Expression of Nuclear Factor-Kappa B and Placental Apoptosis in Pregnancies Complicated with Intrauterine Growth Restriction and Preeclampsia: An Immunohistochemical Study

Aban, Meral; Cinel, Leyla; Arslan, Murat; Dilek, Umut; Kaplanoğlu, Mustafa; Arpacı, Rabia Bozdoğan; Dılek, Saffet

doi:10.1620/tjem.204.195

Cited by 65 publications

(52 citation statements)

References 31 publications

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“…Similarly at both 95% and 21% oxygen, but not at 8% oxygen, M30 staining increased between the incubation time points of 6 h and 24 h. M30 antibody, as an apoptotic detection marker, has proven to be superior to the TUNEL method for the detection of apoptosis in villous and extravillous trophoblast (Kadyrov et al 2001). These findings are supported by those previously described in placentae recovered from pregnancies complicated by preeclampsia, which is associated with a significantly higher M30 index than that measured in control placentas (Aban et al 2004;Lee et al 2005). Thus, in summary, hyperoxic conditions have been shown significantly to increase apoptosis in human term placental explants in vitro.…”

Section: Discussionsupporting

confidence: 84%

Effect of high oxygen on placental function in short-term explant cultures

et al. 2007

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Ex situ culture of human gestational tissues has been routinely used as a model to investigate tissue function. The objective of this study was to determine the effect of varying oxygen concentrations on human term placental explants over a 24-h time period. Specifically, the effect of incubating placental explants in oxygen concentrations of 8%, 21% or 95% on tissue viability, metabolism and cell death was measured by assessing glucose consumption, lactate production, release of lactate dehydrogenase, parathyroid hormone-related protein (PTHrP), tumour necrosis factor-alpha (TNF-alpha) and 8-isoprostane, immunoreactivity for cleaved-caspase-9 and immunohistochemistry for the caspase-3-cleaved cytokeratin-18 neoepitope, M30. Exposure to higher oxygen concentrations significantly increased the rates of glucose consumption and lactate production. Apoptosis was significantly increased under conditions of higher oxygen as evidenced by increased M30 in placental explant sections. Similarly, hyperoxia significantly increased the releases of PTHrP, TNF-alpha and 8-isoprostane. Thus, incubation of placental explants with oxygen concentrations of 95% and, to a lesser extent, 21% oxygen was associated with the modulation of multiple cellular response pathways including those associated with tissue viability and cell death. These data are consistent with the hypothesis that hyperoxia activates pathways and mechanisms involved in cellular metabolism, necrosis and apoptosis, thereby shifting the balance from a steady state towards cell death.

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Section: Discussionsupporting

confidence: 84%

Effect of high oxygen on placental function in short-term explant cultures

et al. 2007

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“…These findings agreed with those of Aban et al who researched complicated pregnancies. 26 Bax immunoreactivity was negative in cytotrophoblasts and mesenchymal cells and was mild in syncytiotrophoblasts in the control group; whereas moderate response was observed cytototrophoblasts and syncytiotrophoblasts and mild response in mesenchymal cells in hypothyroid placentas. These findings correlate with findings of Cobellis et al who investigated apoptosis in growth retardation as a consequence of pre-eclampsia.…”

Section: Control Groupmentioning

confidence: 69%

“…Caspase-3 is involved in the development of apoptotic cell death. [21][22][23][24][25][26] An abnormal level of apoptosis has also been correlated with a large variety of gestational pathologies such as in the placentas of abortions, ectopic pregnancy, intrauterine growth retardation, post-term pregnancy, pre-eclampsia and maternal hypertension syndrome. 17,[27][28][29] Apoptosis has occasionally been observed in histological sections of normal thyroid.…”

mentioning

confidence: 99%

Maternal Hypothyroidism and Its Rolein the Placenta: A Morphometric andImmunohistochemical Study

