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3. Vital Signs: Update on Zika Virus–Associated Birth Defects and Evaluation of All U.S. Infants with Congenital Zika Virus Exposure — U.S. Zika Pregnancy Registry, 2016

Author

Reynolds, M. R., Jones, A. M., Petersen, E. E., Lee, E. H., Rice, M. E., Bingham, A., Ellington, S. R., Evert, N., Reagan-Steiner, S., Oduyebo, T., Brown, C. M., Martin, S., Ahmad, N., Bhatnagar, J., Macdonald, J., Gould, C., Fine, A. D., Polen, K. D., Lake-Burger, H., Hillard, C. L., Hall, N., Mahsa Yazdy, Slaughter, K., Sommer, J. N., Adamski, A., Raycraft, M., Fleck-Derderian, S., Gupta, J., Newsome, K., Baez-Santiago, M., Slavinski, S., White, J. L., Moore, C. A., Shapiro-Mendoza, C. K., Petersen, L., Boyle, C., Jamieson, D. J., Meaney-Delman, D., Honein, M. A., Adair, J., Ruberto, I., Haselow, D. T., Im, L., Jilek, W., Lehmann, M. S., Olney, R., Porse, C. C., Ramstrom, K. C., Sowunmi, S., Marzec, N. S., Davis, K., Esponda-Morrison, B., Zachariah Fraser, M., O’connor, C. A., Chung, W., Richardson, F., Sexton, T., Stocks, M. E., Woldai, S., Bundek, A. M., Zambri, J., Goldberg, C., Eisenstein, L., Jackson, J., Kopit, R., Logue, T., Mendoza, R., Feldpausch, A., Graham, T., Mann, S., Park, S. Y., Carter, K. K., Potts, E. J., Stevens, T., Simonson, S., Tonzel, J. L., Davis, S., Robinson, S., Hyun, J. K., Jenkins, E. M., Piccardi, M., Reid, L. D., Dunn, J. E., Higgins, C. A., Lin, A. E., Munshi, G. S., Sandhu, K., Scotland, S. J., Soliva, S., Copeland, G., Signs, K. A., Schiffman, E., Byers, P., Hand, S., Mulgrew, C. L., Hamik, J., Koirala, S., Ludwig, L. A., Fredette, C. R., Garafalo, K., Worthington, K., Ropri, A., Ade, J. N., Alaali, Z. S., Blog, D., Brunt, S. J., Bryant, P., Burns, A. E., Carson, K., Dupuis, A. P., Sullivan-Frohm, A., Griffin, J., Hidalgo, C., Lance, L. A., Many, P. S., Naizby, B. E., Polfleit, M. J., Rahman, T., Rem, T., Robbins, A. E., Rowlands, J. V., Seaver, C., Seward, K. A., Smith, L., Sohi, I., Wester, R. E., Bush, S., Dean, A. B., Demarest, V., Dufort, E. M., Furuya, A. M., Fuschino, M., Kulas, K. E., Lamson, D. M., Lee, W. T., Limberger, R., Marchewka, M. J., Popowich, M., St George, K., Wong, S. J., Zeng, L., Glaze, V. H., Souto, M. I., Ackelsberg, J., Alex, B., Ballen, V., Baumgartner, J., Bloch, D., Clark, S., Conners, E., Cooper, H., Davidson, A., Dentinger, C., Deocharan, B., Vito, A., Fu, J., Hrusa, G., Iqbal, M., Iwamoto, M., Jones, L., Kubinson, H., Lash, M., Layton, M., Lee, C. T., Liu, D., Mcgibbon, E., Moy, M., Ngai, S., Parton, H. B., Peterson, E., Poy, J., Rakeman, J., Stoute, A., Thompson, C., Weiss, D., Westheimer, E., Winters, A., Younis, M., Chan, R. L., Cronquist, L. J., Caton, L., Lind, L., Nalluswami, K., Perella, D., Brady, D. S., Gosciminski, M., Mcauley, P., Drociuk, D., Leedom, V., Witrick, B., Bollock, J., Hartel, M. B., Lucinski, L. S., Mcdonald, M., Miller, A. M., Ponson, T. A., Price, L., Nance, A. E., Peterson, D., Cook, S., Martin, B., Oltean, H., Neary, J., Baker, M. A., Cummons, K., Bryan, K., Arnold, K. E., Arth, A. C., Bollweg, B. C., Cragan, J. D., Dawson, A. L., Denison, A. M., Dziuban, E. J., Estetter, L., Silva-Flannery, L., Free, R. J., Galang, R. R., Gary, J., Goldsmith, C. S., Green, C., Hale, G. L., Hayes, H. M., Igbinosa, I., Kelly Keating, M., Khan, S., Kim, S. Y., Lampe, M., Lewis, A., Mai, C., Martines, R. B., Miers, B., Moore, J., Muehlenbachs, A., Nahabedian, J., Panella, A., Parihar, V., Patel, M. M., Brett Rabeneck, D., Rasmussen, S. A., Ritter, J. M., Rollin, D. C., Sanders, J. H., Shieh, W. -J, Simeone, R. M., Simon, E. L., Sims, J. R., Spivey, P. J., Talley-Mcrae, H., Tshiwala, A. K., Maldeghem, K., Viens, L., Wainscott-Sargent, A., Williams, T., and Zaki, S.

Subjects
0301 basic medicine, Gerontology, medicine.medical_specialty, Microcephaly, Health (social science), Epidemiology, Health, Toxicology and Mutagenesis, Vital signs, Congenital Abnormalities, Zika virus, 03 medical and health sciences, Fetus, 0302 clinical medicine, Health Information Management, Central Nervous System Diseases, Pregnancy, Humans, Medicine, Eye Abnormalities, Neural Tube Defects, Registries, 030212 general & internal medicine, Pregnancy Complications, Infectious, Pregnancy registry, biology, Vital Signs, Zika Virus Infection, business.industry, Obstetrics, Public health, Infant, Newborn, Brain, Infant, Gestational age, Zika Virus, General Medicine, biology.organism_classification, medicine.disease, United States, 030104 developmental biology, Female, business
Abstract

