Paul F. Wehrle scite author profile

Antibody to polyribophosphate, the capsular polysaccharide of Haemophilus influenzae type b, was measured in healthy ambulatory children by a radioactive antigen-binding assay. Titers fell from birth through nine months of age, then increased until six years, when they plateaued. Antibody activity was not correlated with the child's sex, ethnic status, or area of residence. Doses of 0.2-50 microgram of polyribophosphate given as single or booster doses had similar effects on antibody activity. Of 368 doses given to infants two to six months of age, 7% produced a significant antibody response; of 95 doses given to infants seven to 12 months old, 17% produced a response. The geometric mean titers of antibody resulting from immunization with polyribophosphate given at various times in relation to diphtheria-pertussistetanus vaccine did not differ significantly from one another or from titers observed in infants given only the latter vaccine. These data indicate that purified polyribophosphate will not provoke humoral immunity in young infants against H. influenzae type b and that it should no longer be considered as a candidate vaccine for this purpose.

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Tobramycin: Maternal-Fetal Pharmacology

Bernard

Garcia-Cázares

Ballard

et al. 1977

Antimicrob Agents Chemother

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To investigate the maternal-fetal transfer of tobramycin (TBM) and its distribution in the fetus, a single dose of 2 mg/kg was administered intramuscularly to 35 pregnant patients (13 first trimester, 22 second trimester) 0.5 to 34 h before hysterectomy. TBM concentration was assayed microbiologically in maternal serum, fetal tissues (placenta, brain, lung, liver, and kidney), and fluids (amniotic, cerebrospinal fluid [CSF], urine, and serum). Mean maternal serum half-life (1.54 h) and mean peak serum concentration ofTBM were within ranges reported for nonpregnant adults. In fetal serum, half-life was 5.2 h, and TBM levels did not exceed 0.58 ,g/ml. For intervals up to 34 h, the mean TBM concentration in placental tissues was 1.4 gg/g. Concentration differences related to fetal maturation were found for fetal CSF, amniotic fluid, and fetal kidney. No antimicrobial activity was found in the fetal CSF of >16 weeks' gestation. TBM was present predominantly in the second trimester amniotic fluid specimens. Fetal kidney concentrations reached 7.2 ug/g at 34 h after maternal drug administration. Higher TBM concentrations were related to advanced maturation ofthe fetal kidney. Second trimester fetal urine concentrations for TBM ranged from 0.1 to 3.4 gg/ml, and the fetal urinary half-life was 3.7 h. Knowledge of fetal pharnacology is essential for weighing the fetal benefits or risks of antimicrobial therapy for the infected gravid patient.

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Los Angeles Student Nurse Study

Hammer

Hasselblad

Portnoy

et al. 1974

Archives of Environmental Health: An International Journal

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Paul F. Wehrle

Additional evidence against measles vaccine administration to infants less than 12 months of age: Altered immune response following active/passive immunization

Meningitis Due toListeria monocytogenes

Antibody to Polyribophosphate of Haemophilus influenzae Type b in Infants and Children: Effect of Immunization with Polyribophosphate

Tobramycin: Maternal-Fetal Pharmacology

Los Angeles Student Nurse Study

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