| Literature DB >> 23342375 |
Randy E Sacco1, Jodi L McGill, Mitchell V Palmer, John D Lippolis, Timothy A Reinhardt, Brian J Nonnecke.
Abstract
Respiratory syncytial virus (RSV) is the most common viral cause of childhood acute lower respiratory tract infections. It is estimated that RSV infections result in more than 100,000 deaths annually worldwide. Bovine RSV is a cause of enzootic pneumonia in young dairy calves and summer pneumonia in nursing beef calves. Furthermore, bovine RSV plays a significant role in bovine respiratory disease complex, the most prevalent cause of morbidity and mortality among feedlot cattle. Infection of calves with bovine RSV shares features in common with RSV infection in children, such as an age-dependent susceptibility. In addition, comparable microscopic lesions consisting of bronchiolar neutrophilic infiltrates, epithelial cell necrosis, and syncytial cell formation are observed. Further, our studies have shown an upregulation of pro-inflammatory mediators in RSV-infected calves, including IL-12p40 and CXCL8 (IL-8). This finding is consistent with increased levels of IL-8 observed in children with RSV bronchiolitis. Since rodents lack IL-8, neonatal calves can be useful for studies of IL-8 regulation in response to RSV infection. We have recently found that vitamin D in milk replacer diets can be manipulated to produce calves differing in circulating 25-hydroxyvitamin D3. The results to date indicate that although the vitamin D intracrine pathway is activated during RSV infection, pro-inflammatory mediators frequently inhibited by the vitamin D intacrine pathway in vitro are, in fact, upregulated or unaffected in lungs of infected calves. This review will summarize available data that provide parallels between bovine RSV infection in neonatal calves and human RSV in infants.Entities:
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Year: 2012 PMID: 23342375 PMCID: PMC3528288 DOI: 10.3390/v4123731
Source DB: PubMed Journal: Viruses ISSN: 1999-4915 Impact factor: 5.048
Figure 1Lung from an RSV-infected calf at day 7 post-infection. Note multifocal to coalescing areas of plum-red consolidation in cranial and ventral aspects of right cranial and middle lobes. Consolidated areas surround and divide foci of pale pink hyperinflated lung (arrow). Scattered multifocal areas of consolidation are also present in the ventral third of the right caudal lobe (arrowheads). Original figure: [31].
Figure 2Histological lesions observed in lung of calves after experimental infection with bovine RSV. Calves were challenged via aerosol with bovine RSV. On day 7 post-infection, samples of lung were collected for histological evaluation. A representative image from a single calf is shown. (A) Moderate interstitial thickening and wide interlobular septae due to edema. Original magnification, 4X. (B) Alveolar septae are thickened due to cellular infiltrates found to be macrophages, lymphocytes and lesser numbers of neutrophils when viewed at higher magnification. Original magnification, 20X. (C) Bronchioles are filled with neutrophils, sloughed epithelial cells, and necrotic cell debris. Original magnification, 20X. (D) There is partial to complete loss of bronchiolar epithelial cells with attenuation of remaining cells. In some bronchioles, epithelial cells form multinucleated syncytial cells (arrows). Original magnification, 40X. Figure adapted from: [31].
Features common to hRSV in infants and bRSV in calves.
| Feature | Human RSV | Bovine RSV | References |
|---|---|---|---|
| Age-dependency | More prevalent in children <2 yrs old | More prevalent in calves <6 mo old | [ |
| Seasonal periodicity | More common in fall and winter | More common in fall and winter | [ |
| Histopathology | Bronchiolitis; interstitial pneumonia; | Bronchiolitis; interstitial pneumonia; | [ |
| Prominent neutrophil and macrophage infiltration | Prominent neutrophil and macrophage infiltration | ||
| CXC chemokines | CXCL8 (IL-8) upregulated | CXCL8 (IL-8) upregulated | [ |
| Adaptive immunity | Th2 cytokine bias | Th2 cytokine bias | [ |
| Vaccine-enhanced disease | Observed with formalin-inactivated vaccine | Observed with formalin-inactivated vaccine | [ |