Literature DB >> 12614591

Time course of cortical hemorrhages after closed traumatic brain injury: statistical analysis of posttraumatic histomorphological alterations.

Manfred Oehmichen1, Till Walter, Christoph Meissner, Hans-Jürgen Friedrich.   

Abstract

We examined 305 autopsied brains for histomorphological alterations to determine the time course of reactions in cortical hemorrhages following traumatic closed brain injury. Eighteen morphological criteria were considered: red blood cells (RBCs), polymorphonuclear leukocytes (PMNs), macrophages (Ms), RBC-containing Ms, hemosiderin, hematoidin, lipid-containing Ms, fibroblasts, endothelial cells, collagenous fibres, gemistocytic astrocytes, fibrillary gliosis, hemosiderin-containing astrocytes, neuronal damage, neuronophagy, axonal swelling (beta-amyloid precursor protein: beta-APP), axonal bulbs (van Gieson stain), and mineralisation of neurons. The interval between the time of brain injury and death ranged from 1 min to 58 years. Following routine staining and immunohistochemical staining of microglia (CD68), astrocytes (GFAP) and injured axons (beta-APP), paraffin sections were examined by light microscopy for the presence of the selected histomorphological features. For each cytomorphological phenomenon, the time at which it could be demonstrated for the first time and for the last time (observation period) was determined. The relative frequency of each criterion was established for each observation period. The limits of confidence for the respective relative frequencies were estimated with a reliability of 95% according to Clopper and Pearson. An apparent correlation was found between the frequency of a given histomorphological phenomenon and the length of the posttraumatic interval. To check for accuracy of prediction, half of the cases (group 1; n = 153) were used to develop a multistage evaluation model; half (group 2; n = 152) were used to evaluate the validity of the data of group 1. Applying this model, 117 of the 152 control group cases (76.97%) could be correctly classified and further 26 cases (17.11%) being assigned to an interval close to the correct interval. Thus, this model allows classification of the correct posttraumatic interval or an interval close to the correct posttraumatic interval in about 95% of cases. We developed a software program that allows the estimation of survival time of TBI based on the relative frequency of the 18 morphological features. Applying this software will help to estimate the posttraumatic interval of cortical hemorrhages following TBI of unknown survival time.

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Year:  2003        PMID: 12614591     DOI: 10.1089/08977150360517218

Source DB:  PubMed          Journal:  J Neurotrauma        ISSN: 0897-7151            Impact factor:   5.269


  19 in total

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Review 3.  Neuroimaging biomarkers in mild traumatic brain injury (mTBI).

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Review 6.  The science behind the quest to determine the age of bruises-a review of the English language literature.

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Review 7.  Evidence to support mitochondrial neuroprotection, in severe traumatic brain injury.

Authors:  Shyam Gajavelli; Vishal K Sinha; Anna T Mazzeo; Markus S Spurlock; Stephanie W Lee; Aminul I Ahmed; Shoji Yokobori; Ross M Bullock
Journal:  J Bioenerg Biomembr       Date:  2014-10-31       Impact factor: 2.945

8.  The 70 kDa heat shock protein protects against experimental traumatic brain injury.

Authors:  Jong Youl Kim; Nuri Kim; Zhen Zheng; Jong Eun Lee; Midori A Yenari
Journal:  Neurobiol Dis       Date:  2013-06-29       Impact factor: 5.996

9.  Diffusion tensor imaging reliably detects experimental traumatic axonal injury and indicates approximate time of injury.

Authors:  Christine L Mac Donald; Krikor Dikranian; Philip Bayly; David Holtzman; David Brody
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10.  Time-dependent appearance of intrathrombus neutrophils and macrophages in a stasis-induced deep vein thrombosis model and its application to thrombus age determination.

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Journal:  Int J Legal Med       Date:  2009-02-05       Impact factor: 2.686

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