Peculiar Fibronectin immunohistochemical staining in placental tissue of pathological pregnancies associated with insufficient placentation

A Fruscalzo; M Orsaria; AP Londero; S Marzinotto; N Nardini; L Driul; L Mariuzzi

doi:10.1055/s-0035-1566683

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Z Geburtshilfe Neonatol 2015; 219 - P09_13
DOI: 10.1055/s-0035-1566683

Peculiar Fibronectin immunohistochemical staining in placental tissue of pathological pregnancies associated with insufficient placentation

A Fruscalzo ¹, M Orsaria ², AP Londero ³, S Marzinotto ², N Nardini ², L Driul ⁴, L Mariuzzi ²

¹St. Franziskus-Hospital Münster, Klinik für Gynäkologie und Geburtshilfe, Münster, Germany
²University of Udine, Institute of Pathology, Udine, Italy
³S. Polo Hospital, Obstetrics and Gynecology, Monfalcone, Italy
⁴University of Udine, Obstetrics and Gynecology, Udine, Italy

Congress Abstract

Objective: To investigate the role of Fibronectin, an extracellular matrix protein essential in the process of trophoblastic invasion, in the development of pregnancy-related pathologies associated with insufficient placentation.

Materials and methods: Retrospective study including 36 early (< 34^th gestational age) preeclampsia (PE), 14 late (≥34^th gestational age) PE, 6 HELLP syndrome (hemolysis, elevated liver enzymes, low platelet count), 18 small for gestational age (SGA) fetuses (under the 10^th percentile), 17 early intrauterine growth restriction (IUGR), 35 late IUGR, and 64 controls. Fibronectin localization was evaluated in placental tissue microarray by immunohistochemistry and the amount assessed by intensity semi-quantitative score (3 = strong, 2 = moderate, and 1 = weak).

Results: Fibronectin was present in cytoplasm and peri-cytoplasm areas. Moreover, in general Fibronectin cytoplasm staining had a higher intensity score among cases compared to controls. Furthermore, both cytoplasm and peri-cytoplasm Fibronectin intensity was higher in early PE (1, IQR 0 – 1), HELLP (1, IQR 1 – 1), and early IUGR (1, IQR 1 – 1) than in controls of 22 – 34 weeks' gestation (0, IQR 0 – 1) (p < 0.05). Intensity was also greater in late PE (1, IQR 0 – 1) than late IUGR (0, IQR 0 – 0) and controls (0, IQR 0 – 1) of 34 – 42 weeks' gestation, as well as in late PE associated with IUGR (1, IQR 0 – 1) than in IUGR alone (0, IQR 0 – 0) and in early IUGR (1, IQR 1 – 1) than late IUGR (0, IQR 0 – 0) (p < 0.05). In addition, peri-cytoplasmic Fibronectin was found to be significantly more represented in late PE associated with IUGR (2, IQR 1 – 2) than in controls (1, IQR 0 – 1) (p < 0.05).

Conclusions: Fibronectin shows higher staining among PE, HELLP and IUGR cases compared to controls, probably reflecting a common underlying pathological mechanism coupled with insufficient placentation. Late IUGR seems to be unaffected by Fibronectin amount, suggesting a peculiar pathogenetic pattern.