Placental Pathology in Placental Mesenchymal Dysplasia with 13q12.11 Deletion and a 25-Week Gestation Female Infant

Johnson, Sheryl; Walters-Sen, Lauren; Stanek, Jerzy

doi:10.12659/ajcr.907329

Cited by 7 publications

(8 citation statements)

References 13 publications

(14 reference statements)

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“…[16][17][18] Rarely, unusual placental features can be seen in isolated cases of genetic fetal anomalies and suggest chromosomal anomalies. 9,19,20 In our large unselected population of placentas from the second half of high-risk pregnancy which included also some cases analyzed here, fetal congenital anomalies grouped with oligohydramnios, amnion nodosum, nonmacerated stillbirth, termination of pregnancy, villous hemosiderosis, hydropic placenta, and hypocoiled umbilical cord. 21 In the second trimester, fetal malformations clustered with termination of pregnancy only, in the preterm third trimester, with neonatal mortality, villous hemosiderosis, single umbilical artery, polyhydramnios, and hydropic placenta, while in term pregnancy, with single umbilical artery and nonmacerated stillbirth.…”

Section: Introductionmentioning

confidence: 99%

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Patterns of Placental Injury in Congenital Anomalies in Second Half of Pregnancy

Stanek

2019

Pediatr Dev Pathol

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Background Placental pathology in fetal congenital anomalies in second half of pregnancy is largely unknown. Methods Twenty-six clinical and 45 independent placental phenotypes from pregnancies ≥20 weeks of gestation with congenital anomalies divided into 4 groups were retrospectively compared with analysis of variance or χ 2 with 3 degrees of freedom and with Bonferroni correction for multiple comparisons: group 1 : 112 cases with heart malformations (with or without chromosomal anomalies), group 2 : 41 cases with abnormal karyotypes and anomalies other than heart malformations, group 3 : 87 cases with intrathoracic or intraabdominal mass-forming anomalies (mostly congenital diaphragmatic hernias and adenomatoid airway malformation), and group 4 : 291 miscellaneous cases with mostly skeletal, renal, and central nervous system anomalies not fulfilling the criteria of inclusion into groups 1 to 3. Results Eight of 26 clinical (30.8%) and 16 of 45 (35.5%) placental phenotypes varied statistically significantly among the 4 groups ( P < .05), of those, 7 (26.9%) and 4 (8.9%), respectively, remained statistically significant after Bonferroni correction ( P Bonferroni ≤ .002). Those placental phenotypes were placental weight, chorionic disc chorionic microcysts, fetal vascular ectasia, and luminal vascular abnormalities of chorionic villi. Conclusions Fetal anomalies in second half of pregnancy feature abnormal clinical phenotypes much more frequently than abnormal placental phenotypes. Chromosomal abnormalities with or without heart malformations tend to feature villous edema, and erythroblastosis of fetal blood, likely due to fetal heart failure. Mass-forming fetal anomalies feature placental histological lesions of shallow placental implantation, diffuse chronic hypoxic patterns of placental injury, and lesions of fetal vascular malperfusion, likely stasis-induced.

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Section: Introductionmentioning

confidence: 99%

“…16–18 Rarely, unusual placental features can be seen in isolated cases of genetic fetal anomalies and suggest chromosomal anomalies. 9,19,20…”

Section: Introductionmentioning

confidence: 99%

Patterns of Placental Injury in Congenital Anomalies in Second Half of Pregnancy

Stanek

2019

Pediatr Dev Pathol

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“…There has been only a single reported case of triploidy associated with PMD [36]. Other chromosomally abnormal cases reported included trisomy 13 (47,XX,t(1:13)(q32;q32)+ 13) [37], and a 228kb deletion at 13q12.11 involving the gap junction beta-6 (GJB6) gene detected by single nucleotide polymorphism (SNP) microarray analysis has been reported [38]. In a review study by Cohen MC et al [36] Klinefelter syndrome (47,XXY) has been diagnosed with PMB.…”

Section: Pmd and Fetal Aneuploidymentioning

confidence: 99%

Placental Mesenchymal Dysplasia; Current Understanding of the Sonographic, Histologic, and Molecular Findings of a Rare and Challengin Disorder

Lazebnik

2020

JGWH

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“…Описаны также разнообразные аномалии кариотипа, представленные, как правило, в виде единичных наблюдений (мозаицизм по трисомии 9, трисомия 13, синдром Клайнфелтера, диандрическая триплоидия, материнская делеция GRB10 (7р12.2), делеция GJB6 (13q12.11) и др.) [3,7,8]. Доля мозаичных клеток может значительно различаться, что, вероятно, является основной причиной морфологического и клинического полиморфизма МДП.…”

Section: оригинальные исследования Original Investigationsunclassified

“…Васкуляризация промежуточных и терминальных ворсин в большинстве случаев соответ-строме кистозно-измененных ворсин при сохранении экспрессии в трофобласте, [10,11], описано также очаговое отсутствие экспрессии белка как в цитотрофобласте, так и в строме [12]. В плацентах с делециями GRB10 и GJB6 экспрессия р57 была положительной в трофобласте и строме ворсин [7,8].…”

Section: оригинальные исследованияunclassified

Placental mesenchymal dysplasia

Voloshchuk¹,

Barinova²,

Чечнева³

et al. 2019

Arkh. patol.

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Placental Pathology in Placental Mesenchymal Dysplasia with 13q12.11 Deletion and a 25-Week Gestation Female Infant

Cited by 7 publications

References 13 publications

Patterns of Placental Injury in Congenital Anomalies in Second Half of Pregnancy

Patterns of Placental Injury in Congenital Anomalies in Second Half of Pregnancy

Placental Mesenchymal Dysplasia; Current Understanding of the Sonographic, Histologic, and Molecular Findings of a Rare and Challengin Disorder

Placental mesenchymal dysplasia

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