Permanent Anatomic Closure of the Ductus Arteriosus in Newborn Baboons: The Roles of Postnatal Constriction, Hypoxia, and Gestation

Clyman, Ronald I.; Chan, Cecilia Y.; Mauray, Françoise; Chen, Yao Qi; Cox, Wesley J.; Seidner, S; Lord, Edith M.; Weiss, Hali E.; Waleh, Nahid; Evans, Sydney M.; Koch, Cameron J.

doi:10.1203/00006450-199901000-00005

Cited by 129 publications

(175 citation statements)

References 30 publications

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“…As a result of the constriction, the inner muscle wall of the ductus arteriosus develops profound ischemic hypoxia which leads to the formation of vascular endothelial growth factor, transforming growth factorbeta, and other inflammatory mediators and growth factors that transform the ductus into a non-contractile ligament. 3 Conversely, in preterm infants, the ductus often fails to constrict in the days following birth. Even in those preterm infants who achieve ductus constriction, the ductus frequently fails to develop the level of profound hypoxic ischemia needed to cause remodeling of the artery.…”

Section: Pathophysiologymentioning

confidence: 99%

“…When this occurs, the center of the ductus wall becomes profoundly ischemic. 3 In the premature (24 week gestation) ductus, the vessel wall is only about 200 mm in thickness (Figure 2). The scattered vasa vasorum in the vessel lie in the adventitia and do not penetrate the muscle media.…”

Section: Pathophysiologymentioning

confidence: 99%

“…As a result, the preterm ductus arteriosus is less likely to develop the severe degree of hypoxia that is necessary for ductus remodeling. 3 In order for the preterm ductus to develop the degree of ischemia needed to set up the remodeling cascade, it is essential that it develop complete luminal obliteration and complete elimination of nutrient flow to its wall.…”

Section: Pathophysiologymentioning

confidence: 99%

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Patent ductus arteriosus: pathophysiology and management

2006

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Patent ductus arteriosus (PDA) in preterm newborns prior to 28 weeks of gestation has led to many challenges regarding the type and timing of treatment regimens. A PDA results in increased pulmonary blood flow and redistribution of flow to other organs. Several co-morbidities (i.e., necrotizing enterocolitis, intracranial hemorrhage, pulmonary edema/ hemorrhage, bronchopulmonary dysplasia, and retinopathy) are associated with the presence of a PDA, but whether or not a PDA is responsible for their development is still unclear. The prostaglandin inhibitor, indomethacin, is effective in the treatment of PDA. Questions regarding the optimal timing of the intervention -early prophylaxis or treatment, once signs and symptoms become evident -have challenged physicians for decades. Both evidence and experience are explored in this article. Comparative physiology between the full-term and preterm newborn and the barriers preventing the necessary cascade of events leading to permanent constriction of the PDA are reviewed.

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Section: Pathophysiologymentioning

confidence: 99%

Section: Pathophysiologymentioning

confidence: 99%

Section: Pathophysiologymentioning

confidence: 99%

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Patent ductus arteriosus: pathophysiology and management

2006

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“…[1][2][3][4] The physiological mechanism involved in this process are now beginning to be understood. 1,24,25 The presence of sPDA in our study represents a combination of failure of the ductus to close and the reopening of a previously closed ductus. Postnatally, many factors are known to influence the temporary or permanent closure of a ductus arteriosus.…”

Section: Discussionmentioning

confidence: 81%

The effects of indomethacin tocolysis on the postnatal response of the ductus arteriosus to indomethacin in extremely low birth weight infants

