Acute thymic involution in fetuses and neonates with chorioamnionitis

Chorioamnionitis represents the leading cause of preterm birth and related pathologic conditions as well as of fetal death and frequently occurs in symptom-free mothers. Recent radiologic findings have indicated that thymus size is significantly reduced in preterm infants born to mothers with subcli...

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Bibliographic Details
Published in:Human pathology 2000-09, Vol.31 (9), p.1121-1128
Main Authors: Toti, Paolo, De Felice, Claudio, Stumpo, Michela, Schürfeld, Karin, Leo, Luigi Di, Vatti, Rosella, Bianciardi, Giorgio, Buonocore, Giuseppe, Seemayer, Thomas A., Luzi, Pietro
Format: Article
Language:English
Subjects:
Abortion, Spontaneous
Abortion, Therapeutic
Acute Disease
Adult
Atrophy
Biological and medical sciences
Biomarkers - analysis
Chorioamnionitis - complications
Chorioamnionitis - pathology
Diseases of mother, fetus and pregnancy
Female
Gestational Age
Gynecology. Andrology. Obstetrics
Humans
Immunohistochemistry
Infant, Newborn
Lymphocytes - metabolism
Lymphocytes - pathology
Medical sciences
Pregnancy
Pregnancy. Fetus. Placenta
Retrospective Studies
Sepsis - complications
Sepsis - pathology
Thymus Gland - metabolism
Thymus Gland - pathology
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Description
Summary:Chorioamnionitis represents the leading cause of preterm birth and related pathologic conditions as well as of fetal death and frequently occurs in symptom-free mothers. Recent radiologic findings have indicated that thymus size is significantly reduced in preterm infants born to mothers with subclinical, histologically proven chorioamnionitis. However, an accurate morphologic description of the thymus gland in fetuses and neonates with chorioamnionitis is lacking, although it is known that infection and other stress processes may cause lymphocyte depletion in the thymuses of infants and older babies (acute stress involution). We describe morphologic modifications in the thymus of fetuses with histologically proven chorioamnionitis and newborn infants with chorioamnionitis and proven sepsis. The main findings included (1) decreased organ volume (ANOVA, P < .0024); (2) reduced corticomedullary ratio ( P 10 −6); (3) significant changes in the relationship between thymic parenchyma and thymic interstitial tissue with resulting increased organ complexity ( P = .03); (4) severe reduction of thymocytes; and (5) other degenerative processes such as monocyte/macrophage infiltration of Hassall's bodies. These results indicate that chorioamnionitis, with or without sepsis, is associated with significant morphologic modifications in the thymus. We wish to note that the described thymic pathology is only one aspect of the fetal systemic inflammatory response syndrome with which chorioamnionitis is associated. H UM P ATHOL 31:1121-1128.
ISSN:0046-8177
1532-8392
DOI:10.1053/hupa.2000.16676