AI Article Synopsis

  • The third-stage larvae of Angiostrongylus cantonensis secrete a proteolytic enzyme crucial for penetrating the intestinal wall and developing fully.
  • The protease exhibits activity at an optimal pH of 10.0 and has collagenolytic and elastinolytic functions, which are inhibited by specific protease inhibitors.
  • Experiments showed that adding these inhibitors significantly reduced the larvae's ability to penetrate the intestines, indicating the enzyme's role in their entry into the host's bloodstream.

Article Abstract

The infective third-stage larvae of Angiostrongylus cantonensis secrete a proteolytic enzyme that is thought to be essential for both larval penetration into the intestinal wall of the host and full development. Protease activity in these larvae during culture in vitro was determined by zymography, pH optimum, and substrate and inhibitor specificity. Excretory-secretory (ES) products of the third-stage larvae showed protease activity as three bands with molecular masses of 66, 30, and 23 kD by gelatin zymography. The optimal pH value for this protease activity was 10.0. The protease was found to have collagenolytic as well as elastinolytic activity, but these activities were inhibited by serine protease or metalloprotease inhibitors. The importance of this protease in larval penetration of the intestinal wall and entering the blood stream was observed in vitro by cocultured third-stage larvae of A. cantonensis with specific protease inhibitors in the intestines of BALB/c mice. The penetration rates of larvae significantly decreased when serine protease or metalloprotease inhibitors were added to the intestines. These results showed that serine protease and metalloprotease in ES products of A. cantonensis third-stage larvae are associated with larval penetration of the intestinal walls of mice.

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