Your search keyword '"LaRussa, Philip S"' showing total 7 results

1. Respiratory Pathogens in Children 1 Month to 5 Years of Age Presenting With Undifferentiated Acute Respiratory Distress in 2 District-Level Hospitals in Ghana.

Author

Wilson, Patrick T, Baiden, Frank, Brooks, Joshua C, Giessler, Katie M, Apio, Gavin, Punguyire, Damien, Moresky, Rachel T, Sylverken, Justice, Nyarko-Jectey, Kwadwo, Tagbor, Harry, and LaRussa, Philip S

Subjects

ENTEROVIRUSES, POLYMERASE chain reaction, PUBLIC hospitals, ADULT respiratory distress syndrome, RESPIRATORY infections, RESPIRATORY syncytial virus, RNA viruses, WEATHER, DESCRIPTIVE statistics, CHILDREN

Abstract

Ghanaian children (2176) aged <5 years who presented with undifferentiated acute respiratory distress were tested for respiratory pathogens using a BioFire FilmArray polymerase chain reaction assay. Rhinovirus and/or enterovirus was detected in 36% of the assays, respiratory syncytial virus in 11%, and parainfluenza in 7%. Respiratory syncytial virus and metapneumovirus were detected more frequently in the rainy season than in the dry season. [ABSTRACT FROM AUTHOR]

Published

2019

2. Arm Paralysis After Routine Childhood Vaccinations: Application of Advanced Molecular Methods to the Causality Assessment of an Adverse Event After Immunization.

Author

Shaw, Jana, Halsey, Neal A., Weinberg, Adriana, Schmid, D. Scott, George, Kirsten St., Weldon, William C., Jordan, Michael, Bryant, Patrick W., LaRussa, Philip S., Bradshaw, Deborah Y., Harrington, Theresa, and Gershon, Anne

Subjects

ARM paralysis, VACCINATION complications, IMMUNIZATION complications, VARICELLA-zoster virus, CEREBROSPINAL fluid, MAGNETIC resonance imaging

Abstract

Post-licensure surveillance for adverse events following immunizations (AEFI) can identify rare complications of vaccinations and rigorous vaccine adverse event causality assessments can help to identify possible causal relationships. We report the development of arm paralysis after varicella vaccination in a 1-year-old child. Paralysis was initially presumed to be due to vOka because of the temporal relationship between vaccination and onset of arm weakness; however, molecular studies identified wild-type varicella zoster virus VZV (WT-VZV) in the CSF, leading the authors to conclude that WT-VZV was the probable cause. This case illustrates the complexity of assessing AEFI causality, and the importance of careful and complete evaluations when determining the most likely cause of an AEFI. [ABSTRACT FROM AUTHOR]

Published

2017

3. Effectiveness of 2 Doses of Varicella Vaccine in Children.

Author

Shapiro, Eugene D., Vazquez, Marietta, Esposito, Daina, Holabird, Nancy, Steinberg, Sharon P., Dziura, James, LaRussa, Philip S., and Gershon, Anne A.

Subjects

VARICELLA-zoster virus diseases, IMMUNIZATION of children, POLYMERASE chain reaction, LOGISTIC regression analysis, VACCINATION

Abstract

Background. Because of ongoing outbreaks of varicella, a second dose of varicella vaccine was added to the routine immunization schedule for children in June 2006 by the Centers for Disease Control and Prevention. Methods. We assessed the effectiveness of 2 doses of varicella vaccine in a case-control study by identifying children ≥4 years of age with varicella confirmed by polymerase chain reaction assay and up to 2 controls matched by age and pediatric practice. Effectiveness was calculated using exact conditional logistic regression. Results. From July 2006 to January 2010, of the 71 case subjects and 140 matched controls enrolled, no cases (0%) vs 22 controls (15.7%) had received 2 doses of varicella vaccine, 66 cases (93.0%) vs 117 controls (83.6%) had received 1 dose, and 5 cases (7.0%) vs 1 control (0.7%) did not receive varicella vaccine (P < .001). The effectiveness of 2 doses of the vaccine was 98.3% (95% confidence level [CI]: 83.5%-100%; P < .001). The matched odds ratio for 2 doses vs 1 dose of the vaccine was 0.053 (95% CI: 0.002-0.320; P < .001). Conclusion. The effectiveness of 2 doses of varicella vaccine in the first 2.5 years after recommendation of a routine second dose of the vaccine for children is excellent. Odds of developing varicella were 95% lower for children who received 2 doses compared with 1 dose of varicella vaccine. [ABSTRACT FROM AUTHOR]

Published

2011

4. Primary Vaccine Failure after 1 Dose of Varicella Vaccine in Healthy Children.

Author

Michalik, David E., Steinberg, Sharon P., LaRussa, Philip S., Edwards, Kathryn M., Wright, Peter F., Arvin, Ann M., Gans, Haley A., and Gershon, Anne A.

