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1 ed toxicity (five thromboembolic events, one bowel perforation).
2         Two patients had a delayed diagnosed bowel perforation.
3 lar access thrombosis (2%), stroke (2%), and bowel perforation (1%).
4 ed deaths (disseminated disease, 4 patients; bowel perforation, 1 patient).
5 ntestinal stoma formation in children, while bowel perforation (14, 31.8%) was the main indications i
6  with inadequate distribution (7%) and small-bowel perforation (3%) make the otherwise less toxic 32P
7  despite the PKD group's higher incidence of bowel perforation and increased age at time of transplan
8 colonoscopy-related complications, including bowel perforation and major bleeding.
9 On multivariable analysis, bile duct injury, bowel perforation, and high clinical severity were assoc
10 ocedures (hepatic arterial hemorrhage, small bowel perforation, and liver decompensation salvaged by
11 onal age, ductus closure, occurrence of NEC, bowel perforation, and mortality.
12 atment were gastrointestinal bleeding, small-bowel perforation, and the development of enterocolic fi
13 A on colonoscopy complications, specifically bowel perforation, aspiration pneumonia, and splenic inj
14 %) in emergency neonatal surgeries involving bowel perforation, bowel resection, congenital diaphragm
15                                              Bowel perforation can lead to significant bacterial spil
16                      The primary outcome was bowel perforation, defined using a validated algorithm.
17 al adhesions are at potential higher risk of bowel perforation during implantation of an indwelling p
18 e that typhoid fever accounts for 43% of all bowel perforation during the period of enhanced surveill
19                                Delayed small bowel perforation following BAT is thought to occur seco
20 is is the first case report of delayed small bowel perforation following BAT with extensive portomese
21 re of any other case report of delayed small bowel perforation following BAT without signs of intraab
22                               Isolated small bowel perforation following blunt abdominal trauma (BAT)
23 sity contributed to extensive hemorrhage and bowel perforation for each tissue above a certain energy
24 cate that there is increased risk of NEC and bowel perforation in premature infants with PDA receivin
25 ctivated FXII (FXIIa) modifies the course of bowel perforation-induced peritoneal sepsis in mice.
26 idity and mortality rates, and delayed small bowel perforation is even rarer.
27 cations included bile duct injury (n = 397), bowel perforation (n = 96), and hemorrhage (n = 78).
28              As major complication one small bowel perforation occurred (1/59; 1.7%).
29 reased risk of aspiration pneumonia, but not bowel perforation or splenic injury.
30                                           No bowel perforations or fistulas occurred.
31 (OR 1.71, 95% CI 1.31-2.24), small and large bowel perforation (OR 4.33, 95% CI 4.12-4.56), and pepti
32 (OR 4.06, 95% CI 3.03-5.44), small and large bowel perforation (OR 6.97, 95% CI 6.60-7.37), and pepti
33          Progression-free survival (PFS) and bowel perforation rates were taken from recently reporte
34 cept for acute medical conditions, including bowel perforation (relative risk [RR] = 3.0, 95% confide
35                         Vascular thromboses, bowel perforation, septicemia, and retransplantation, ea
36   Treatment with 14E11 within 12 hours after bowel perforation significantly improved survival compar
37 ications (bleeding, transfusion requirement, bowel perforation, surgical intervention, and graft loss
38 GOG 218 at the baseline estimates of PFS and bowel perforation, the cost of PC was $2.5 million, comp
39                                              Bowel perforation was noted in 27 cases (30%).
40 events such as hypertension, thrombosis, and bowel perforation were also observed at rates consistent
41 was seen with the 7-day infusions (including bowel perforation), with 600,000 IU/m2 as the maximum-to