Background In collaboration with state, tribal, local, and territorial health departments, CDC established the U.S. Zika Pregnancy Registry (USZPR) in early 2016 to monitor pregnant women with laboratory evidence of possible recent Zika virus infection and their infants. Methods This report includes an analysis of completed pregnancies (which include live births and pregnancy losses, regardless of gestational age) in the 50 U.S. states and the District of Columbia (DC) with laboratory evidence of possible recent Zika virus infection reported to the USZPR from January 15 to December 27, 2016. Birth defects potentially associated with Zika virus infection during pregnancy include brain abnormalities and/or microcephaly, eye abnormalities, other consequences of central nervous system dysfunction, and neural tube defects and other early brain malformations. Results During the analysis period, 1,297 pregnant women in 44 states were reported to the USZPR. Zika virus-associated birth defects were reported for 51 (5%) of the 972 fetuses/infants from completed pregnancies with laboratory evidence of possible recent Zika virus infection (95% confidence interval [CI] = 4%-7%); the proportion was higher when restricted to pregnancies with laboratory-confirmed Zika virus infection (24/250 completed pregnancies [10%, 95% CI = 7%-14%]). Birth defects were reported in 15% (95% CI = 8%-26%) of fetuses/infants of completed pregnancies with confirmed Zika virus infection in the first trimester. Among 895 liveborn infants from pregnancies with possible recent Zika virus infection, postnatal neuroimaging was reported for 221 (25%), and Zika virus testing of at least one infant specimen was reported for 585 (65%). Conclusions and implications for public health practice These findings highlight why pregnant women should avoid Zika virus exposure. Because the full clinical spectrum of congenital Zika virus infection is not yet known, all infants born to women with laboratory evidence of possible recent Zika virus infection during pregnancy should receive postnatal neuroimaging and Zika virus testing in addition to a comprehensive newborn physical exam and hearing screen. Identification and follow-up care of infants born to women with laboratory evidence of possible recent Zika virus infection during pregnancy and infants with possible congenital Zika virus infection can ensure that appropriate clinical services are available.

Published
2017

6. Nipah Virus: A Recently Emergent Deadly Paramyxovirus

Author

Chua, K. B., Bellini, W. J., Rota, P. A., Harcourt, B. H., Tamin, A., Lam, S. K., Ksiazek, T. G., Rollin, P. E., Zaki, S. R., Shieh, W.-J., Goldsmith, C. S., Gubler, D. J., Roehrig, J. T., Eaton, B., Gould, A. R., Olson, J., Field, H., Daniels, P., Ling, A. E., Peters, C. J., Anderson, L. J., and Mahy, B. W. J.

Published
2000

8. Fatal laboratory-acquired infection with an attenuated Yersinia pestis strain--Chicago, Illinois, 2009

Author

Ritger, K., Black, S., Weaver, K., Jones, J., Gerber, S., Conover, C., Soyemi, K., Metzger, K., King, B., Mead, P., Molins, C., Schriefer, M., Shieh, W.-J., Zaki, S., and Medina-Marino, A.

Subjects
Medical research -- Health aspects, Medicine, Experimental -- Health aspects, Infection -- Research -- Health aspects, Public health -- Health aspects, Health
Abstract

On September 18, 2009, the Chicago Department of Public Health (CDPH) was notified by a local hospital of a suspected case of fatal laboratory-acquired infection with Yersinia pestis, the causative [...]

Published
2011

9. Fatal encephalitis and myocarditis in young domestic geese (Anser anser domesticus) caused by West Nile virus

Author

Swayne, D. E., Beck, J. R., Smith, C. S., Shieh, W. J., and Zaki, S. R.

Subjects
viruses, Antibodies, Viral, Disease Outbreaks, Death, Immunoenzyme Techniques, Songbirds, Disease Models, Animal, Myocarditis, Animals, Domestic, Geese, Animals, New York City, West Nile virus, West Nile Fever, Research Article
Abstract

During 1999 and 2000, a disease outbreak of West Nile (WN) virus occurred in humans, horses, and wild and zoological birds in the northeastern USA. In our experiments, WN virus infection of young domestic geese (Anser anser domesticus) caused depression, weight loss, torticollis, opisthotonus, and death with accompanying encephalitis and myocarditis. Based on this experimental study and a field outbreak in Israel, WN virus is a disease threat to young goslings and viremia levels are potentially sufficient to infect mosquitoes and transmit WN virus to other animal species.

Published
2001

10. Idiopathic granulomatous mastitis in hispanic women--Indiana, 2006-2008

Author

Goldman, M., Selke, H.M., Pardo, I., Clare, S.E., Emerson, R.E., Howell, J.F., Shieh, W.-J., Zaki, S., Sanchez, C., Sinkowitz-Cochran, R.L., Srinivasan, A., Jhung, M., Chester, T.J., Ritchey, M., Jarquin, V.G., and Meites, E.

Subjects
Hispanic American women -- Health aspects, Mastitis -- Development and progression, Mastitis -- Statistics, Mastitis -- Demographic aspects, Mastitis -- Diagnosis
Abstract

Idiopathic granulomatous mastitis (IGM) is a rare inflammatory breast lesion of unknown etiology that occurs in women of childbearing age; only a few hundred cases have been reported worldwide (1,2). [...]

Published
2009

11. Progressive Vaccinia: Case Description and Laboratory-Guided Therapy With Vaccinia Immune Globulin, ST-246, and CMX001

Author

Lederman, E. R., primary, Davidson, W., additional, Groff, H. L., additional, Smith, S. K., additional, Warkentien, T., additional, Li, Y., additional, Wilkins, K. A., additional, Karem, K. L., additional, Akondy, R. S., additional, Ahmed, R., additional, Frace, M., additional, Shieh, W.-J., additional, Zaki, S., additional, Hruby, D. E., additional, Painter, W. P., additional, Bergman, K. L., additional, Cohen, J. I., additional, and Damon, I. K., additional

Published
2012
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12. A Large Outbreak of Typhoid Fever Associated With a High Rate of Intestinal Perforation in Kasese District, Uganda, 2008-2009

Author

Neil, K. P., primary, Sodha, S. V., additional, Lukwago, L., additional, O-tipo, S., additional, Mikoleit, M., additional, Simington, S. D., additional, Mukobi, P., additional, Balinandi, S., additional, Majalija, S., additional, Ayers, J., additional, Kagirita, A., additional, Wefula, E., additional, Asiimwe, F., additional, Kweyamba, V., additional, Talkington, D., additional, Shieh, W.-J., additional, Adem, P., additional, Batten, B. C., additional, Zaki, S. R., additional, and Mintz, E., additional

Published
2012
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18. The Pathology of Rotavirus-Associated Deaths, Using New Molecular Diagnostics

Author

Lynch, M., primary, Shieh, W.-J., additional, Tatti, K., additional, Gentsch, J. R., additional, Harris, T. F., additional, Jiang, B., additional, Guarner, J., additional, Bresee, J. S., additional, Greenwald, M., additional, Cullen, S., additional, Davies, H. D., additional, Trevenen, C., additional, Zaki, S. R., additional, and Glass, R. I., additional

Published
2003
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19. Laboratory investigation of human deaths from vampire bat rabies in Peru.

Author

Warner, C K, primary, Goldsmith, C S, additional, Niezgoda, M, additional, Smith, J S, additional, Zaki, S R, additional, Orciari, L A, additional, Rupprecht, C E, additional, Wright, C W, additional, Sanderlin, D W, additional, Shieh, W J, additional, Yager, P A, additional, Shaddock, J H, additional, and Whitfield, S G, additional

Published
1999
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25. Immunohistochemical and in situ hybridization studies of influenza A virus infection in human lungs.

