Effects of Macrolide Antibiotics on Rat Embryonic Heart Function In Vitro

Nilsson, Mats; Webster, William S.

doi:10.1002/bdrb.21107

Cited by 16 publications

(9 citation statements)

References 73 publications

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“…Hypokalemia, hyperthermia, or metabolic acidosis could all potentiate the effect of hypoxia. In a recent systematic review, there was strong evidence that hypokalemia was a risk factor for QT‐prolongation (Vandael et al, ), while hyperthermia has been shown to increase the number of arrhythmias in whole rat embryo culture (Nilsson and Webster, ). In other in vitro models, decreased intracellular pH exacerbated the HR response to hypoxia (Zhou et al, ).…”

Section: Concluding Commentsmentioning

confidence: 99%

“…This was based on its known risk of TdP and two studies from Hungary (Czeizel et al, ) and Sweden (Kallen et al, ) identifying a doubling in incidence of cardiac defects, especially VSDs. Preclinical in vivo animal studies have been negative for erythromycin (Karlsson et al, ), although in vitro embryo culture studies did identify the IKr blocking potential, but only at high concentrations unlikely to occur with oral dosing in humans (Nilsson and Webster, ). A follow‐up Swedish study confirmed the association with cardiac defects (Källén and Danielsson, ), but others have been largely negative (Cooper et al, ; Crider et al, ; Romoren et al, ; Lin et al, ).…”

Section: Introductionmentioning

confidence: 99%

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Early Gestational Hypoxia and Adverse Developmental Outcomes

Ritchie

Oakes

Kennedy

et al. 2017

Birth Defects Research

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Hypoxia is a normal and essential part of embryonic development. However, this state may leave the embryo vulnerable to damage when oxygen supply is disturbed. Embryofetal response to hypoxia is dependent on duration and depth of hypoxia, as well as developmental stage. Early postimplantation rat embryos were resilient to hypoxia, with many surviving up to 1.5 hr of uterine clamping, while most mid-gestation embryos were dead after 1 hour of clamping. Survivors were small and many had a range of defects, principally terminal transverse limb reduction defects. Similar patterns of malformations occurred when embryonic hypoxia was induced by maternal hypoxia, interruption of uteroplacental flow, or perfusion and embryonic bradycardia. There is good evidence that high altitude pregnancies are associated with smaller babies and increased risk of some malformations, but these results are complicated by increased risk of pre-eclampsia. Early onset pre-eclampsia itself is associated with small for dates and increased risk of atrio-ventricular septal defects. Limb defects have clearly been associated with chorionic villus sampling, cocaine, and misoprostol use. Similar defects are also observed with increased frequency among fetuses who are homozygous for thalassemia. Drugs that block the potassium current, whether as the prime site of action or as a side effect, are highly teratogenic in experimental animals. They induce embryonic bradycardia, hypoxia, hemorrhage, and blisters, leading to transverse limb defects as well as craniofacial and cardiovascular defects. While evidence linking these drugs to birth defects in humans is not compelling, the reason may methodological rather than biological. Birth Defects Research 109:1358-1376, 2017.© 2017 Wiley Periodicals, Inc.

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Section: Concluding Commentsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Early Gestational Hypoxia and Adverse Developmental Outcomes

Ritchie

Oakes

Kennedy

et al. 2017

Birth Defects Research

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“…Det ble heller ikke inkludert en kontrollgruppe der andre antibiotika var brukt, slik at en mulig effekt av den underliggende infeksjonen ikke kan utelukkes. Forfatterne av den svenske studien har tidligere foreslått at evnen makrolider har til å blokkere en spesiell kaliumkanal i hjertet (hERG-kanaler) kunne vaere en plausibel teratogen meksmisme (35), noe andre har trukket i tvil (36). På bakgrunn av hovedvekten av data, inkludert norske, og fordi den biologiske plausibiliteten er diskuterbar, mener vi makrolider bør kunne vaere annenhåndsvalg, altså i de tilfellene førstehåndsvalget ikke kan brukes på grunn av allergi eller andre kontraindikasjoner.…”

Section: Diskusjonunclassified

Bruk av antibiotika i svangerskapet

Nordeng¹,

Nordeng²,

Høye³

2016

Tidsskriftet

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“…Fetal bradycardia may manifest as a result of congenital channelopathies, maternal autoantibodies, or following exposure to cardioactive drugs (Strasburger and Wakai ; Nilsson et al. ; Nilsson and Webster ).…”

Section: Introductionmentioning

confidence: 99%

Long-term programming effects on blood pressure following gestational exposure to the I _Kr blocker Dofetilide

et al. 2018

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A slow embryonic heart rate in early‐mid gestation is associated with increased risk of embryonic death and malformation, however, the long‐term consequences remain unknown. We administered Dofetilide (Dof, 2.5 mg/kg), a drug that produces embryo‐specific bradycardia, to pregnant rats from gestational days 11–14. Embryonic heart rate and rhythm were determined using embryo culture. Cardiovascular function was assessed in surviving adult offspring at rest, during acute psychological stress (air jet stress, AJS), and after 7 days of repeated AJS. Dof reduced embryonic HR by 40% for ~8 h on each of the treatment days. On postnatal day 3, Dof offspring were ~10% smaller. Blood pressure was elevated in adult Dof rats (systolic blood pressure, night: 103.8 ± 3.9 vs. 111.2 ± 3.0 mmHg, P = 0.01). While the pressor response to AJS was similar in both groups (control 17.7 ± 3.4; Dof 18.9 ± 0.9 mmHg, P = 0.74), after 7 days repeated AJS, clear habituation was present in control (P = 0.0001) but not Dof offspring (P = 0.48). Only Dof offspring showed a small increase in resting blood pressure after 7 days repeated stress (+3.9 ± 1.7 mmHg, P = 0.05). The results indicate that embryonic bradycardia programs hypertension and impaired stress adaptation, and have implications for the maternal use of cardioactive drugs during pregnancy.

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Effects of Macrolide Antibiotics on Rat Embryonic Heart Function In Vitro

Cited by 16 publications

References 73 publications

Early Gestational Hypoxia and Adverse Developmental Outcomes

Early Gestational Hypoxia and Adverse Developmental Outcomes

Bruk av antibiotika i svangerskapet

Long-term programming effects on blood pressure following gestational exposure to the I _Kr blocker Dofetilide

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Effects of Macrolide Antibiotics on Rat Embryonic Heart Function In Vitro

Cited by 16 publications

References 73 publications

Early Gestational Hypoxia and Adverse Developmental Outcomes

Early Gestational Hypoxia and Adverse Developmental Outcomes

Bruk av antibiotika i svangerskapet

Long-term programming effects on blood pressure following gestational exposure to the I Kr blocker Dofetilide

Contact Info

Product

Resources

About

Long-term programming effects on blood pressure following gestational exposure to the I _Kr blocker Dofetilide