et al. 2006

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Background: Antenal indomethacin reportedly decreases the responses of a symptomatic patent ductus arteriosus (sPDA) to postnatal indomethacin treatment. Whether a similar exposure affects the responses to indomethacin prophylaxis is unknown.Objective: To evaluate the clinical responsiveness of ductus arteriosus to indomethacin prophylaxis and to the treatment of sPDA in extremely low birth weight (ELBW) infants following indomethacin tocolysis.Methods: Retrospective cohort study of 58 ELBW infants whose mothers received indomethacin tocolysis (study) and 58 ELBW infants whose mothers did not (controls), matched by gender, gestational age (GA), birth weight and postnatal sPDA management (prophylaxis or early treatment).Results: Indomethacin was used as a tocolytic at a median dose of 250 mg, for a duration of 2 days, and ending 1 day before delivery. Study and control mothers were comparable in demographics, antenatal steroid use, cesarean delivery, but were different in the incidence of preeclampsia and preterm labor. Study and control infants were similar in birth weight, GA, indomethacin prophylaxis, early sPDA treatment, mortality, necrotizing enterocolitis, severe intraventricular hemorrhage and stage 3-5 retinopathy of prematurity. Seventeen of 43 study and 16 of 43 control infants who received indomethacin prophylaxis developed sPDA and were combined with early treatment sPDA infants (15 to each group). Two of 32 study and two of 31 control infants underwent surgical ligation whereas the remaining were treated with indomethacin. Sixteen of 30 (53%) and 13 of 29 (45%) were successfully treated and did not require ligation. Study infants were divided according to their mothers' indomethacin total dose (28 infants received p225 mg and 30 infants received >225 mg). Both subgroups were demographically and clinically comparable and their response to indomethacin prophylaxis and treatment were similar. Conclusion:In ELBW infants, exposure to indomethacin tocolysis does not affect the clinical responsiveness of the ductus arteriosus to prophylaxis or that of the sPDA to indomethacin treatment.

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“…1,14,17 It is possible that in some preterm infants, whether spontaneously or indomethacin mediated, the ductus arteriosus frequently fails to develop the level of profound ischemia needed to cause remodeling, thus allowing the vessel to remain open, or if it is already closed, to reopen. 1,17,18 Satisfactory clinical responses to postnatal indomethacin treatment for sPDA are expected to be about 50% for infants at 24 to 25 weeks of GA and 60% or higher for those ELBW infants of older GA. 3,19 In the present study, successful indomethacin treatment of sPDA was noted in 38% of indomethacin prophylaxis infants and in 59% of those managed expectantly. It is possible that indomethacin prophylaxis, although failing to prevent an sPDA, may have preselected a group of infants that having failed once are predisposed to fail a second indomethacin treatment.…”

Section: Discussionmentioning

confidence: 99%

Indomethacin prophylaxis or expectant treatment of patent ductus arteriosus in extremely low birth weight infants?

et al. 2007

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Background: Indomethacin prophylaxis or expectant treatment are common strategies for the prevention or management of symptomatic patent ductus arteriosus (sPDA). Objective:To compare the clinical responses of extremely low birth weight (ELBW) infants to indomethacin prophylaxis with hat of other infants who were managed expectantly by being treated with indomethacin or surgically only after an sPDA was detected.Methods: Retrospective cohort investigation of 167 ELBW infants who received indomethacin prophylaxis (study) and 167 ELBW infants (control) treated expectantly who were matched by year of birth (1999 to 2006), birth weight, gestational age (GA) and gender.Results: Mothers of the two groups of infants were comparable demographically and on the history of preterm labor, pre-eclampsia, antepartum steroids and cesarean delivery. Study and control infants were similar in birth weight, GA, low 5 min Apgar scores, surfactant administration, the need for arterial blood pressure control, bronchopulmonary dysplasia and neonatal mortality. Necrotizing enterocolitis, spontaneous intestinal perforations, intraventricular hemorrhage grade III to IV, periventricular leukomalacia and stage 3 to 5 retinopathy of prematurity occurred also with similar frequency in both groups of infants. In the indomethacin prophylaxis group, 29% of the infants developed sPDA, and of them 38% responded to indomethacin treatment. In the expectantly treated group, 37% developed sPDA, and of them 59% responded to indomethacin treatment. Overall, surgical ligation rate for sPDA was similar between both groups of patients.Conclusion: In our experience, indomethacin prophylaxis does not show any advantages over expectant early treatment on the management of sPDA in ELBW infants. Although no deleterious effects were observed, prophylaxis exposed a significant number of infants who may have never developed sPDA, to potential indomethacin-related complications.

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Permanent Anatomic Closure of the Ductus Arteriosus in Newborn Baboons: The Roles of Postnatal Constriction, Hypoxia, and Gestation

Cited by 129 publications

References 30 publications

Patent ductus arteriosus: pathophysiology and management

Patent ductus arteriosus: pathophysiology and management

The effects of indomethacin tocolysis on the postnatal response of the ductus arteriosus to indomethacin in extremely low birth weight infants

Indomethacin prophylaxis or expectant treatment of patent ductus arteriosus in extremely low birth weight infants?

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