Author

Guarner, J, Shieh, W J, Dawson, J, Subbarao, K, Shaw, M, Ferebee, T, Morken, T, Nolte, K B, Freifeld, A, Cox, N, and Zaki, S R

Abstract

Influenza viruses are responsible for acute febrile respiratory disease. When deaths occur, definitive diagnosis requires viral isolation because no characteristic viral inclusions are seen. We examined the distribution of influenza A virus in tissues from 8 patients with fatal infection using 2 immunohistochemical assays (monoclonal antibodies to nucleoprotein [NP] and hemagglutinin [HA]) and 2 in situ hybridization (ISH) assays (digoxigenin-labeled probes that hybridized to HA and NP genes). Five patients had prominent bronchitis; by immunohistochemical assay, influenza A staining was present focally in the epithelium of larger bronchi (intact and detached necrotic cells) and in rare interstitial cells. The anti-NP antibody stained primarily cell nuclei, and the anti-HA antibody stained mainly the cytoplasm. In 4 of these cases, nucleic acids (ISH) were identified in the same areas. Three patients had lymphohistiocytic alveolitis and showed no immunohistochemical or ISH staining. Both techniques were useful for detection of influenza virus antigens and nucleic acids in formalin-fixed paraffin-embedded tissues and can enable further understanding of fatal influenza A virus infections in humans.

Published
2000
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26. Japanese Encephalitis in Two Children--United States, 2010.

Author

Chen, L., Peek, M., Stokich, D., Todd, R., Anderson, M., Murphy, F. K., Hoffman, R., Evans, A., Jordan-Villegas, A., McCracken Jr., G., Chung, W. M., Tran, J., Raj, P., Shieh, W.-J., Schmitz, A., Zaki, S., Hills, S. L., Lambert, A., Panella, A., and Laven, J.

Subjects
JAPANESE encephalitis viruses, VENTRICULAR tachycardia, MENINGOENCEPHALITIS, FEVER, HEADACHE, NECK pain, GIRLS
Abstract

The article describes the cases of two children in the U.S. who were infected with Japanese encephalitis virus (JEV) in 2010. An 11-year-old girl was presented to a hospital with fever, headache and neck pain. She died after developing ventricular tachycardia and her autopsy showed histopathologic changes suggesting meningoencephalitis. JEV ribonucleic acid was also identified. A six-year-old boy was presented with fever, somnolence and headache. Examination showed JEV-specific immunoglobulin M and neutralizing antobodies. INSET: What is already known on the topic?.

Published
2011

27. Idiopathic Granulomatous Mastitis in Hispanic Women--Indiana, 2006-2008.

Author

Goldman, M., Selke, H. M., Pardo, I., Clare, S. E., Emerson, R. E., Howell, J. F., Shieh, W.-J., Zaki, S., Sanchez, C., Sinkowitz-Cochran, R. L., Srinivasan, A., Jung, M., Chester, T. J., Ritchey, M., Jarquin, V. G., and Meites, E.

Subjects
BREAST diseases, DISEASES in women, WOMEN'S health, INDIANA. Dept. of Health
Abstract

The article deals with the investigation conducted by the Indiana State Department of Health and the Centers for Disease Control & Prevention (CDC) into a cluster of seven idiopathic granulomatous mastitis (IGM) diagnoses in multigravid Hispanic women from 2006 to 2008. According to the article, IGM is a rare inflammatory breast lesion prevalent in women of childbearing age. Particular focus is given on the etiology of the breast masses and associated epidemiologic and clinical features. Findings from histopathologic evaluations are presented. It details the case-control study initiated to determine the possible risk factors for disease. INSET: What is already known on this topic?.

Published
2010

28. Evaluation of placental and fetal tissue specimens for Zika virus infection — 50 states and district of Columbia, January-December, 2016

Author

Reagan-Steiner, S., Simeone, R., Simon, E., Bhatnagar, J., Oduyebo, T., Free, R., Denison, A. M., Rabeneck, D. B., Ellington, S., Petersen, E., Gary, J., Hale, G., Keating, M. K., Martines, R. B., Muehlenbachs, A., Ritter, J., Lee, E., Davidson, A., Conners, E., Scotland, S., Sandhu, K., Bingham, A., Kassens, E., Smith, L., St George, K., Ahmad, N., Tanner, M., Beavers, S., Miers, B., Maldeghem, K., Khan, S., Rabe, I., Gould, C., Meaney-Delman, D., Honein, M. A., Shieh, W. -J, Jamieson, D. J., Fischer, M., Zaki, S. R., Kretschmer, M., Tarter, K., Yaglom, H., Alhajmohammad, S., Chhabra, D., Jilek, W., Madala, M., Messenger, S., Porse, C. C., Salas, M., Singh, D., Skallet, S., Sowunmi, S., Marzec, N. S., Davis, K., Esponda-Morrison, B., Fraser, M. Z., O’connor, C. A., Chung, W. M., Richardson, F., Stocks, M. E., Bundek, A. M., Zambri, M. L., Allen, A., Etienne, M. K., Jackson, J., Landis, V., Logue, T., Muse, N., Prieto, J., Rojas, M., Feldpausch, A., Graham, T., Mann, S., Park, S. Y., Freeman, D., Potts, E. J., Stevens, T., Simonson, S., Tonzel, J. L., Davis, S., Robinson, S., Hyun, J. K., Jenkins, E. M., Brown, C., Soliva, S., Schiffman, E., Byers, P., Hand, S., Mulgrew, C. L., Hamik, J., Koirala, S., Ludwig, E., Fredette, C. R., Mathewson, A. A., Garafalo, K., Worthington, K., Ropri, A., Bloch, D., Clark, S., Cooper, H., Fine, A. D., Hrusa, G., Iwamoto, M., Kubinson, H., Lee, C. T., Slavinski, S., Wilson, E., Winters, A., Yang, D. Y., Ade, J. N., Alaali, Z., Alvarez, K., Backenson, P. B., Blog, D., Dean, A., Dufort, E., Furuya, A. M., Fuschino, M., Hull, R., Kleabonas, M., Kulas, K., Kurpiel, P., Lance, L. A., Leak, E., Limberger, R. J., Ostrowski, S., Polfleit, M., Robbins, A., Rowlands, J. V., Sohi, I., Sommer, J. N., White, J., Wiley, D., Zeng, L., Chan, R. L., Macfarquhar, J., Cronquist, L., Lind, L., Nalluswami, K., Perella, D., Brady, D. S., Gosciminski, M., Mcauley, P., Teevan, B. E., Drociuk, D., Leedom, V., Witrick, B., Bollock, J., Kightlinger, L., Hartel, M. B., Lucinski, L. S., Mcdonald, M., Miller, A. M., Ponson, T. A., Price, L., Broussard, K., Nance, A. E., Peterson, D., Martin, B., Browne, S., Griffin-Thomas, L. A., Macdonald, J. O., Neary, J., Oltean, H., Adamski, A., Baez-Santiago, M., Bollweg, B. C., Cragan, J. D., Ermias, Y., Estetter, L. B. C., Fleck-Derderian, S., Goldsmith, C. S., Groenewold, M. R., Hayes, H., Igbinosa, I., Jenkinson, T. G., Jones, A. M., Lewis, A., Moore, C. A., Newsome, K. B., Parihar, V., Patel, M. M., Paulino, A., Rasmussen, S. A., Raycraft, M., Reynolds, M. R., Rollin, D. C., Sanders, J. H., Shapiro-Mendoza, C., Silva-Flannery, L., Spivey, P., Tshiwala, A. K., Williams, T. R., Bower, W. A., Davlantes, E., Forward, T. R., Fukunaga, R., Hines, J., Hu, S. S., Leung, J., Lewis, L., Martin, S., Mcnamara, L., Omura, J. D., Robinson, C. L., Schmit, K., Self, J. L., Shah, M., Straily, A., Dyne, E. A., Vu, M., and Williams, C.

