(A–D) EM images. Naive pancreas shows normal zymogen granules (white arrows), normal nuclei (black arrows), and normal endoplasmic reticulum (yellow arrows) (A). Two days after AcA infusion, pancreata showed abnormal acinar cells with signs of cell injury and necrosis (B–D). In B and D, pleomorphic nuclei (black arrows), mitochondrial swelling (red arrow), disorganized rough endoplasmic reticulum (yellow arrows), and debris-filled vacuoles (green arrows). In C, abnormal appearing zymogen granules (white arrow), pleomorphic nuclei (black arrows), enlarged Golgi apparatus (blue arrow), and disorganized rough endoplasmic reticulum (yellow arrows). n = 3/time-point. Scale bars: 5 μm (A–C); 2 μm (D). (E) In vitro cell viability assessed by PI staining using flow cytometry comparing acinar cell clusters and isolated islets 1 hour after harvesting. Acinar and islet viability were normalized to their respective control acini and islets not exposed to 1% AcA. Viability of the islet cells was significantly higher than acinar cells after exposure to AcA at 1 and 5 minutes (n = 3/time point in each group). Two-way repeated-measures ANOVA followed by Holm-Šidák test for multiple comparisons. F_2,8=832.9; P < 0.0001. ****P < 0.0001. (F) In vitro cell viability assessed by PI staining using flow cytometry comparing intact islets (dissociated with trypsin after exposure to 1% AcA) and dissociated islets (dissociated with trypsin before exposure to AcA) 24 hours after harvesting. Islet cell viability was normalized to their respective control not exposed to AcA. The viability of the intact islet cells was significantly higher than the dissociated islet cells after exposure to AcA at 1 and 5 minutes. n = 3/time point in the intact islets group; n = 2/time point in the dissociated islets group. Two-way repeated-measures ANOVA followed by Holm-Šidák test for multiple comparisons. F_2,8=462.2; P < 0.0001. ****P < 0.0001.