Six full-term newborn infants are described who suffered from severe adult respiratory distress syndrome (ARDS). The triggering event was intrauterine/perinatal asphyxia in five, and group B streptococcal (GBS) septicemia in three. All had severe respiratory distress/failure and were ventilated mechanically with high concentrations of inspired oxygen and positive end-expiratory pressure. Radiography of the chest showed dense bilateral consolidation with air bronchograms and reduced lung volume. Persistent pulmonary hypertension (PPH) was documented in all cases. The coincidence of ARDS and PPH rendered respiratory management extremely difficult. For this reason high-frequency ventilation was instituted in all patients in order to improve CO2 elimination and induce respiratory alkalosis. Acute complications of respiratory therapy were encountered in five patients (pneumothorax, pulmonary interstitial emphysema, pneumopericardium). Three infants died (irreversible septic shock, progressive severe hypoxemia, and sudden cardiac arrest) after 17, 80, and 175 h of life. Histologic examination of the lungs was possible in all fatal cases and revealed typical changes of acute to subacute stages of ARDS. Three infants survived, the mean time of mechanical respiratory support being 703 h. Two patients were still dependent on oxygen after 1 month of life, and all survivors had increased interstitial markings and increased lung volumes on their chest roentgenograms at this time.
We report on 2 children, brother and sister, who presented with cardiomyopathy
and muscular hypotonia at the age of 8 months. They both excreted significant amounts
of 3-hydroxy-3-methylglutaric acid (3-HMG) and 3-methylglutaconic acid (3-MGC) but
no 3-methylglutaric acid (3-MG). Enzyme analysis in fibroblasts revealed normal activities
of 3-hydroxy-3-methylglutaryl-CoA (HMG-CoA) lyase and of 3-methylglutaconyl
hydratase and other enzymes of 3-HMG metabolism. Loading tests with leucine did not
affect the excretion of 3-HMG and 3-MGC. The girl died as a result of her cardiomyopathy.
while the boy recovered and was treated with cardiac supportive therapy. He
showed a steady improvement during his clinical course with biochemical normalization
of the urinary excretion of 3-HMG, concomitant with marked improvement in the hypertrophic
cardiomyopathy. In cultured fibroblasts from both patients a reduced activity
of complex II/III of the respiratory chain was measured which may be the cause of this
new type of 3-HMG uria. Analysis of mitochondrial DNA heart muscle, liver and fibroblast
culture of the patient did not reveal any major mitochondrial DNA rearrangements
(deletion, duplication) or any point mutation that had been described in association
with mitochondrial cardiomyopathy.
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