32. A man with chest pain and glomerulonephritis.

Author

Turner, J. W., Pien, B. C., Ardoin, S. A., Anderson, A. M., Shieh, W. J., Zaki, S. R., Bhatnagar, J., Guarner, J., Howell, D. N., and Woods, C. W.

Subjects
*DIAGNOSIS, *SYMPTOMS, *MYOCARDIAL infarction, *BARTONELLA infections, *COMMUNICABLE diseases
Abstract

Presents a case study of the medical treatment of a man with chest pain and glomerulonephritis. Details of the patient's symptoms and the results of initial examinations; Claim that the patient's employment as a pest exterminator exposed him to chemicals, rodents, and animal carcasses; Report that the patient returned after initial treatment with a myocardial infarction, fever, and deteriorating renal function; Results of blood tests showing positive results for Bartonella henselae and B. quintana transmitted from feral kittens; Improvement of the patient's condition with doxycycline; Reflections on the treatment decisions and diagnosis in the case.

Published
2005
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33. The frequency and function of nucleoprotein-specific CD8 + T cells are critical for heterosubtypic immunity against influenza virus infection.

Author

Amoah S, Cao W, Sayedahmed EE, Wang Y, Kumar A, Mishina M, Eddins DJ, Wang W-C, Burroughs M, Sheth M, Lee J, Shieh W-J, Ray SD, Bohannon CD, Ranjan P, Sharma SD, Hoehner J, Arthur RA, Gangappa S, Wakamatsu N, Johnston HR, Pohl J, Mittal SK, and Sambhara S

Subjects
Animals, Mice, Mice, Inbred C57BL, Female, Adoptive Transfer, Interferon-gamma immunology, Interferon-gamma metabolism, Nucleocapsid Proteins immunology, Lung immunology, Lung virology, RNA-Binding Proteins immunology, RNA-Binding Proteins genetics, Nucleoproteins immunology, Nucleoproteins genetics, Viral Core Proteins immunology, Viral Core Proteins genetics, Orthomyxoviridae Infections immunology, Orthomyxoviridae Infections virology, CD8-Positive T-Lymphocytes immunology, T-Lymphocytes, Cytotoxic immunology
Abstract

Cytotoxic T lymphocytes (CTLs) mediate host defense against viral and intracellular bacterial infections and tumors. However, the magnitude of CTL response and their function needed to confer heterosubtypic immunity against influenza virus infection are unknown. We addressed the role of CD8 + T cells in the absence of any cross-reactive antibody responses to influenza viral proteins using an adenoviral vector expressing a 9mer amino acid sequence recognized by CD8 + T cells. Our results indicate that both CD8 + T cell frequency and function are crucial for heterosubtypic immunity. Low morbidity, lower viral lung titers, low to minimal lung pathology, and better survival upon heterosubtypic virus challenge correlated with the increased frequency of NP-specific CTLs. NP-CD8 + T cells induced by differential infection doses displayed distinct RNA transcriptome profiles and functional properties. CD8 + T cells induced by a high dose of influenza virus secreted significantly higher levels of IFN-γ and exhibited higher levels of cytotoxic function. The mice that received NP-CD8 + T cells from the high-dose virus recipients through adoptive transfer had lower viral titers following viral challenge than those induced by the low dose of virus, suggesting differential cellular programming by antigen dose. Enhanced NP-CD8 + T-cell functions induced by a higher dose of influenza virus strongly correlated with the increased expression of cellular and metabolic genes, indicating a shift to a more glycolytic metabolic phenotype. These findings have implications for developing effective T cell vaccines against infectious diseases and cancer., Importance: Cytotoxic T lymphocytes (CTLs) are an important component of the adaptive immune system that clears virus-infected cells or tumor cells. Hence, developing next-generation vaccines that induce or recall CTL responses against cancer and infectious diseases is crucial. However, it is not clear if the frequency, function, or both are essential in conferring protection, as in the case of influenza. In this study, we demonstrate that both CTL frequency and function are crucial for providing heterosubtypic immunity to influenza by utilizing an Ad-viral vector expressing a CD8 epitope only to rule out the role of antibodies, single-cell RNA-seq analysis, as well as adoptive transfer experiments. Our findings have implications for developing T cell vaccines against infectious diseases and cancer., Competing Interests: The authors declare no conflict of interest.

Published
2024
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34. Bioterrorism-related inhalational anthrax: the first 10 cases reported in the United States.

Author

Jernigan JA, Stephens DS, Ashford DA, Omenaca C, Topiel MS, Galbraith M, Tapper M, Fisk TL, Zaki S, Popovic T, Meyer RF, Quinn CP, Harper SA, Fridkin SK, Sejvar JJ, Shepard CW, McConnell M, Guarner J, Shieh WJ, Malecki JM, Gerberding JL, Hughes JM, and Perkins BA

Subjects
Adult, Aged, Anthrax epidemiology, Anthrax transmission, Bacillus anthracis physiology, Female, Humans, Male, Middle Aged, United States epidemiology, Anthrax physiopathology, Bioterrorism, Inhalation Exposure adverse effects
Abstract

From October 4 to November 2, 2001, the first 10 confirmed cases of inhalational anthrax caused by intentional release of Bacillus anthracis were identified in the United States. Epidemiologic investigation indicated that the outbreak, in the District of Columbia, Florida, New Jersey, and New York, resulted from intentional delivery of B. anthracis spores through mailed letters or packages. We describe the clinical presentation and course of these cases of bioterrorism-related inhalational anthrax. The median age of patients was 56 years (range 43 to 73 years), 70% were male, and except for one, all were known or believed to have processed, handled, or received letters containing B. anthracis spores. The median incubation period from the time of exposure to onset of symptoms, when known (n=6), was 4 days (range 4 to 6 days). Symptoms at initial presentation included fever or chills (n=10), sweats (n=7), fatigue or malaise (n=10), minimal or nonproductive cough (n=9), dyspnea (n=8), and nausea or vomiting (n=9). The median white blood cell count was 9.8 X 10(3)/mm(3) (range 7.5 to 13.3), often with increased neutrophils and band forms. Nine patients had elevated serum transaminase levels, and six were hypoxic. All 10 patients had abnormal chest X-rays; abnormalities included infiltrates (n=7), pleural effusion (n=8), and mediastinal widening (seven patients). Computed tomography of the chest was performed on eight patients, and mediastinal lymphadenopathy was present in seven. With multidrug antibiotic regimens and supportive care, survival of patients (60%) was markedly higher (<15%) than previously reported.

