The administration of a vasoconstrictor in combination
with a local anesthetic has evolved as a method for decreasing systemic toxicity, increasing the duration of anesthesia, and providing hemostasis during surgery. The importance of a vasoconstrictor agent is undis- puted. Lidocaine with epinephrine has been the most commonly used throughout the world. However, epinephrine-containing anesthetics may cause unwanted side effects in patients with cardiovascular disease after systemic absorption. 1-3 To avoid any such adverse cardiovascular effects, especially in high-risk patients, some authors have recommended the use of epinephrine-free anesthetics. 4 However, many investi- gators have reported that plain lidocaine provided unsatisfactory levels of anesthesia or hemostasis, or both. 5,6 Inadequate anesthesia results in stressful pain Cardiovascular response to epinephrine-containing local anesthesia in patients with cardiovascular disease Hitoshi Niwa, DDS, PhD, a Mitsutaka Sugimura, DDS, PhD, b Yuu Satoh, DDS, c and Ai Tanimoto, DDS, d Osaka, Japan OSAKA UNIVERSITY Objective. The purpose of the present study was to examine the safety of epinephrine-containing local anesthesia for use on patients with cardiovascular disease. Study design. Twenty-seven patients with cardiovascular disease were studied. The cardiac functional capacity of 9 patients was New York Heart Association class I; 11, class II; and 7, class III. Hemodynamic responses to intraoral injection of 1.8 mL of 2% lidocaine with 1:80,000 epinephrine were measured with impedance cardiography. Results. Systolic blood pressure and heart rate increased by 4.1% and 5.1%, respectively, immediately after the lidocaine- epinephrine injection. Consequently, rate pressure product increased by 10.0%. Cardiac index increased by 14.2%, and total peripheral resistance decreased by approximately 10%. No patient complained of cardiac symptoms. There were no significant differences in hemodynamic responses related to the extent of the cardiac functional capacity. Conclusion. We concluded that lidocaine-epinephrine was safe and had few, if any, hemodynamic consequences in patients with cardiovascular disease. (Oral Surg Oral Med Oral Pathol Oral Radiol Endod 2001;92:610-6) a Professor, Department of Dental Anesthesiology. b Associate Professor, Department of Dental Anesthesiology. c Assistant Professor, Department of Dental Anesthesiology. d Clinical Instructor, Department of Dental Anesthesiology. Received for publication Apr 16, 2001; returned for revision May 16, 2001; accepted for publication Jul 11, 2001. Copyright 2001 by Mosby, Inc. 1079-2104/2001/$35.00 + 0 7/13/118903 doi:10.1067/moe.2001.118903 for the patient, whose body releases greater amounts of endogenous catecholamine. It should be kept in mind that epinephrine is released endogenously in greater amounts than that used in dental anesthesia. 7-10 Therefore, a local anesthetic with epinephrine may be selected to obtain adequate levels of anesthesia and hemostasiseven in patients with cardiovascular disease. There have been many studies of the hemodynamic effects of dental anesthesia with epinephrine-containing local anesthetic solutions in young, healthy patients. 11-15 Tolas et al 13 reported no significant cardiovascular changes after injection of a single cartridge of an anes- thetic containing 18 g epinephrine, despite a 2-fold increase in plasma epinephrine. Knoll-Kohler et al 14 and Chernow et al 15 also demonstrated only a small reduction in mean arterial blood pressure and a slight increase in heart rate after the injection of low-dose epinephrine. Consequently, many investigators had believed that the cardiac effects of epinephrine- containing local anesthetics were small. 