| Literature DB >> 21151528 |
Laure Dix1, Matthias Roth-Kleiner, Maria-Chiara Osterheld.
Abstract
Necrotizing enterocolitis (NEC) is a severe neonatal disease affecting particularly preterm infants. Its exact pathogenesis still remains unknown. In this study, we have compared the prevalence of vascular obstructive lesions in placentae of premature newborns which developed NEC and of a control group. We further compared separately the findings of placentae of infants of less than 30 weeks of gestation, the age group in which NEC occurs most frequently. We found signs of fetal vascular obstructive lesions in 65% of the placentae of preterm patients developing NEC, compared to only 17% of the placentae of preterm patients in the control group. In the age groups below 30 weeks of gestation, 58.5% of placentae of later NEC patients presented such lesions compared to 24.5% in the control group. The significant difference between NEC and control group suggests a strong association between fetal vascular obstructive lesions and NEC. Therefore, we propose that fetal vascular obstructive lesions might be considered as a risk factor for the development of NEC in premature infants.Entities:
Year: 2010 PMID: 21151528 PMCID: PMC2989861 DOI: 10.4061/2010/838917
Source DB: PubMed Journal: Patholog Res Int ISSN: 2042-003X
Figure 1Characteristic histological findings of placental vascular obstructive lesions (all images colored by hematoxylin and eosin; magnification 40×). (a) Occlusive thrombus (arrow) in a dilated chorionic vein. (b) Hemorrhagic endovasculitis (HEV): extravasated blood cells (arrow) around a vessel in a stem villus. (c) Muscular hypertrophy and old occlusions (arrows) in stem vessels (obliterative endarteritis) (OE). (d) Avascular villi demonstrating hyaline villous stroma devoid of vessels.
FVOL: fetal vascular obstructive lesions defined as placentae with the presence of one or more of the following lesions: MT: multiple thrombi, IT: isolated thrombus, OE: obliterative endarteritis, HEV: hemorrhagic endovasculitis. P-value*: comparison between the three different control groups and the study group* P-value**: comparison between the very preterm control group and the very preterm study group**.
| Total number of placentae | FVOL | Type of vascular obstructive lesions | ||||
|---|---|---|---|---|---|---|
| MT | IT | OE | HEV | |||
| Study group* | 77 | 50 (64.9%) | 30 (39.0%) | 15 (19.5%) | 15 (19.5%) | 11 (14.3%) |
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| Very preterm study group (<30 weeks) ∗ ∗ | 41 | 24 (58.5%) | 14 (34.1%) | 10 (24.4%) | 5 (12.2%) | 3 (7.3%) |
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Control group | 769 | 130 (16.9%) | 37 (4.8%) | 59 (7.7%) | 20 (2.6%) | 25 (3.3%) |
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Preterm control group (<37 weeks) | 279 | 47 (16.8%) | 15 (5.4%) | 27 (9.7%) | 9 (3.2%) | 7 (2.5%) |
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Very preterm control group (<30 weeks) | 53 | 13 (24.5%) | 7 (13.2%) | 5 (9.4%) | 4 (7.5%) | 3 (5.7%) |
Prevalence of chorioamnionitis (CA) and vasculitis in the different study populations. Comparisons are given between vascular obstructive lesions associated with chorioamnionitis, vasculitis, and without these inflammatory conditions. P-value*: comparison between the three different control groups and the corresponding study group. P-value**: comparison between the very preterm control group and the very preterm study group**.
| Number of placentae with CA | Number of placentae with vasculitis | Vascular obstructive lesions | |||
|---|---|---|---|---|---|
| With CA | With vasculitis | Without CA and vasculitis | |||
| Study group* | 16 (20.8%) | 14 (18.2%) | 12 (15.6%) | 9 (11.7%) | 37 (48%) |
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| Very preterm study group (<30 weeks) ∗ ∗ | 12 (29.2%) | 9 (21.9%) | 7 (17%) | 5 (12.2%) | 19 (46.3%) |
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Control group (<37 weeks) | 138 (17.9%) | 101 (13.1%) | 16 (2.1%) | 5 (0.65%) | 93 (12.25%) |
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Preterm control group (<37 weeks) | 29 (10.4%) | 34 (12.2%) | 1 (0.36%) | 1 (0.36%) | 39 (14%) |
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Very preterm control group (<30 weeks) | 32 (60%) | 26 (49%) | 5 (9.4%) | 1 (1.9%) | 7 (13.2%) |