Types of Disease and Pathological Changes

C. septicum is common in soil and the intestinal tract of most animal species. It causes myonecrosis known as malignant edema in cattle, sheep, pigs, horses, and other animals of all ages (Otter and Uzal 2020). This is a gas gangrene and is not easily distinguished from similar disease caused by C. perfringens, C. novyi, and P. sordellii. In the abomasum of sheep, the disease is sometimes known as braxy in the United States, Australia, and Europe. This disease affects young unvaccinated sheep that have been feeding on frosted root crops and frozen grass and it is therefore seen in the winter months. The frozen feed damages the mucosal epithelium of the abomasum, which allows C. septicum already present to colonize the tissue causing abomasitis and enterotoxemia (Chapter 28). C. septicum also causes necrotizing enterocolitis in humans.

Unlike blackleg, malignant edema is caused by introduction of the pathogen into a wound, and the wound must be sufficient to cause anaerobic conditions. Where a wound is contaminated with soil or feces, this may include facultative anaerobes such as Enterobacterales. These grow vigorously in the wound and consume available oxygen, causing the anoxic conditions needed for growth of anaerobes. Once clostridial spores have germinated, the vegetative organism produces the plethora of enzymes and toxins that cause further tissue damage and initiate the characteristic myonecrosis (Figure 29.2). At this stage the facultative organism may be overtaken by, or irrelevant to, the aggressive, toxin‐driven clostridial infection.

Virulence Factors and Pathogenomics

The toxin of primary importance in disease from C. septicum is the α‐toxin (Csa; Kennedy et al. 2005). This toxin is a lethal and necrotizing, β‐barrel, pore‐forming cytolysin belonging to the same family as aerolysin from Aeromonas hydrophila and the ɛ‐toxin from C. perfringens types B and D. C. septicum α‐toxin is encoded by the csa gene and is secreted as an inactive 46‐kDa monomer. The toxin binds to glycosylphosphatidylinositol (GPI)‐anchored proteins on the cell surface and is then cleaved to its 43‐kDa active form by host‐ cell‐associated proteases (Gordon et al. 1997). It has been demonstrated to be essential for the virulence of C. septicum: deletion of the csa gene causes C. septicum to be avirulent in the mouse model of myonecrosis and complementation of the mutation with the wildtype csa gene restores its pathogenic ability.

As the 43 kDa toxin forms aggregates (oligomers) on the cell surface, it undergoes a conformational change such that the β‐hairpin transmembrane domain within domain 2 is exposed and the oligomer forms a heptameric prepore β‐barrel structure. This is then inserted into the host‐cell membrane to form a pore of approximately 1.6 nm. Formation of these pores in the host cells has been shown to be essential for the pathogenesis of disease. Furthermore, because the α‐toxin can bind to different types of GPI‐anchored proteins of different animal species, the toxin can form pores in a broad range of animal host cells.

Additional toxins of C. septicum are thought to contribute to the development of lesions. The beta‐toxin is a DNase; gamma‐toxin is a hyaluronidase and delta‐toxin as an oxygen‐labile hemolysin. There is also a neuraminidase and a cholesterol‐dependent cytolysin known as septicolysin.

Pathogenesis

The lesions of malignant edema begin with rapid swelling at the wound site, which becomes distended with gas (emphysema). Swelling is due to inflammation, bloody subcutaneous edema fluid, and gas (CO₂ and H₂) produced from the rapid fermentation of sugars and other compounds by the Clostridium. As the lesion develops, it comprises necrotic muscle and fascia. The diseased animal will become systemically ill and die, usually within 36 hours of the lesion first developing.

Types of Disease and Pathological Changes

C. chauvoei causes blackleg in cattle, sometimes also known as blackquarter or by other local names. This is a severe myositis, or myonecrosis, responsible for killing young cattle (aged 2–24 months) worldwide. The disease progresses rapidly with high mortality. Animals are sometimes found dead without previous clinical signs; others show difficulty walking and become recumbent before dying.

The lesions are usually in skeletal muscle, such as the leg or neck muscles, but may be found in the diaphragm or even the tongue. They are sometimes very large lesions of hemorrhagic and necrotic tissue that appear very dark, almost black, in color (Figure 29.3). There are sometimes pockets of emphysema, and serosanguinous fluid is often present. Lesions may also occur in the heart, sometimes multiple lesions, together with fibrinous exudate in the pericardial sac. If trauma is required for anaerobic conditions to initiate spore germination, it is difficult to see how that might occur in the heart, although racing frantically to escape biting flies might be one explanation. However, other factors might cause altered redox or ischemia in the heart muscle that allows the infection to begin, or perhaps a different trigger starts the activation of spores in that site.

Virulence Factors and Pathogenomics

During growth, toxins and enzymes are produced. These include a neuraminidase (NanA) that is thought to have an important role in degradation of tight junctions and hyaluronidase (NagH), both of which contribute to rapid spreading of the lesion. Another factor involved in spreading is motility and so the flagellae are considered to be necessary for lesion development. However, the most likely toxin required for the production of the lesions is the cytotoxin CctA. This is a β‐barrel pore‐forming toxin of 32 kDa and a member of the pore‐forming leukocidin superfamily related to the well characterized α‐toxin of Staphylococcus aureus and Staphylococcus pseudintermedius. CctA is the main hemolytic and cytotoxic protein produced by C. chauvoei. Recombinant CctA has also been shown to provide protection as an immunizing antigen against blackleg (Frey et al. 2012

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