13,15 However, Dionne et al 16 has shown marked increases in cardiac output, stroke volume (SV), and heart rate measured by impedance cardiography after lidocaine with epineph- rine anesthesia in patients; they found no observable ORAL MEDICINE Editor: Martin S. Greenberg ORAL SURGERY ORAL MEDICINE ORAL PATHOLOGY Vol. 92 No. 6 December 2001 ORAL SURGERY ORAL MEDICINE ORAL PATHOLOGY Niwa et al 611 Volume 92, Number 6 effects on blood pressure. These results show that commonly used measurements such as heart rate and blood pressure underestimate the hemodynamic effects of epinephrine. Therefore, more sensitive tests are neces- sary. In addition, most previous studies have been on young, healthy subjects without a history of cardiovas- cular disease, so the question remains with respect to how a group of patients with cardiovascular disease would respond when epinephrine was included in the anesthetic. Thus, the purpose of the present study was to inves- tigate the hemodynamic changes produced by infiltra- tion anesthesia with 1.8 mL of 2% lidocaine with 1:80,000 epinephrine in patients with cardiovascular disease. To examine the hemodynamic effects of local anesthesia on such patients, the SV, cardiac index, and total peripheral resistance were measured by imped- ance cardiography. In addition, we also explored the hemodynamic response to low doses of epinephrine in patients receiving -blocking agents. METHOD Characteristics of the patient population The subjects were 27 patients (16 men and 11 women) hospitalized in the National Cardiovascular Center Table I. Clinical characteristics of the studied patients Cardiovascular Cardiac function/ Sex, age (y) disease fractional shortening (%) Medication NYHA I M, 72 HCVD 33 Nifedipine M, 54 OMI, HCVD 31 Amlodipine, enalapril M, 47 ARVD 39 (LVEF = 49%) Mexiletine, propranolol F, 57 HCVD Unknown Nilvadipine M, 75 OMI 17 Nicorandil, isosorbide, cilazapril, digoxin, furosemide F, 66 OMI 41 (LVEF = 65%) Amlodipine, metoprolol, doxazosin, spirono- lactone F, 53 HCVD 34 Amlodipine F, 29 HCM (LVEF = 60%) Verapamil, metoprolol, furosemide F, 68 AP, OMI, HCVD 35 Nicorandil, diltiazem NYHA II M, 76 OMI, unstable AP 24 Isosorbide, spironolactone, furosemide F, 68 AVR, MVR, CHF 46 Nifedipine, digoxin, isosorbide F, 58 MSR, AVR, WPW 15 Cibenzoline, spironolactone, furosemide M, 32 DCM 31 Amiodarone, mexiletine, metoprolol M, 49 Myocarditis 17 Amlodipine, enalapril, carvedilol M, 56 AP 43 (LVEF = 61%) Isosorbide, nitroglycerin, nicorandil, meto- prolol M, 61 MVR, PH 32 Nitroglycerin, digoxin, spironolactone, furosemide M, 48 OMI 24 (LVEF = 37%) Digoxin, amiodarone, isosorbide, propranolol, mexiletine, spironolactone, furosemide F, 40 ASD 13 (LVEF = 39%) Digoxin, spironolactone, furosemide M, 48 Ebsteins anomaly 46 (LVEF = 66%) Bepridil, nisoldipine, atenolol, digoxin F, 63 HCVD 11 (LVEF = 34%) Enalapril, digoxin NYHA III F, 50 Primary PH (LVEF = 56%), (RVEF = 26%) Dobutamine, alprostadil alfadex (PGE1), spironolactone M, 30 TOF, PA, AR 20 (LVEF = 35%) Docarpamine, mexiletine, spironolactone M, 28 DCM 15 (LVEF = 12%) Digoxin, metoprolol, alacepril, isosorbide, pimobendan, spironolactone, furosemide M, 67 OMI, unstable AP 23 Nifedipine, isosorbide, metoprolol, diltiazem M, 70 DCM 12 (LVEF = 28%) Digoxin, enalapril, metoprolol, spironolactone, furosemide F, 46 ASD, PH, Eisenmengers syndrome (LVEF = 52%), (RVEF = 30%) Digoxin, furosemide M, 20 DCM 15 Metoprolol, verapamil, captopril, spironolac- tone, furosemide HCVD, Hypertensive cardiovascular disease; OMI, old myocardial infarction; ARVD, arrhythmogenic right ventricular dysplasia; LVEF, left ventricular ejection frac- tion; HCM, hypertrophic cardiomyopathy; AP, angina pectoris; AVR, aortic valve replacement; MVR, mitral valve replacement; CHF, congestive heart failure; MSR, mitral stenosis and regurgitation; WPW, Wolff-Parkinson-White syndrome; DCM, dilated cardiomyopathy; PH, pulmonary hypertension; ASD, atrial septal defect; RVEF, right ventricular ejection fraction; TOF, tetralogy of Fallot; PA, pulmonary atresia; AR, aortic regurgitation. 