Published
2001
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35. Predominant kidney involvement in a fatal case of hantavirus pulmonary syndrome caused by Sin Nombre virus.

Author

Passaro DJ, Shieh WJ, Hacker JK, Fritz CL, Hogan SR, Fischer M, Hendry RM, and Vugia DJ

Subjects
Adult, Antibodies, Viral blood, Antibodies, Viral immunology, DNA, Viral blood, Female, Orthohantavirus genetics, Orthohantavirus immunology, Hantavirus Pulmonary Syndrome immunology, Hantavirus Pulmonary Syndrome physiopathology, Humans, Kidney pathology, Lung immunology, Lung pathology, Lung virology, Orthohantavirus isolation & purification, Hantavirus Pulmonary Syndrome virology, Kidney virology
Abstract

A 27-year-old woman presented to a hospital with symptoms resembling pyelonephritis; respiratory distress did not develop until nearly a day after admission and she subsequently died. The Unexplained Deaths and Critical Illnesses Project of the Centers for Disease Control and Prevention confirmed Sin Nombre virus infection by the results of serological testing and sequencing of the viral genome; staining of Sin Nombre virus antigen in the pulmonary capillaries was relatively weak.

Published
2001
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36. Leptospirosis mimicking acute cholecystitis among athletes participating in a triathlon.

Author

Guarner J, Shieh WJ, Morgan J, Bragg SL, Bajani MD, Tappero JW, and Zaki SR

Subjects
Acute Disease, Adult, Antigens, Bacterial analysis, Cholecystectomy, Cholecystitis microbiology, Diagnosis, Differential, Enzyme-Linked Immunosorbent Assay, Female, Gallbladder microbiology, Humans, Immunohistochemistry, Leptospira immunology, Leptospira isolation & purification, Leptospirosis microbiology, Male, Middle Aged, Sports, Cholecystitis diagnosis, Fever of Unknown Origin diagnosis, Leptospirosis diagnosis
Abstract

Leptospirosis, a disease acquired by exposure to contaminated water, is characterized by fever accompanied by various symptoms, including abdominal pain. An acute febrile illness occurred in athletes who participated in an Illinois triathlon in which the swimming event took place in a freshwater lake. Of 876 athletes, 120 sought medical care and 22 were hospitalized. Two of the athletes had their gallbladders removed because of abdominal pain and clinical suspicion of acute cholecystitis. We applied an immunohistochemical test for leptospirosis to these gallbladders and demonstrated bacterial antigens staining (granular and filamentous patterns) around blood vessels of the serosa and muscle layer. Rare intact bacteria were seen in 1 case. These results show that leptospirosis can mimic the clinical symptoms of acute cholecystitis. If a cholecystectomy is performed in febrile patients with suspicious environmental or animal exposure, pathologic studies for leptospirosis on formalin-fixed, paraffin-embedded tissues may be of great value.

Published
2001
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37. Pathologic studies of fatal cases in outbreak of hand, foot, and mouth disease, Taiwan.

Author

Shieh WJ, Jung SM, Hsueh C, Kuo TT, Mounts A, Parashar U, Yang CF, Guarner J, Ksiazek TG, Dawson J, Goldsmith C, Chang GJ, Oberste SM, Pallansch MA, Anderson LJ, and Zaki SR

Subjects
Enterovirus Infections epidemiology, Enterovirus Infections pathology, Enterovirus Infections virology, Humans, Immunohistochemistry, Taiwan epidemiology, Disease Outbreaks
Abstract

In 1998, an outbreak of enterovirus 71-associated hand, foot, and mouth disease occurred in Taiwan. Pathologic studies of two fatal cases with similar clinical features revealed two different causative agents, emphasizing the need for postmortem examinations and modern pathologic techniques in an outbreak investigation.

Published
2001
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38. Influenza A virus infection complicated by fatal myocarditis.

Author

Nolte KB, Alakija P, Oty G, Shaw MW, Subbarao K, Guarner J, Shieh WJ, Dawson JE, Morken T, Cox NJ, and Zaki SR

Subjects
Antigens, Viral analysis, Autopsy, Child, Fatal Outcome, Female, Forensic Medicine methods, Humans, Immunohistochemistry, In Situ Hybridization, Influenza, Human pathology, Lung pathology, Myocarditis microbiology, Myocarditis pathology, Myocardium pathology, Nasopharynx metabolism, Risk Factors, Influenza A virus, Influenza, Human complications, Myocarditis etiology
Abstract

Influenza virus typically causes a febrile respiratory illness, but it can present with a variety of other clinical manifestations. We report a fatal case of myocarditis associated with influenza A infection. A previously healthy 11-year-old girl had malaise and fever for approximately 1 week before a sudden, witnessed fatal collapse at home. Autopsy revealed a pericardial effusion, a mixed lymphocytic and neutrophilic myocarditis, a mild lymphocytic interstitial pneumonia, focal bronchial/bronchiolar mucosal necrosis, and histologic changes consistent with asthma. Infection with influenza A (H3N2) was confirmed by virus isolation from a postmortem nasopharyngeal swab. Attempts to isolate virus from heart and lung tissue were unsuccessful. Immunohistochemical tests directed against influenza A antigens and in situ hybridization for influenza A genetic material demonstrated positive staining in bronchial epithelial cells, whereas heart sections were negative. Sudden death is a rare complication of influenza and may be caused by myocarditis. Forensic pathologists should be aware that postmortem nasopharyngeal swabs for viral culture and immunohistochemical or in situ hybridization procedures on lung tissue might be necessary to achieve a diagnosis. Because neither culturable virus nor influenza viral antigen could be identified in heart tissue, the pathogenesis of influenza myocarditis in this case is unlikely to be the result of direct infection of myocardium by the virus. The risk factors for developing myocarditis during an influenza infection are unknown.

Published
2000
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39. Acute encephalomyelitis during an outbreak of enterovirus type 71 infection in Taiwan: report of an autopsy case with pathologic, immunofluorescence, and molecular studies.

