| Literature DB >> 25144542 |
Robert Trimble, Jane Atkins, Troy C Quigg, Cara C Burns, Gregory S Wallace, Mary Thomas, Anil T Mangla, Anthony J Infante.
Abstract
Poliovirus transmission has been eliminated in most of the world through the use of inactivated poliovirus vaccine (IPV) and live, attenuated oral poliovirus vaccine (OPV). In the United States, use of OPV was discontinued by the year 2000 because of the potential for vaccine-associated paralytic polio (VAPP); an average of eight cases were reported each year in the United States during 1980-2000. Polio eradication efforts in other parts of the world continue to rely on OPV to take advantage of transmission of poliovirus vaccine strains to unvaccinated persons in the population, lower cost, and ease of administration. In 2013, an infant aged 7 months who recently immigrated to the United States from India was referred to a hospital in San Antonio, Texas. The infant had fever, an enlarging skin lesion in the deltoid region with axillary lymphadenopathy, decreased activity, and inability to bear weight on the left leg, progressing to paralysis of the left leg over a 6-week period. Recognition of lymphopenia on complete blood count led to immune evaluation, which revealed the presence of severe combined immunodeficiency syndrome (SCIDS), an inherited disorder. A history of OPV and bacille Calmette-Guérin (BCG) vaccination in India led to the diagnoses of VAPP and BCG-osis, which were confirmed microbiologically. This report demonstrates the importance of obtaining a comprehensive clinical history in a child who has recently immigrated to the United States, with recognition that differing vaccine practices in other countries might require additional consideration of potential etiologies.Entities:
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Year: 2014 PMID: 25144542 PMCID: PMC5779436
Source DB: PubMed Journal: MMWR Morb Mortal Wkly Rep ISSN: 0149-2195 Impact factor: 17.586
Laboratory, imaging, and microbiologic study results for a male patient aged 7 months recently immigrated from India who was brought to a hospital emergency department — San Antonio, Texas, July 2013
| Type of study | Results |
|---|---|
|
| |
| CBC | ALC-216 cells/mm3 |
| Lymphocyte subsets | CD3 = 6 cells/mm3; CD4 = 2; CD8 = 0; CD19 = 1; CD16/56 = 189 |
| HIV 1/2 | Negative |
| Immunoglobulins | IgA undetectable; IgM undetectable; IgG 140 mg/dL |
| CSF | 83 WBCs/mm3; 50% PMNs; 42% MNCs; 2% lymphocytes; protein = 48 mg/dL; glucose = 49 mg/dL |
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| |
| Chest radiograph | Normal |
| Brain and spine MRI | 8-mm lesion in right cerebral peduncle; prominent abnormal T2 weighted signal at cord T11 level on the left; additional abnormal signal and contrast enhancement of several nerve roots |
| Chest, abdomen, pelvis CT | Enlarged lymph nodes: left supraclavicular, left axilla, retroperitoneal |
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| |
| Blood | No bacterial growth at 48 hrs; later positive for AFB identified as |
| CSF | Negative bacterial meningitis screen and Gram stain; negative fungal smear and culture; negative PCR for HSV-1, HSV-2, and CMV |
| Stool | Enterovirus isolated; identified as iVDPV1 |
| Lymph node FNA | AFB stain positive; identified as |
Abbreviations: CBC = complete blood count; ALC = absolute lymphocyte count; HIV = human immunodeficiency virus; IgA = immunoglobulin A; IgM = immunoglobulin M; CSF = cerebrospinal fluid; WBCs = white blood cells; PMNs = polymorphonuclear neutrophils; MNCs = mononuclear cells; MRI = magnetic resonance imaging; CT = computed tomography; AFB = acid-fast bacilli; BCG = bacille Calmette-Guérin; PCR = polymerase chain reaction; HSV = herpes simplex virus; CMV = cytomegalovirus; iVDPV1 = immunodeficiency-associated vaccine-derived poliovirus type 1; FNA = fine-needle aspiration.