612 Niwa et al ORAL SURGERY ORAL MEDICINE ORAL PATHOLOGY December 2001 (Suita, Japan) for treatment of heart disease. All patients required dental treatment, which was performed with them under local anesthesia. Each patient received a full explanation of the necessity and risk of the treatment and gave written informed consent before the study. Descriptive data for these 27 patients are listed in Table I. They were suffering from various cardiovascular disor- ders including ischemic heart disease, cardiomyopathy, and valve disease. Patients with serious arrhythmia, idio- pathic hypertrophic subaortic stenosis, and/or pace- makers were excluded. The patients continued to receive their prescribed cardiac drugs including calcium channel antagonists, -blocking agents, and nitrates. Nine patients were taking 1 selective -blocking agents, and 3 were taking nonselective ones. Pretreatment cardiac evaluation Detailed cardiac evaluations are listed in Table I. Cardiac functional capacity was assessed by cardiolo- gists according to the criteria of the New York Heart Association (NYHA 17 ; Table II). The functional capacity of 9 patients was class I; 11, class II; and 7, class III. Left ventricular function was evaluated with echocardiography, left ventriculography, and/or radioiso- tope angiography before the dental treatment. Study protocol Arterial blood pressure (systolic blood pressure; diastolic blood pressure; mean arterial pressure [MAP]) and heart rate (HR) were monitored by using an automatic noninvasive pressure device (Life Scope 7; Nihon Kohden Co Ltd, Tokyo, Japan). To evaluate the left ventricular function during and after infiltration anesthesia, noninvasive impedance cardiograms (CIC- 1000; Sorba Medical Systems, Inc, Brookfield, Wis) were recorded throughout the study. SV was measured every 20 seconds by using a computer-interfaced impedance device. Cardiac index (CI), total peripheral resistance (TPR), and rate pressure product were calcu- lated by the CIC-1000. The patients first rested in the supine position for 30 minutes, after which baseline measurements were obtained. The local anesthetic solution used consisted of 1.8 mL (1 cartridge) of 2% lidocaine with 1:80,000 epinephrine (L-E; Astra Zeneca, Osaka, Japan). In total, 22.5 g of epinephrine and 36 mg of lidocaine were used. The L-E was administered into the operative site over a period of 60 seconds. In all patients, the aspiration technique was used to prevent injection of the anesthetic into the vasculature and care was taken to inject as painlessly as possible. Each hemo- dynamic parameter was measured at 0, 2, 5, and 10 minutes after the intraoral injection of L-E. Patients rested for this period, then dental treatment was started. Statistical analysis Data were expressed as the percentages of hemody- namic changes from the baseline value. The results were statistically analyzed by using repeated measures 1-way analysis of variance, and the Bonferroni correc- tion was performed for multiple comparisons. A P value of <.05 was considered statistically significant. RESULTS The data from all 3 NYHA groups were initially analyzed together. Table III shows the hemodynamic response to L-E injection in all 27 patients. There was a 4.1% increase in systolic blood pressure and a 5.1% increase in HR immediately after the injection, although diastolic blood pressure and MAP remained unchanged. SV and CI increased significantly from 0 to 10 minutes after the injection; the greatest increases in SV and in CI, 13.4% and 14.2%, respectively, were recorded 2 minutes after the injection. A significant decrease in TPR occurred from 0 to 10 minutes; the maximal decrease of TPR was approximately 10% at 2 and 5 minutes. Rate pressure product increased by 10.0% to its maximum