Prenatal Programming of Pulmonary Hypertension Induced by Chronic Hypoxia or Ductal Ligation in Sheep

Papamatheakis, Demosthenes G.; Chundu, Madalitso; Blood, Arlin B.; Wilson, Sean

doi:10.1086/674767

Cited by 16 publications

(22 citation statements)

References 210 publications

(473 reference statements)

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“…Mechanisms and pathways identified using apposite PHN models hypoxia models, in functional reductions in soluble guanylyl cyclase (sGC) function, cyclic guanosine monophosphate (cGMP)-dependent vasorelaxation, increased phosphodiesterase type 5 (PDE5) and enhanced Endothelin-1 (ET-1) contraction. In contrast, significant differences were found in the cellular processes between the two models: a significant decrease in the levels of endothelial nitric oxide synthase (eNOS) and calcium activated potassium channels (BKCa) in ligation models; an increase of these molecules in chronic hypoxia [22] . Other models for PHN are the exposure-based models, including short-term neonatal hyperoxia, fetal and/or post-natal hypoxia and a two-hit model of prenatal hypoxia followed by postnatal hyperoxia.…”

Section: The Relevant Models For Phnmentioning

confidence: 94%

“…Of note are the experimental investigations on animal models, given the inadequate availability of patient tissues and inability to perform mechanistic studies in humans. Several animal PH's models have been developed for performing studies into the functional and structural changes, which occur during the development of pulmonary circulation and PH [21][22][23][24][25][26][27][28][29][30][31][32][33][34] . Unfortunately, to date not a single preclinical model perfectly replicates human PH.…”

Section: Phn and Foetal Programming: Focus On Mechanisms And Pathwaysmentioning

confidence: 99%

“…Some relevant models for PHN have been developed and studied. Of note are the results obtained by the utero ligation of the ductus arteriosus and chronic perinatal hypoxia in sheep fetuses and newborns [22] . They have demonstrated that the mechanisms associated with PH are dependent on the type and grade of stress to which the fetus is subjected [22] .…”

Section: The Relevant Models For Phnmentioning

confidence: 99%

“…Of note are the results obtained by the utero ligation of the ductus arteriosus and chronic perinatal hypoxia in sheep fetuses and newborns [22] . They have demonstrated that the mechanisms associated with PH are dependent on the type and grade of stress to which the fetus is subjected [22] . Specifically, similarities were observed between the ligation and End-products of endothelial-derived nitric oxide (NO) heme-oxidation, nitrate and nitrite produce exogenous NO, which mediates an increased vasoactive signaling activity during hypoxia and stress Alteration in maternal microbiome Table 1.…”

Section: The Relevant Models For Phnmentioning

confidence: 99%

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Fetal programming and its effects on vascular pulmonary circulation

Balistreri

2018

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Into the scientific community, consensus about the emerging concept of "the fetal origin of adult diseases" is growing. It sustains that the parental (of the two parents) adversities, and the related external influences, during the intra-utero/ perinatal life of each eutherian mammal organism, human included, can permanently set the structure and functionality of specific body systems (i.e., immune, endocrine, nervous and cardiovascular systems), predisposing them to early ageing and disease during adulthood. The pulmonary circulation system also appears to be one of its targets. Established evidence supports the strong association between developmental programming and pulmonary arterial remodeling and dysfunction. Here, a revised overview of this topic is reported, by stressing the efforts and advances in identifying the molecular and cellular mechanisms and pathways involved.

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Section: The Relevant Models For Phnmentioning

confidence: 94%

Section: Phn and Foetal Programming: Focus On Mechanisms And Pathwaysmentioning

confidence: 99%

Section: The Relevant Models For Phnmentioning

confidence: 99%

Section: The Relevant Models For Phnmentioning

confidence: 99%

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Fetal programming and its effects on vascular pulmonary circulation

Balistreri

2018

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“…Etiologies of pulmonary hypertension of the neonate are varied and they are not clearly understood, but the condition is marked by a high morbidity and mortality of the presenting newborns. [26][27][28] Chronic in utero exposure to high altitude environment 13,16 and epigenetic factors 29 are some natural causative factors of neonatal pulmonary hypertension. Among other things, the data presented here show that chronic hypoxia exposure alone is sufficient to induce neonatal pulmonary hypertension in support of existing information and further show, for the first time, that chronic neonatal hypoxia exposure contributes to increase in pulmonary vascular tone of newborns.…”

