Microwave-enhanced in situ end-labeling of fragmented DNA: parametric studies in relation to postmortem delay and fixation of rat and human brainPJ Lucassen, WC Chung, JP Vermeulen, M Van Lookeren Campagne, JH Van Dierendonck and DF Swaab Graduate School Neurosciences Amsterdam, Netherlands Institute for Brain Research, The Netherlands. In situ end-labeling (ISEL) identifies DNA fragmentation in apoptotic or necrotic nuclei in tissue sections. However, application of ISEL on human brain requires conservation of DNA integrity during the postmortem delay (PMD) and good accessibility of fragmented DNA after (prolonged) tissue fixation. We therefore investigated ISEL in relation to PMD and fixation in rat and human brain. Application on a unilateral lesion model in perfused rat brain revealed that prolonged post- fixation strongly diminished ISEL results. However, microwave pre- treatment can counteract these masking effects without inducing nonspecific labeling contralaterally. On the other hand, in briefly post-fixed, perfused brain or immersion-fixed rat and human PMD brain, microwave pre-treatment was deleterious and induced strong nonspecific labeling. In young rat brain, PMD did not influence the low numbers of apoptotic nuclei until 24 hr PMD, when massive nuclear labeling occurred. In human cortex, DNA fragmentation patterns were independent of duration of fixation or PMD and were already present from 4.25 hr PMD onwards. Our data suggest that ISEL on human brain represents antemortem DNA damage rather than PMD artifacts. Furthermore, microwave pre-treatment appears beneficial only in particular fixation conditions.
Volume 43,
Issue 11,
pp. 1163-1171,
11/01/1995
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P. P. H. Van Sloun, I. Varlet, E. Sonneveld, J. J. W. A. Boei, R. J. Romeijn, J. C. J. Eeken, and N. De Wind Involvement of Mouse Rev3 in Tolerance of Endogenous and Exogenous DNA Damage Mol. Cell. Biol., April 1, 2002; 22(7): 2159 - 2169. [Abstract] [Full Text] [PDF] |
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H.-K. Hsu, R.-C. Yang, H.-C. Shih, Y.-L. Hsieh, U-Y. Chen, and C. Hsu Prenatal Exposure of Testosterone Prevents SDN-POA Neurons of Postnatal Male Rats From Apoptosis Through NMDA Receptor J Neurophysiol, November 1, 2001; 86(5): 2374 - 2380. [Abstract] [Full Text] [PDF] |
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P. J. Lucassen, M. B. Muller, F. Holsboer, J. Bauer, A. Holtrop, J. Wouda, W. J. G. Hoogendijk, E. R. De Kloet, and D. F. Swaab Hippocampal Apoptosis in Major Depression Is a Minor Event and Absent from Subareas at Risk for Glucocorticoid Overexposure Am. J. Pathol., February 1, 2001; 158(2): 453 - 468. [Abstract] [Full Text] [PDF] |
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B.-F. Chen, M.-L. Chen, D.-C. Liang, H.-C. Liu, and S.-H. Chen The Relationship of N-myc Amplification and Apoptosis in Neuroblastoma International Journal of Surgical Pathology, January 1, 1999; 7(1): 19 - 25. [Abstract] [PDF] |
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F. Labat-Moleur, C. Guillermet, P. Lorimier, C. Robert, S. Lantuejoul, E. Brambilla, and A. Negoescu TUNEL Apoptotic Cell Detection in Tissue Sections: Critical Evaluation and Improvement J. Histochem. Cytochem., March 1, 1998; 46(3): 327 - 334. [Abstract] [Full Text] |
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B. G. Short, D. M. Zimmerman, and L. W. Schwartz Automated Double Labeling of Proliferation and Apoptosis in Glutathione S-transferase-positive Hepatocytes in Rats J. Histochem. Cytochem., September 1, 1997; 45(9): 1299 - 1306. [Abstract] [Full Text] [PDF] |
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S.-R. Shi, R. J. Cote, and C. R. Taylor Antigen Retrieval Immunohistochemistry: Past, Present, and Future J. Histochem. Cytochem., March 1, 1997; 45(3): 327 - 344. [Abstract] [Full Text] [PDF] |
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