Author

Hsueh C, Jung SM, Shih SR, Kuo TT, Shieh WJ, Zaki S, Lin TY, Chang LY, Ning HC, and Yen DC

Subjects
Antigens, Viral analysis, Base Sequence, Child, Coxsackievirus Infections pathology, Coxsackievirus Infections virology, DNA Primers chemistry, DNA, Viral analysis, Encephalitis, Viral pathology, Encephalitis, Viral virology, Enterovirus genetics, Enterovirus immunology, Fatal Outcome, Female, Fluorescent Antibody Technique, Indirect, Hand, Foot and Mouth Disease pathology, Hand, Foot and Mouth Disease virology, Humans, Microscopy, Fluorescence, Molecular Sequence Data, Reverse Transcriptase Polymerase Chain Reaction, Coxsackievirus Infections epidemiology, Disease Outbreaks, Encephalitis, Viral epidemiology, Enterovirus isolation & purification, Hand, Foot and Mouth Disease epidemiology
Abstract

We report a fatal case of enterovirus type 71 (EV 71) infection in an 8-year-old girl during a summer outbreak of hand, foot, and mouth disease in 1998 in Taiwan. The clinical course was rapidly progressive, with manifestations of hand, foot, and mouth disease, aseptic meningitis, encephalomyelitis, and pulmonary edema. The patient died 24 hours after admission. Postmortem study revealed extensive inflammation in the meninges and central nervous system and marked pulmonary edema with focal hemorrhage. Brain stem and spinal cord were most severely involved. The inflammatory infiltrates consisted largely of neutrophils involving primarily the gray matter with perivascular lymphocytic cuffing, and neuronophagia. The lungs and heart showed no evidence of inflammation. EV 71 was isolated from the fresh brain tissues and identified by immunofluorescence method with type-specific EV 71 monoclonal antibody. It was also confirmed by neutralization test and reverse-transcriptase polymerase chain reaction with sequence analysis. The present case was the first example in which EV 71 was demonstrated to be the causative agent of fatal encephalomyelitis during its epidemic in Taiwan.

Published
2000
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40. The role of pathology in an investigation of an outbreak of West Nile encephalitis in New York, 1999.

Author

Shieh WJ, Guarner J, Layton M, Fine A, Miller J, Nash D, Campbell GL, Roehrig JT, Gubler DJ, and Zaki SR

Subjects
Antigens, Viral analysis, Autopsy, Brain virology, Humans, Immunohistochemistry, Neurons pathology, Neurons virology, New York City epidemiology, Spinal Cord virology, West Nile Fever epidemiology, West Nile virus immunology, Brain pathology, Disease Outbreaks, Spinal Cord pathology, West Nile Fever pathology, West Nile Fever virology, West Nile virus isolation & purification
Abstract

An outbreak of encephalitis occurred in New York City in late August 1999, the first caused by West Nile virus in North America. Histopathologic and immunopathologic examinations performed on human autopsy materials helped guide subsequent laboratory and epidemiologic investigations that led to identification of the etiologic agent.

Published
2000
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41. Risk factors for Nipah virus infection among abattoir workers in Singapore.

Author

Chew MH, Arguin PM, Shay DK, Goh KT, Rollin PE, Shieh WJ, Zaki SR, Rota PA, Ling AE, Ksiazek TG, Chew SK, and Anderson LJ

Subjects
Adult, Animals, Antibodies, Viral blood, Case-Control Studies, Encephalitis, Viral diagnosis, Encephalitis, Viral transmission, Female, Humans, Immunoglobulin M blood, Malaysia, Male, Occupational Diseases diagnosis, Occupational Diseases virology, Paramyxoviridae Infections diagnosis, Paramyxoviridae Infections transmission, Pneumonia, Viral diagnosis, Pneumonia, Viral transmission, Risk Factors, Singapore epidemiology, Swine, Swine Diseases transmission, Swine Diseases virology, Abattoirs, Disease Outbreaks, Encephalitis, Viral epidemiology, Occupational Diseases epidemiology, Paramyxoviridae Infections epidemiology, Pneumonia, Viral epidemiology, Zoonoses transmission
Abstract

During 10-19 March 1999, 11 workers in 1 of 2 Singaporean abattoirs developed Nipah-virus associated encephalitis or pneumonia, resulting in 1 fatality. A case-control study was conducted to determine occupational risk factors for infection. Case patients were abattoir A workers who had anti-Nipah IgM antibodies; control subjects were randomly selected abattoir A workers who tested negative for anti-Nipah IgM. All 13 case patients versus 26 (63%) of 41 control subjects reported contact with live pigs (P=.01). Swine importation from Malaysian states concurrently experiencing a Nipah virus outbreak was banned on 3 March 1999; on 19 March 1999, importation of Malaysian pigs was banned, and abattoirs were closed. No unusual illnesses among pigs processed during February-March were reported. Contact with live pigs appeared to be the most important risk factor for human Nipah virus infection. Direct contact with live, potentially infected pigs should be minimized to prevent transmission of this potentially fatal zoonosis to humans.

Published
2000
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42. Transmission of Black Creek Canal virus between cotton rats.

Author

Hutchinson KL, Rollin PE, Shieh WJ, Zaki S, Greer PW, and Peters CJ

Subjects
Animals, Antibodies, Viral blood, Antigens, Viral analysis, Disease Reservoirs, Enzyme-Linked Immunosorbent Assay, Female, Orthohantavirus immunology, Hantavirus Pulmonary Syndrome transmission, Hantavirus Pulmonary Syndrome virology, Immunohistochemistry, Infectious Disease Transmission, Vertical, Male, Pregnancy, Pregnancy Complications, Infectious veterinary, RNA, Viral analysis, Rats, Rodent Diseases immunology, Rodent Diseases virology, Orthohantavirus isolation & purification, Hantavirus Pulmonary Syndrome veterinary, Rodent Diseases transmission, Sigmodontinae virology
Abstract

Black Creek Canal (BCC) virus is a hantavirus associated with hantavirus pulmonary syndrome in southeastern North America. The virus was isolated from the spleen of a cotton rat (Sigmodon hispidus) trapped in southern Florida. Our previous studies have shown that we could consistently infect male cotton rats with BCC virus in the laboratory. These animals became persistently infected and virus could be detected in salivary glands, urine, and feces. In this report we show: (1) female and male cotton rats are equally susceptible to BCC virus infection, (2) susceptibility to infection was not influenced by age, (3) all inoculated rats transmitted the infection to uninoculated cage mates, and (4) offspring of infected rats became infected despite the presence of high maternal antibodies. The course of BCC virus infection, as determined by antibody response and the ability to isolate or detect virus, appeared to be similar regardless of whether the rats obtained their infection by inoculation or contact with inoculated rats. J. Med. Virol. 60:70-76, 2000. Published 2000 Wiley-Liss, Inc.

Published
2000
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43. Reversal of virus-induced systemic shock and respiratory failure by blockade of the lymphotoxin pathway.

