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The history of appendicitis has been briefly reviewed and a plea made for a renewed interest in this disease on the part of all physicians.A series of one hundred consecutive cases of acute suppurative appendicitis, with two deaths, has been presented. In twenty-five of these the appendix had perforated with one death—a mortality rate of 4.0 per cent. In the seventy-five cases without perforation there was one death—a mortality rate of 1.33 per cent. The mortality rate for the entire series was 2.0 per cent.These attacks occurred for the most part in young and middle aged patients, 70 per cent being less than thirty years old and 80 per cent less than forty.The symptoms as seen in this series have been presented as follows: pain, tenderness, rigidity, vomiting, rapid pulse, fever, leucocytosis, diarrhea and constipation. The constant presence of pain, although not usually severe, and the overwhelming frequency of tenderness and rigidity have been pointed out. Nausea and vomiting in association with abdominal pain have been emphasized as of major significance.The importance of early diagnosis and operation and their relationship to mortality and morbidity has been stressed.The danger of laxatives has been reiterated.Treatment has been discussed with a plea for early operation.The advantages of certain points in technic have been mentioned.A frank statement of the need for more and earlier consultations in suspected appendicitis and a discussion of the responsibilities of both physician and surgeon have been presented.  相似文献   
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Several case reports have implicated Ginkgo biloba in clinically adverse bleeding disorders. Ginkgo biloba has been reported to increase pain-free walking distance among patients with peripheral artery disease (PAD). Standard PAD therapy includes 325 mg/day aspirin. The objective of this study was to examine potential adverse effects of concomitant aspirin and Ginkgo biloba on platelet function. Ginkgo biloba (EGb 761, 300 mg/day) was compared with placebo for effects on measures of platelet aggregation among adults consuming 325 mg/day aspirin in a randomized, double-blind, placebo-controlled, parallel design trial of 4-week duration. Participants were adults, age 69 +/- 10 years, with PAD or risk factors for cardiovascular disease. Outcome measures included platelet function analysis (PFA-100 analyzer) using ADP as an agonist (n = 26 placebo; n = 29 ginkgo), and platelet aggregation using ADP, epinephrine, collagen and ristocetin as agonists (n = 21 placebo; n = 23 ginkgo). Participants kept daily logs of bleeding or bruising episodes. There were no clinically or statistically significant differences between treatment groups for any agonists, for either PFA-100 analysis or platelet aggregation. Reports of bleeding or bruising were infrequent and similar for both study groups. In conclusion, in older adults with PAD or cardiovascular disease risk, a relatively high dose of Ginkgo biloba combined with 325 mg/day daily aspirin did not have a clinically or statistically detectable impact on indices of coagulation examined over 4 weeks, compared with the effect of aspirin alone. No adverse bleeding events were observed, although the trial was limited to a small sample size.  相似文献   
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BACKGROUND: Studies have shown that alcoholics have smaller brain volumes than non-alcoholic cohorts, but an effect of family history (FH) of heavy drinking on brain volume has not been demonstrated. We examined the relationship between an FH of heavy drinking and both brain shrinkage as measured by the ratio of brain volumes to intracranial volume (ICV) as well as maximal brain growth as measured by ICV in early-onset and late-onset alcoholics. METHODS: With T1-weighted resonance imaging, we measured ICV, brain volume, and white and gray matter volume in adult treatment-seeking late-onset and early-onset alcoholics with either a positive or a negative FH of heavy alcohol use, and in healthy control subjects. We also calculated brain shrinkage using a ratio of soft tissue volumes to ICV. RESULTS: The FH positive alcoholic patients had significantly smaller ICVs than FH negative patients, suggesting smaller premorbid brain growth. Brain shrinkage did not correlate with FH. Late-onset alcoholics showed a greater difference in ICV between FH positive and FH negative patients than early-onset alcoholics. Late-onset FH positive patients also had significantly lower IQ scores than late-onset FH negative patients, and IQ scores were correlated with ICV. CONCLUSIONS: These data provide evidence that parental alcohol use might increase risk for alcoholism in offspring in part by a genetic and/or environmental effect that might be related to reduced brain growth.  相似文献   
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