|
|||||
|
|
Recent advances in understanding the pathogenesis of the hemolytic uremic syndromes |
|
| Authors: | Bernard S. Kaplan Thomas G. Cleary Thomas G. Obrig |
| Affiliation: | (1) Division of Nephrology, The Children's Hospital of Philadelphia, University of Philadelphia, 19104 Philadelphia, USA;(2) Division of Pediatric Infectious Diseases, University of Texas Medical School at Houston, 77225 Houston, TX, USA;(3) Department of Microbiology and Immunology, Albany Medical College, 12208 Albany, NY, USA |
| Abstract: | One of the requirements for an agent to cause hemolytic uremic syndrome (HUS) is its ability to injure endothelial cells. Shiga-like toxin (SLT) can do this. SLT is produced byEscherichia coli andShigella dysenteriae serotype 1; both have been implicated as causes of typical HUS. Endothelial cells have receptors (GB3) for SLT and the toxin can inhibit eukaryotic protein synthesis, thereby causing cell death. Glomerular endothelial cell injury or death results in a decreased glomerular filtration rate and many of the perturbations seen in HUS. It is no longer certain that hemolysis is the result of a microangiopathy. Cell injury results in release of von Willebrand multimers; if these are ultra-large, thrombosis may ensue. There is also increasing evidence that neutrophils have a role in the pathogenesis of typical HUS.Streptococcus pneumoniae can also cause HUS and care must be taken to avoid giving plasma to patients withS. pneumoniae-associated HUS. There is compelling evidence that types of HUS are inherited by autosomal recessive and autosomal dominant modes. Patients with autosomal recessive HUS may have recurrent episodes. Mortality and morbidity rates are high for the inherited forms. |
| Keywords: | Hemolytic uremic syndrome Escherichia coli 0157 |
| 本文献已被 SpringerLink 等数据库收录! | |