at 0 minutes. During the study, no patient complained of any cardiac symptom such as chest pain, palpitation, or dyspnea. There were no aggravated arrhythmias or abnormal changes in elec- trocardiograms in any of the patients. Table III shows the hemodynamic responses to L-E compared with the functional classifications of NYHA. There were no significant differences in blood pressure Table II. New York Heart Association Functional Classification 17 Class I Patients with cardiac disease but without resulting limitations of physical activity. Ordinary physical activity does not cause undue fatigue, palpitations, dyspnea, or anginal pain. Class II Patients with cardiac disease resulting in slight limitations of physical activity. They are comfortable at rest. Ordinary physical activity results in fatigue, palpitations, dyspnea, or anginal pain. Class III Patients with cardiac disease resulting in marked limitation of physical activity. They are comfortable at rest. Less than ordinary physical activity causes fatigue, palpitation, dyspnea, or anginal pain. Class IV Patients with cardiac disease resulting in inability to carry on any physical activity without discomfort. Symptoms of cardiac insufficiency or of the anginal syndrome may be present even at rest. If any physical activity is undertaken, discomfort is increased. ORAL SURGERY ORAL MEDICINE ORAL PATHOLOGY Niwa et al 613 Volume 92, Number 6 response among functional classes I, II, and III at any time. Although the greatest increase in HR was recorded immediately after the injection in each class, there were no significant differences among the 3 groups. Significant changes in SV, CI, and TPR were seen only in class I and class II patients. However, there were no significant differences among the 3 groups. The interaction between L-E and -blocking agents is depicted in Fig 1. MAP increased by 13.2% in the patients receiving nonselective -blocking agents. Consequently, there were significant differences in the MAP responses among the 3 groups. The increase in HR was observed only in patients without -blocker therapy. Although the SV and CI responses seemed to be smaller in the patients receiving nonselective - blocking agents than in patients in the other groups, there were no significant differences among the 3 groups. On the other hand, there were significant differences in the TPR response among the 3 groups. DISCUSSION The use of epinephrine in local anesthetics for patients with cardiovascular disease has been contro- versial. There have been many guidelines for the rational use of vasoconstrictors in patients with cardio- vascular disease. In 1964, a Working Conference of the American Dental Association and the American Heart Association 18 stated that the concentrations of vaso- constrictors normally used in dental local anesthetic solutions were not contraindicated in patients with cardiovascular disease when administered carefully and with preliminary aspiration. However, they did not suggest maximal recommended doses of vasoconstric- tors for cardiac patients, and this lapse proved to be dangerous. 19 Malamed 7 recommended a much smaller maximal dose of vasoconstrictor (no more than 40 g of epinephrine at one appointment) for patients with severe cardiovascular disease. Little et al 20 recommend that one, and probably two, cartridges of 2% lidocaine Table III. Cardiovascular response to L-E injection NYHA-FC 0 min 2 min 5 min 10 min SBP (%) I- III +4.1 9.9 * +2.5 6.1 * +0.9 6.1 1.2 5.0 I +4.9 12.6 +2.3 9.0 0.5 6.0 2.6 3.5 II +3.3 8.7 +2.9 5.4 +3.1 7.3 +0.6 6.2 III +3.8 9.3 +2.3 2.3 0.5 3.6 1.9 4.0 DBP (%) I-III +2.0 9.2 0.2 10.0 0.3 10.7 2.2 13.6 I +4.9 13.1 2.2 10.7 0.5 16.2 0.6 20.4 II 0.7 6.9 +1.0 11.0 2.3 6.7 3.4 8.9 III +2.3 5.5 +0.3 8.4 +1.7 7.5 2.2 13.6 MAP (%) I-III +2.9 7.6 +1.0 7.1 0.1 6.2 1.9 7.5 I +4.6 10.1 0.0 9.3 1.1 7.2 1.9 10.1 II +1.3 6.7 +1.6 7.0 +0.1 6.5 1.8 6.4 III +3.2 5.6 +1.5 4.5 +0.8 5.0 1.9 6.4 HR (%) I-III +5.1 8.2 * +1.6 11.4 +0.8 5.9 +1.8 4.3 I +6.0 10.0 * +1.1 19.7 1.2 8.5 +1.5 4.6 II +5.5 8.1 * +1.8 4.6 +2.1 4.1 +3.1 4.8 III +3.1 6.5 +1.8 3.2 +1.6 3.8 0.1 2.5 SV (%) I-III +6.9 17.1 * +13.4 17.3 * +11.2 11.6 * +5.3 11.2 * I +4.2 11.7 +14.8 10.8 * +11.9 7.2 * +9.8 10.7 * II +10.5 24.5 +16.5 24.0 * +13.7 14.6 * +1.4 11.3 III +4.7 6.8 +6.9 10.6 +6.6 11.2 +5.6 11.0 CI (%) I-III +12.1 16.9 * +14.2 18.2 * +12.4 13.2 * +7.6 10.5 * I +10.7 12.5 * +11.6 14.2 * +10.4 6.0 * +12.3 11.6 * II +15.7 22.6 * +19.5 23.2 * +16.2 16.2 * +4.8 7.0 * III +8.3 11.8 +9.4 13.3 +9.1 15.1 +6.1 13.0 TPR (%) I-III 6.6 13.6 * 9.8 14.5 * 9.9 12.3 * 8.1 10.9 * I 5.3 17.5 9.6 14.9 10.6 5.7* 12.7 7.3* II 9.1 12.2* 12.0 15.9* 11.6 15.2* 5.2 11.6 III 4.3 11.3 6.5 13.1 6.4 14.4 6.7 13.0 RPP (%) I-III +10.0 13.3 * +3.1 8.2 +2.2 9.2 +1.0 6.8 I +12.1 14.3 * +0.1 11.8 1.0 10.0 0.1 5.5 II +9.8 13.6 +4.7 6.5 +5.3 10.6 +3.7 8.7 III +7.5 13.2 +4.4 3.5 +1.4 3.1 1.8 3.1 Values are expressed as percentage of hemodynamic change from baseline value (mean SD). NYHA-FC, New York Heart Association functional capacity; SBP, systolic blood pressure; DBP, diastolic blood pressure; MAP, mean arterial pressure; HR, heart rate; SV, stroke volume; CI, cardiac index; TPR, total peripheral resistance; RPP, rate pressure product. *P <.05, versus baseline value. 614 Niwa et al ORAL SURGERY ORAL MEDICINE ORAL PATHOLOGY December 2001 with 1:100,000 epinephrine (18 to 36 g of epineph- rine) were of little clinical significance to most patients with hypertension or other cardiovascular diseases. Kaneko 21 recommended that the total dose of epineph- rine should be limited to less than 40 g in moderate cases or 20 g in serious cases, with epinephrine concentrations of 1:100,000 or less. Current clinical practice has tacitly accepted the safety of epinephrine use in patients with cardiovascular disease. However, there have been some criticisms of these guidelines. First, previous investigators have not provided explicit criteria for the categorization of a patient with severe cardiovascular disease. Second, the recommendations were made on the basis of the results from healthy, young volunteers, and these results should not be extrapolated to patients with cardiovas- cular disease. Hemodynamic changes due to epineph- rine in local anesthetic may be well tolerated in healthy, young subjects; however, it is not clear whether patients with preexisting cardiovascular disease would tolerate them as well. Third, most recommendations have been made on the basis of the changes in HR and blood pressure produced by epinephrine. However, it has become evident that the information obtained by conventional monitoring of such variables as blood pressure and HR are inadequate for explaining the pathophysiologic changes that may occur in the patient. 14,16 Therefore, these recommenda- tions need to be validated with more sensitive methods for further examination of patients with cardiovascular disease. There have been several reports of the hemodynamic effects of epinephrine in patients with cardiovascular disease. Cintron et al 22 reported that dental anesthesia with 1.0 mL of 2% lidocaine with 1:100,000 epineph- rine caused no significant changes in HR or blood pres- sure and was well tolerated by patients with recent myocardial infarction. Middlehurst and Coulthard 23 reported that approximately 5 mL of 2% lidocaine with 1:50,000 epinephrine and 0.25 IU/mL of vasopressin did not cause ischemic changes in patients with heart disease. Davenport et al 6 studied the hemodynamic effects of moderate doses of epinephrine during peri- odontal surgery in patients with stable cardiovascular disease and found no significant changes in HR or blood pressure, despite the elevation of the plasma epinephrine concentration. In contrast, Leviner et al 4 reported that local anesthesia without vasoconstrictor should be preferred for use in severely compromised patients. However, detailed cardiac functions were not measured in any of these previous studies. In the present study, hemodynamic responses to 22.5 g of epinephrine were studied with impedance cardi- ography. This method is noninvasive and places no stress on the patients. Its reliability has been estab- lished in previous studies. 