Author

Puglielli MT, Browning JL, Brewer AW, Schreiber RD, Shieh WJ, Altman JD, Oldstone MB, Zaki SR, and Ahmed R

Subjects
Animals, Antibodies, Monoclonal pharmacology, Disease Models, Animal, Female, Humans, Lymphocytic Choriomeningitis immunology, Lymphocytic Choriomeningitis pathology, Lymphocytic Choriomeningitis therapy, Lymphotoxin beta Receptor, Male, Mice, Mice, Inbred NZB, Respiratory Insufficiency immunology, Respiratory Insufficiency pathology, Shock, Septic immunology, Shock, Septic pathology, Signal Transduction, Time Factors, Receptors, Tumor Necrosis Factor antagonists & inhibitors, Respiratory Insufficiency therapy, Shock, Septic therapy
Abstract

At present, little is known about the pathogenesis of acute virus-induced shock and pulmonary failure. A chief impediment in understanding the underlying disease mechanisms and developing treatment strategies has been the lack of a suitable animal model. This study describes a mouse model of virus-induced systemic shock and respiratory distress, and shows that blockade of the lymphotoxin beta receptor pathway reverses the disease.

Published
1999
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44. Long-term disease surveillance in Bandundu region, Democratic Republic of the Congo: a model for early detection and prevention of Ebola hemorrhagic fever.

Author

Lloyd ES, Zaki SR, Rollin PE, Tshioko K, Bwaka MA, Ksiazek TG, Calain P, Shieh WJ, Kondé MK, Verchueren E, Perry HN, Manguindula L, Kabwau J, Ndambi R, and Peters CJ

Subjects
Adult, Democratic Republic of the Congo epidemiology, Disease Outbreaks prevention & control, Ebolavirus isolation & purification, Hemorrhagic Fever, Ebola prevention & control, Humans, Immunohistochemistry methods, Infection Control, Models, Theoretical, Skin virology, Software Design, Time Factors, Hemorrhagic Fever, Ebola diagnosis, Hemorrhagic Fever, Ebola epidemiology, Population Surveillance methods
Abstract

After the large-scale outbreak of Ebola hemorrhagic fever (EHF) in Bandundu region, Democratic Republic of the Congo, a program was developed to help detect and prevent future outbreaks of EHF in the region. The long-term surveillance and prevention strategy is based on early recognition by physicians, immediate initiation of enhanced barrier-nursing practices, and the use of an immunohistochemical diagnostic test performed on formalin-fixed skin specimens of patients who die of suspected viral hemorrhagic fever. The program was implemented in September 1995 during a 4-day workshop with 28 local physicians representing 17 of 22 health zones in the region. Specimen collection kits were distributed to clinics in participating health zones, and a follow-up evaluation was conducted after 6 months. The use of a formalin-fixed skin specimen for laboratory confirmation of EHF can provide an appropriate method for EHF surveillance when linked with physician training, use of viral hemorrhagic fever isolation precautions, and follow-up investigation.

Published
1999
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45. Isolated case of Ebola hemorrhagic fever with mucormycosis complications, Kinshasa, Democratic Republic of the Congo.

Author

Kalongi Y, Mwanza K, Tshisuaka M, Lusiama N, Ntando E, Kanzake L, Shieh WJ, Zaki SR, Lloyd ES, Ksiazek TG, and Rollin PE

Subjects
Adult, Antibodies, Viral blood, Antigens, Viral metabolism, Blindness etiology, Democratic Republic of the Congo, Ebolavirus immunology, Ebolavirus isolation & purification, Eyelid Diseases complications, Eyelid Diseases microbiology, Eyelid Diseases virology, Female, Hemorrhagic Fever, Ebola diagnosis, Hemorrhagic Fever, Ebola virology, Humans, Immunoglobulin G blood, Immunoglobulin M blood, Mucormycosis microbiology, Mucormycosis virology, Opportunistic Infections complications, Opportunistic Infections microbiology, Opportunistic Infections virology, Hemorrhagic Fever, Ebola complications, Mucormycosis complications
Abstract

A patient with undiagnosed Ebola (EBO) hemorrhagic fever (EHF) was transferred from Kikwit to a private clinic in Kinshasa, Democratic Republic of the Congo. A diagnosis of EHF was suspected on clinical grounds and was confirmed by detection of EBO virus-specific IgM and IgG in serum of the patient. During the course of the disease, although she had no known predisposing factors, the patient developed a periorbital mucormycosis abscess on eyelid tissue that was biopsied during surgical drainage; the abscess was histologically confirmed. Presence of EBO antigen was also detected by specific immunohistochemistry on the biopsied tissue. The patient survived the EBO infection but had severe sequelae associated with the mucormycosis. Standard barrier-nursing precautions were taken upon admission and upgraded when EHF was suspected; there was no secondary transmission of the disease.

Published
1999
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46. A novel immunohistochemical assay for the detection of Ebola virus in skin: implications for diagnosis, spread, and surveillance of Ebola hemorrhagic fever. Commission de Lutte contre les Epidémies à Kikwit.

Author

Zaki SR, Shieh WJ, Greer PW, Goldsmith CS, Ferebee T, Katshitshi J, Tshioko FK, Bwaka MA, Swanepoel R, Calain P, Khan AS, Lloyd E, Rollin PE, Ksiazek TG, and Peters CJ

Subjects
Adolescent, Adult, Aged, Antigens, Viral metabolism, Democratic Republic of the Congo epidemiology, Disease Outbreaks, Ebolavirus immunology, Ebolavirus ultrastructure, Female, Hemorrhagic Fever, Ebola epidemiology, Hemorrhagic Fever, Ebola transmission, Humans, Immunohistochemistry statistics & numerical data, Inclusion Bodies, Viral ultrastructure, Infant, Liver pathology, Liver virology, Male, Microscopy, Electron, Middle Aged, Retrospective Studies, Sensitivity and Specificity, Skin pathology, Ebolavirus isolation & purification, Hemorrhagic Fever, Ebola diagnosis, Immunohistochemistry methods, Skin virology
Abstract

Laboratory diagnosis of Ebola hemorrhagic fever (EHF) is currently performed by virus isolation and serology and can be done only in a few high-containment laboratories worldwide. In 1995, during the EHF outbreak in the Democratic Republic of Congo, the possibility of using immunohistochemistry (IHC) testing of formalin-fixed postmortem skin specimens was investigated as an alternative diagnostic method for EHF. Fourteen of 19 cases of suspected EHF met the surveillance definition for EHF and were positive by IHC. IHC, serologic, and virus isolation results were concordant for all EHF and non-EHF cases. IHC and electron microscopic examination showed that endothelial cells, mononuclear phagocytes, and hepatocytes are main targets of infection, and IHC showed an association of cellular damage with viral infection. The finding of abundant viral antigens and particles in the skin of EHF patients suggests an epidemiologic role for contact transmission. IHC testing of formalin-fixed skin specimens is a safe, sensitive, and specific method for laboratory diagnosis of EHF and should be useful for EHF surveillance and prevention.

Published
1999
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47. Epidemic leptospirosis associated with pulmonary hemorrhage-Nicaragua, 1995.