Section: Sds-page Electrophoresismentioning

confidence: 99%

Physiological and Biochemical Consequences of Exposure of Neonatal Rats to Chronic Hypoxia

Ibe

Abdallah

Raj

2020

MRAJ

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We studied effect of chronic hypoxia (CH) on expression of platelet activating factor receptor (PAFR) by neonatal rats (pups). We hypothesized that PAFR antagonist will prevent pulmonary hypertension (PH) in pups exposed to CH. Pups were placed in an air-tight chamber ventilated with 13% oxygen, hypoxia (Hpx) or room air normoxia (Nmx) from 1d to 22d of age. Three groups of pups were studied (each group, n=10-14 pups): Group1, pups in Nmx; Group2, pups in Hpx given 5mg/kg PAFR receptor antagonist, WEB 2170, IP, every other day for 22d, (Hpx+WEB); Group3, pups in Hpx control. Hemotocrit, RV/LV+S, PAF binding, PAF synthesis, and PAFR expression were determined. Hyx control group had 2-fold higher RV/LV+S than Nmx group and PAFR antagonist decreased RV/LV+S to the Nmx control value. Lungs of pups in Hpx expressed more PAFR protein than Hpx+WEB and Nmx groups. Additionally, Hpx increased PAF synthesis and PAFR binding whereas WEB treatment decreased PAFR binding, but produced no difference in PAF synthesis compared to Nmx group. Hpx increased NF-kB p65 and TLR4 expression. WEB treatment abrogated expression or NF-kB p65 and TLR4 proteins. Our findings show that chronic hypoxia induces expression of PAFR, NF-kB p65 and TLR4 by pups’ lungs and suggest that increased PAFR expression may be responsible for the right ventricular hypertrophy and PH. Thus a PAFR antagonist may offer a therapeutic intervention for CH-induced PH in human neonates.

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Developmental programming: Interaction between prenatal BPA and postnatal overfeeding on cardiac tissue gene expression in female sheep

Koneva

Vyas

McEachin

et al. 2017

Environ and Mol Mutagen

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Epidemiologic studies and studies in rodents point to potential risks from developmental exposure to BPA on cardiometabolic diseases. Furthermore, it is becoming increasingly evident that the manifestation and severity of adverse outcomes is the result of interaction between developmental insults and the prevailing environment. Consistent with this premise, recent studies in sheep found prenatal BPA treatment prevented the adverse effects of postnatal obesity in inducing hypertension. The gene networks underlying these complex interactions are not known. mRNA-seq of myocardium was performed on four groups of four female sheep to assess the effects of prenatal BPA exposure, postnatal overfeeding and their interaction on gene transcription, pathway perturbations and functional effects. The effects of prenatal exposure to BPA, postnatal overfeeding, and prenatal BPA with postnatal overfeeding all resulted in transcriptional changes (85–141 significant differentially expressed genes). Although the effects of prenatal BPA and postnatal overfeeding did not involve dysregulation of many of the same genes, they affected a remarkably similar set of biological pathways. Furthermore, an additive or synergistic effect was not found in the combined treatment group, but rather prenatal BPA treatment led to a partial reversal of the effects of overfeeding alone. Many genes previously known to be affected by BPA and involved in obesity, hypertension, or heart disease were altered following these treatments, and AP-1, EGR1, and EGFR were key hubs affected by BPA and/or overfeeding.

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Prenatal Programming of Pulmonary Hypertension Induced by Chronic Hypoxia or Ductal Ligation in Sheep

Cited by 16 publications

References 210 publications

Fetal programming and its effects on vascular pulmonary circulation

Fetal programming and its effects on vascular pulmonary circulation

Physiological and Biochemical Consequences of Exposure of Neonatal Rats to Chronic Hypoxia

Developmental programming: Interaction between prenatal BPA and postnatal overfeeding on cardiac tissue gene expression in female sheep

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