Özoğul¹,

Mıçılı²,

Baykara³

et al. 2010

Turkiye Klinikleri J Med Sci

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A AB BS S T TR RA AC CT T O Ob bj je ec ct ti iv ve e: : The aim of this study was to in ves ti ga te the struc tu re and mec ha nism of apop to sis in pla cen tas with ma ter nal hypoth yro i dism. M Ma a t te e r ri i a al l a an nd d M Me et t h ho od ds s: : Se ven nor mal and eight hypoth yro i dic mot hers we re se lec ted. Tis su es we re pre pa red for his toc he mistry, im mu no his toc hemistry and TU NEL as say for de tec ti on of apop to sis and struc tu ral chan ges. R Re e s su ul lt ts s: : In cre a sed TU NELpo si ti ve sta i ning in the cytot rop hob last, syncyti ot rop hob last and me sench ymal cells was shown in the pla cen tas of the hypoth yro id gro up in com pa ri son to the con trol gro up. In the con trol gro up, po si ti ve im mu nos ta i ning for Cas pa se-3 was mo de ra te in the syncyti ot rop hob last cells, whi le it was mild in the cytot rop hob last cells and it was ne ga ti ve in the me sench ymal cells. Im mu nos ta i ning for Bcl-2 was mo de ra te in the syncyti ot rop hob last, cytot rop hob last and me sench ymal cells. Bax im mu nosta i ning was ne ga ti ve in the cytot rop hob last and me sench ymal cells, whi le im mu nos ta i ning was mild in the syncyti ot rop hob last. In the hypoth yro id gro up, Cas pa se-3 im mu nos ta i ning was strong in the syncyti ot rop hob last, cytot rop hob last and me sench ymal cells, whe re as Bcl-2 im mu nos ta i ning was ab sent in the cytot rop hob lasts, and mild in the syncyti ot rop hob lasts and me sench ymal cells. Bax im mu nos ta i ning was mo de ra te in the syncyti ot rop hob lasts and cytot rop hob lasts, ho we ver it was mild in the me sench ymal cells. The me an num ber of syncyti al knots was sig ni fi cantly lo wer in the con trol gro up than the hypoth yro id gro up (p< 0.05). Me an thick ness of me di um si ze blo od ves sels was sig ni fi cantly lo wer in the hypoth yro id gro up than the con trol gro up (p< 0.05). Me an are a of stro mal fib ro sis de mons tra ted in the hypoth yro id gro up was hig her than the con trol gro up (p< 0.05). C Co on nc c l lu u s si i o on n: : We conc lu de that sig ni fi cant his to lo gi cal chan ges oc cur in the pla cen tas of hypoth yroid mot hers with as so ci a ted high in ci den ce of apop to tic mar ker res pon se. K Ke ey y W Wo or rd ds s: : Hypothyroidism; apoptosis; placenta; histology Ö ÖZ ZE ET T A Am ma aç ç: : Bu ça lış ma nın ama cı, ma ter nal hi po ti ro i di zim li pla sen ta la rın ya pı sı nı ve apop to zi sin me ka niz ma sı nı araş tır mak tır. G Ge e r re eç ç v ve e Y Yö ön n t te em m l le er r: : Bu amaç la ye di nor mal ve se kiz hi po ti ro i dik anne se çil di. Do ku lar apop to zi si ve ya pı sal de ği şik lik le ri araş tır mak üze re his to kim ya, im mü no his tokim ya ve TU NEL işa ret le me için ha zır lan dı. B Bu ul l g gu u l la ar r: : Hi po ti ro i dik grup pla sen ta lar kon trol gru bu pla sen ta lar ile kar şı laş tı rıl dı ğın da TU NEL po zi tif si tot ro fob last, sin sit yot ro fob last ve me zen şi mal hüc re sa yı sı nın art tı ğı be...

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“…The diagnosis of IUGR was based on three criteria: ultrasonographic deviation from the normal growth percentile, clinically detected suboptimal growth and having birth weight less than the 10th percentile of the corresponding gestational age (Aban et al, 2004).…”

Section: Methodsmentioning

confidence: 99%