Subjects

VACCINATION of children, IMMUNIZATION, VARICELLA-zoster virus, CHICKENPOX, FLUORESCENT antibody technique, IMMUNOGLOBULINS, SERUM, DRUG efficacy

Abstract

Universal immunization of young children with 1 dose of varicella vaccine was recommended in the United States in 1995, and it has significantly decreased the incidence of chickenpox. Outbreaks of varicella, however, are reported among vaccinated children. Although vaccine effectiveness has usually been ~85%, rates as low as 44% have been observed. Whether this is from primary or secondary vaccine failure— or both—is unclear. We tested serum samples from 148 healthy children immunized against varicella in New York, Tennessee, and California to determine their seroconversion rates, before and after 1 dose of Merck/Oka varicella vaccine. The median age at vaccination was 12.5 months; postvaccination serum samples were obtained on average 4 months later. Serum was tested for antibodies against varicella-zoster virus (VZV) by use of the previously validated sensitive and specific fluorescent antibody to membrane antigen (FAMA) assay. Of 148 healthy child vaccinees, 113 (76%) seroconverted, and 24% had no detectable VZV FAMA antibodies. Our data contrast with reported seroconversion rates of 86%-96% by other VZV antibody tests and suggest that many cases of varicella in immunized children are due to primary vaccine failure. A second dose of varicella vaccine is expected to increase seroconversion rates and vaccine effectiveness. [ABSTRACT FROM AUTHOR]

Published

2008

5. Risk of Herpes Zoster in Adults Immunized with Varicella Vaccine.

Author

Hambleton, Sophie, Steinberg, Sharon P., Larussa, Philip S., Shapiro, Eugene D., and Gershon, Anne A.

Subjects

VACCINATION, HERPES zoster, VACCINATION of children, VARICELLA-zoster virus, CHILDREN'S health, AMERICAN children

Abstract

A program of routine varicella vaccination of children 12-18 months of age, begun in the United States in 1995, has been very successful in reducing the incidence of varicella. Varicella-zoster virus (VZV), in both wild-type and live attenuated forms, is notable for its ability to produce latent infection of sensory neurons from which it can later reactivate to cause herpes zoster (HZ). Therefore, the effects of vaccination on this secondary VZV-related disease are important to consider; in practice, however, such studies are complicated by the typically long delay between acquisition of the virus and its reactivation. Studies of immunocompromised children have shown that vaccination is relatively protective against HZ in this highly vulnerable group. We now present long-term follow-up data on a group of individuals who received varicella vaccine as healthy young adults 10-26 years ago and who have been followed prospectively by means of active surveillance. Among some 2000 person-years of follow-up, 2 cases of HZ have occurred, for a rate of 1.00 case/1000 person- years. Overall, the incidence of HZ in this cohort, therefore, is similar to published data for the US population in the prevaccine era. [ABSTRACT FROM AUTHOR]

Published

2008

6. The Safety Profile of Varicella Vaccine: A 10-Year Review.

Author

Galea, Susan A., Sweet, Ann, Beninger, Paul, Steinberg, Sharon P., Larussa, Philip S., Gershon, Anne A., and Sharrar, Robert G.

Subjects

VIRAL vaccines, VARICELLA-zoster virus, POLYMERASE chain reaction, PUBLIC health surveillance, VACCINATION, IMMUNIZATION

Abstract

Varivax (varicella virus vaccine live [Oka/Merck]; Merck), a live attenuated varicella vaccine, is indicated for vaccination against varicella in appropriate individuals ⩾12 months of age. The 10-year safety profile for Varivax is described using data submitted to Merck from routine global postmarketing surveillance, combined with information from a Varicella Zoster Virus Identification Program, which uses polymerase chain reaction (PCR) analysis to identify the presence and strain of VZV in selected specimens. There were 16,683 reports worldwide voluntarily submitted to Merck, for an overall reporting rate of 3.4 reports/10,000 doses of vaccine distributed. PCR analysis of vesicular rashes that occurred within the first 2 weeks after vaccination was more likely to identify wild-type varicella-zoster virus (VZV), whereas the presence of Oka VZV was generally associated with vesicular rashes that occurred 15-42 days after vaccination. Reports of breakthrough varicella that occurred >42 days after vaccination were associated with wild-type VZV. Among 697 herpes zoster reports, PCR analysis identified Oka VZV in 57 reports and wild-type VZV in 38 reports. There were no primary neurologic adverse events associated with Oka VZV. Secondary transmission of Oka VZV from vaccine recipients with postvaccination vesicular rashes was identified in 3 susceptible household contacts. Disseminated Oka VZV was identified in 6 immunocompromised patients and 1 patient with Down syndrome. This review has shown that the vaccine is generally safe and well tolerated. [ABSTRACT FROM AUTHOR]

Published

2008

7. Antibodies to Varicella-Zoster Virus Glycoproteins I, II, and III in Leukemic and Healthy Children.

Author

LaRussa, Philip S., Gershon, Anne A., Steinberg, Sharon P., and Chartrand, Stephen A.

Abstract

Adot ELISA was used to analyze the antibody response to varicella-zoster virus glycoproteins I, II, and 1lI in leukemic and healthy children who either developed natural varicella or received the live attenuated varicella vaccine. Both groups of children showed an antibody response to these viral glycoproteins. The antibody response to all three glycoproteins showed excellent persistence over the 3-year period ofstudy. None of the glycoproteins provoked an antibody response that could be shown to correlate with protection from breakthrough varicella after household exposure chickenpox or from zoster in leukemic vaccinees. [ABSTRACT FROM PUBLISHER]

Published

1990