Author

Trevejo RT, Rigau-Pérez JG, Ashford DA, McClure EM, Jarquín-González C, Amador JJ, de los Reyes JO, Gonzalez A, Zaki SR, Shieh WJ, McLean RG, Nasci RS, Weyant RS, Bolin CA, Bragg SL, Perkins BA, and Spiegel RA

Subjects
Adolescent, Adult, Animals, Case-Control Studies, Cattle, Child, Child, Preschool, Disasters, Disease Outbreaks, Disease Vectors, Dogs, Hemorrhage microbiology, Horses, Humans, Incidence, Infant, Leptospira classification, Leptospira isolation & purification, Leptospirosis complications, Leptospirosis microbiology, Lung Diseases microbiology, Nicaragua epidemiology, Rodentia, Swine, Water Microbiology, Hemorrhage complications, Leptospirosis epidemiology, Lung Diseases complications
Abstract

In October 1995, epidemic "hemorrhagic fever," without jaundice or renal manifestations, was reported in rural Nicaragua following heavy flooding; 2259 residents were evaluated for nonmalarial febrile illnesses (cumulative incidence, 6.1%) and 15 (0.7%) died with pulmonary hemorrhage. A case-control study found that case-patients were more likely than controls to have ever walked in creeks (matched odds ratio [MOR], 15.0; 95% confidence interval [CI], 1.7-132.3), have household rodents (MOR, 10.4; 95% CI, 1.1-97.1), or own dogs with titers >/=400 to Leptospira species (MOR, 23.4; 95% CI, 3.6-infinity). Twenty-six of 51 case-patients had serologic or postmortem evidence of acute leptospirosis. Leptospira species were isolated from case-patients and potential animal reservoirs. This leptospirosis epidemic likely resulted from exposure to flood waters contaminated by urine from infected animals, particularly dogs. Leptospirosis should be included in the differential diagnosis for nonmalarial febrile illness, particularly during periods of flooding or when pulmonary hemorrhage occurs.

Published
1998
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48. An outbreak of hantavirus pulmonary syndrome, Chile, 1997.

Author

Toro J, Vega JD, Khan AS, Mills JN, Padula P, Terry W, Yadón Z, Valderrama R, Ellis BA, Pavletic C, Cerda R, Zaki S, Shieh WJ, Meyer R, Tapia M, Mansilla C, Baro M, Vergara JA, Concha M, Calderon G, Enria D, Peters CJ, and Ksiazek TG

Subjects
Adult, Child, Preschool, Chile epidemiology, Female, Hantavirus Pulmonary Syndrome pathology, Hantavirus Pulmonary Syndrome physiopathology, Humans, Male, Disease Outbreaks, Orthohantavirus, Hantavirus Pulmonary Syndrome epidemiology
Abstract

An outbreak of 25 cases of Andes virus-associated hantavirus pulmonary syndrome (HPS) was recognized in southern Chile from July 1997 through January 1998. In addition to the HPS patients, three persons with mild hantaviral disease and one person with asymptomatic acute infection were identified. Epidemiologic studies suggested person-to-person transmission in two of three family clusters. Ecologic studies showed very high densities of several species of sigmodontine rodents in the area.

Published
1998
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49. Immunohistochemical and in situ localization of Crimean-Congo hemorrhagic fever (CCHF) virus in human tissues and implications for CCHF pathogenesis.

Author

Burt FJ, Swanepoel R, Shieh WJ, Smith JF, Leman PA, Greer PW, Coffield LM, Rollin PE, Ksiazek TG, Peters CJ, and Zaki SR

Subjects
Adolescent, Adult, Aged, Antibodies, Viral immunology, Antigens, Viral analysis, Base Sequence, DNA Primers chemistry, Female, Hemorrhagic Fever Virus, Crimean-Congo immunology, Hemorrhagic Fever, Crimean immunology, Hemorrhagic Fever, Crimean pathology, Humans, Immunohistochemistry, In Situ Hybridization, Intestines immunology, Intestines pathology, Intestines virology, Liver immunology, Liver pathology, Lung immunology, Lung pathology, Lung virology, Male, Middle Aged, Molecular Sequence Data, RNA Probes, Retrospective Studies, Spleen immunology, Spleen pathology, Spleen virology, Hemorrhagic Fever Virus, Crimean-Congo isolation & purification, Hemorrhagic Fever, Crimean etiology, Liver virology
Abstract

Background: Crimean-Congo hemorrhagic fever (CCHF) is a potentially fatal disease that occurs in parts of Africa, Asia, and eastern Europe, and that is caused by a recently emerged bunyavirus. Rapid laboratory diagnosis of CCHF infection is essential and is currently performed by virus isolation and serology. Histopathologic studies have been limited to a small number of cases, and little is known about the cellular tropism of CCHF virus and the pathogenesis of this disease., Design: We conducted a retrospective case analysis of 12 patients with a diagnosis of CCHF infection, confirmed by virus isolation, who were evaluated at the Special Pathogens Unit, National Institute for Virology, South Africa. The clinicopathologic features of CCHF and the diagnostic role of virus isolation as compared with serology, immunohistochemistry, and in situ hybridization were evaluated. Additionally, the distribution of CCHF virus in human tissues was examined., Results: The clinical and histopathologic features of CCHF resemble those of other viral hemorrhagic fevers. Of the 12 patients with virus isolation-confirmed CCHF infection, 5 were positive by serology, 10 by immunohistochemistry, and 5 by in situ hybridization. Immunohistochemistry and in situ hybridization analyses showed that the mononuclear phagocytes, endothelial cells, and hepatocytes are main targets of infection. Association of parenchymal necrosis in liver with viral infection suggests that cell damage may be mediated by a direct viral cytopathic effect., Conclusions: The diagnosis of CCHF, suspected by history and clinical features, can be supported histopathologically. However, since the pathologic features resemble those of other viral hemorrhagic fevers, an unequivocal diagnosis can be made only by laboratory tests. The utility of immunohistochemistry as a sensitive and rapid diagnostic modality was established by the high degree of concordance with virus isolation. Infection of mononuclear phagocytes, endothelial cells, and hepatocytes may play a critical role in the pathogenesis of CCHF.

Published
1997

50. Effect of environmental factors on whole plant assimilate partitioning and associated gene expression.

Author

Geiger DR, Koch KE, and Shieh WJ

Abstract

Partitioning of assimilated carbon among sink organs is a critical factor that controls the rate and pattern of plant growth. Time-course measurements of plant and organ growth rates are useful for determining how regulation of carbon partitioning controls plant growth. Measuring growth rates over a 24 h period reveals the current pattern of carbon partitioning that can be used to predict growth rates of specific sinks. Comparison of growth rates among sinks under defined conditions can point out key factors that regulate partitioning of recently assimilated carbon among sinks. Internal control of carbon partitioning by developmental programmes regulates the timing and site of carbon distribution among developing parts, thereby establishing the adaptive traits of a species, cultivar or transgenic construct. Regulation of partitioning in response to environmental factors establishes or restores allometric growth among plant parts and functional balance between the supply and use of carbon. Environmental stress often restricts resource availability while successful acclimation sets in motion processes that restore the supply. A key mechanism contributing to regulation of carbon partitioning is an expression of genes that control activity of the enzymes which initiate sucrose metabolism at specific sites and stages of ontogeny.

Published
1996
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