related death; engraftment was rapid and toxicity was as expected. The PFS of the 33 patients treated on this study is 24.2% ± 7.5% and OS is 36.4% ± 8.4% at 5 years. For patients who received at least one transplant PFS is 36.4% ± 11.0% and OS is 45.5% ± 11.2% at 5 years., Conclusions: The treatment of high risk NBL with tandem HDC/SCR is feasible in terms of transplant-related mortality and the ability to collect adequate PBSC for two transplants. The outcomes from this intensified treatment have been used to design a Children's Oncology Group Phase III study testing the efficacy of tandem HDC/SCR., (Copyright © 2012 Wiley Periodicals, Inc.)

Published
2012
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49. Phase II study of irinotecan and temozolomide in children with relapsed or refractory neuroblastoma: a Children's Oncology Group study.

Author

Bagatell R, London WB, Wagner LM, Voss SD, Stewart CF, Maris JM, Kretschmar C, and Cohn SL

Subjects
Adolescent, Antineoplastic Combined Chemotherapy Protocols adverse effects, Camptothecin administration & dosage, Camptothecin adverse effects, Camptothecin analogs & derivatives, Child, Child, Preschool, Dacarbazine administration & dosage, Dacarbazine adverse effects, Dacarbazine analogs & derivatives, Disease-Free Survival, Female, Humans, Infant, Irinotecan, Male, Temozolomide, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Neuroblastoma drug therapy
Abstract

Purpose: This phase II study was conducted to determine the response rate associated with use of irinotecan and temozolomide for children with relapsed/refractory neuroblastoma., Patients and Methods: Patients with relapsed/refractory neuroblastoma measurable by cross-sectional imaging (stratum 1) or assessable by bone marrow aspirate/biopsy or metaiodobenzylguanidine (MIBG) scan (stratum 2) received irinotecan (10 mg/m(2)/dose 5 days a week for 2 weeks) and temozolomide (100 mg/m(2)/dose for 5 days) every 3 weeks. Response was assessed after three and six courses using International Neuroblastoma Response Criteria. Of the first 25 evaluable patients on a given stratum, five or more patients with complete or partial responses were required to conclude that further study would be merited., Results: Fifty-five eligible patients were enrolled. The objective response rate was 15%. Fourteen patients (50%) on stratum 1 and 15 patients (56%) on stratum 2 had stable disease. Objective responses were observed in three of the first 25 evaluable patients on stratum 1 and five of the first 25 evaluable patients on stratum 2. Less than 6% of patients experienced ≥ grade 3 diarrhea. Although neutropenia was observed, less than 10% of patients developed evidence of infection while neutropenic., Conclusion: The combination of irinotecan and temozolomide was well tolerated. The objective response rate of 19% in stratum 2 suggests that this combination may be effective for patients with neuroblastoma detectable by MIBG or marrow analysis. Although fewer objective responses were observed in patients with disease measurable by computed tomography/magnetic resonance imaging, patients in both strata seem to have derived clinical benefit from this therapy.

Published
2011
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50. Outcome of patients with recurrent medulloblastoma or central nervous system germinoma treated with low dose continuous intravenous etoposide along with dose-intensive chemotherapy followed by autologous hematopoietic stem cell rescue.

Author

Grodman H, Wolfe L, and Kretschmar C

Subjects
Adolescent, Adult, Anemia chemically induced, Anemia therapy, Antineoplastic Combined Chemotherapy Protocols adverse effects, Carboplatin administration & dosage, Central Nervous System Neoplasms mortality, Child, Child, Preschool, Female, Germinoma mortality, Hematologic Diseases chemically induced, Hematologic Diseases therapy, Humans, Infusions, Intravenous, Male, Neoplasm Recurrence, Local mortality, Survival Rate, Thiotepa administration & dosage, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Central Nervous System Neoplasms therapy, Etoposide administration & dosage, Germinoma therapy, Hematopoietic Stem Cell Transplantation, Neoplasm Recurrence, Local therapy
Abstract

Background: Adults and children with recurrent malignant central nervous system (CNS) tumors have a poor prognosis despite high dose chemotherapy with a conventional stem cell rescue regimen. In this study we evaluated the results of low dose, continuous infusion etoposide over 21 days added to a conventional high-dose regimen of carboplatin and thiotepa in eight patients with relapsed pediatric CNS tumors., Procedure: Patients with high risk CNS tumors were treated with etoposide 25 mg/m(2)/day by continuous intravenous (IV) infusion from day -22 to day -2, carboplatin 667 mg/m(2)/dose IV (or area under the curve = 9 mg/ml/min according to the Calvert formula on days -8, -7, and -6, and thiotepa 300 mg/m(2)/dose IV on days -5, -4, and -3, followed by autologous hematopoietic stem cell rescue on day 0., Results: Eight adults and children, with a mean age of 12.9 years (age range 5.6-27.8 years), with relapsed primary CNS tumors (metastatic medulloblastoma (7), germinoma (1)), were enrolled. The mean survival post-transplant was 4.8+ years, (range 8-160+ months). The 2- and 5-year overall survival rates were 75% and 50% respectively. None of the survivors required additional salvage irradiation., Conclusion: The strategy of low dose chronic exposure to a topoisomerase inhibitor along with ablative carboplatin and thiotepa with stem cell rescue showed promising survival outcomes in these relapsed patients. This treatment strategy deserves further evaluation in a larger group of high-risk or relapsed primary CNS tumors., (Copyright 2009 Wiley-Liss, Inc.)

Published
2009
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