Basics Definition
Yüklə 1,38 Mb. Pdf görüntüsü
|
|
Anthrax
Basics [Fig-1] Pathophysiology B anthracis endospores enter the body by inhalation, ingestion, injection, or most commonly, via a cut or abrasion. The spores, initially engulfed by macrophages, germinate within these cells to become vegetative bacteria. [22] Vegetative bacteria secrete two exotoxins: oedema toxin and lethal toxin. Oedema toxin contains oedema factor, a calmodulin-dependent adenylate cyclase responsible for inhibition of neutrophil function and the massive oedema associated with cutaneous infection. [23] [24] [25] [26] Lethal toxin is a zinc metalloprotease that stimulates the release of reactive oxygen intermediates and macrophage production of pro-inflammatory cytokines such as tumour necrosis factor and interleukin-1-beta; release of this toxin in systemic infection can lead to sudden death. [27] [28] [29] Both exotoxins are plasmid-mediated and binary, requiring a common binding protein (protective antigen) for entry into the host cell. Cutaneous anthrax is a consequence of low-level, local spore germination resulting in site-specific oedema and necrosis. The primary lesion develops 1 to 7 days after inoculation, progressing into a necrotic eschar accompanied by local oedema within 48 hours. In ingestion anthrax, ingested spores also cause local disease upon germination, resulting in mucosal oedema, ulceration, and ascites formation. [2] Limited oropharyngeal anthrax can also occur with ingestion of spores. In these cases, local spore deposition and germination lead to sore throat, dysphagia, cervical oedema, and local lymphadenitis. Inhalation anthrax is often more severe and may lead to systemic infection. Inhaled spores are engulfed by alveolar macrophages and are transported to mediastinal and peribronchial lymph nodes as they germinate. Triggers responsible for germination are unclear as spores can remain dormant for 2 to 43 days after exposure. [7] B anthracis bacilli subsequently multiply in regional lymph nodes, leading to pulmonary lymphoedema and haemorrhagic mediastinitis. Haematogenous dissemination results in toxaemia, septicaemia, and death. In rare instances, lymphatic or haematogenous spread of B anthracis may also be a complication of cutaneous or ingestion anthrax. Systemic disease can result in anthrax meningitis, characterised by extensive cerebral oedema, inflammatory and haemorrhagic infiltration, and rapid neurological degeneration. [30] Yüklə 1,38 Mb. Dostları ilə paylaş:
|