Literature DB >> 26798703

Inflammatory Cell Infiltrates in Acute and Chronic Thoracic Aortic Dissection.

Darrell Wu1, Justin C Choi2, Aryan Sameri2, Charles G Minard3, Joseph S Coselli2, Ying H Shen2, Scott A LeMaire1.   

Abstract

BACKGROUND: Thoracic aortic dissection (TAD) is a highly lethal cardiovascular disease. Injury to the intima and media allows pulsatile blood to enter the media, leading to dissection formation. Inflammatory cells then infiltrate the site of aortic injury to clear dead cells and damaged tissue. This excessive inflammation may play a role in aneurysm formation after dissection.
METHODS: Using immunohistochemistry, we compared aortic tissues from patients with acute TAD (n = 11), patients with chronic TAD (n = 35), and donor controls (n = 20) for the presence of CD68+ macrophages, neutrophils, mast cells, and CD3+ T lymphocytes.
RESULTS: Tissue samples from patients with acute or chronic TAD generally had significantly more inflammatory cells in both the medial and adventitial layers than did the control samples. In tissues from patients with acute TAD, the adventitia had more of the inflammatory cells studied than did the media. The pattern of increase in inflammatory cells was similar in chronic and acute TAD tissues, except for macrophages, which were seen more frequently in the adventitial layer of acute TAD tissue than in the adventitia of chronic TAD tissue.
CONCLUSIONS: The inflammatory cell content of both acute and chronic TAD tissue was significantly different from that of control tissue. However, the inflammatory cell profile of aneurysmal chronic TAD was similar to that of acute TAD. This may reflect a sustained injury response that contributes to medial degeneration and aneurysm formation.

Entities:  

Keywords:  Inflammation; Macrophage; Mast cell; Neutrophil; T lymphocyte; Thoracic aortic dissection

Year:  2013        PMID: 26798703      PMCID: PMC4682718          DOI: 10.12945/j.aorta.2013.13-044

Source DB:  PubMed          Journal:  Aorta (Stamford)        ISSN: 2325-4637


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