24 The effects of epinephrine may depend on the specifics of the underlying cardiovascular disease. Fig 1. Cardiovascular response to L-E injection in patients receiving -blocking agents. (), patients without - blocker therapy (n = 15); -1 selective, patients taking -1 selective -blocking agents (n = 9); nonselective, patients taking nonselective -blocking agents (n = 3). Mean SD; * P < .05 versus baseline value; # P < .05 () versus nonselective;
P < .05; -1, selective versus non-
selective. Thus, it was impossible to evaluate the effects of epinephrine in patients with each type of disease. Therefore, we divided the patients into 3 groups according to their cardiac functional capacities (NYHA class I to III) and assessed the hemodynamic effects in each group. The criteria of NYHA are simple and widely used. When the results of the 3 groups were combined, MAP remained unchanged by L-E injection, SV and CI increased by 13%, and TPR decreased by 10%. These results suggest that the increased cardiac output and decreased peripheral resistance compensate for each other to maintain blood pressure within control values. The transient increases in HR and systolic blood pres- sure immediately after the injection were likely an expression of endogenous catecholamine release as a result of emotional stress or pain and not a pharmaco- logic effect, because it has been shown that the peak concentration of exogenous epinephrine occurs 3 to 5 minutes after an injection. 25 The hemodynamic responses in this study were greater than those in our previous study. 26 Differences in the emotional conditions and the ages of subjects may have influenced the results. Subjects were real dental patients (mean age, 53 years) scheduled for treatment in the present study, whereas the healthy young volunteers (mean age, 31 years) underwent only dental injection in our previous study. However, further study is necessary to explain this difference, because there remains a controversy over changing -adren- ergic responsiveness with aging. 27-29 It is necessary to evaluate whether the hemodynamic effects of L-E are deleterious to the compromised heart. During the study, no patient complained of cardiac symptoms such as chest pain, palpitation, or dyspnea. Even the class III patients tolerated the hemo- dynamic changes produced by L-E without any symp- toms. Therefore, we speculate that the peak increases in cardiac function produced by L-E are limited and within normal physiologic variation. This study failed to disclose any significant differ- ences in hemodynamic responses among the patients in classes I, II, and III. However, increases in SV and CI were observed only in class I and class II patients; changes in SV and CI were not significant in class III patients. Likewise, TPR decreased significantly only in class I and class II patients. These results suggest that the effects of epinephrine are attenuated in class III patients with severely failing hearts. Recent studies have demonstrated that the sympa- thetic nervous system is unduly activated in patients with congestive heart failure. 30-32 This augmented activity is part of a vital compensatory mechanism that supports cardiac function. The high plasma concentra- tions of norepinephrine observed in these patients exert positive inotropic effects from stimulation of myocar- dial -adrenergic receptors. However, if heart failure lasts for a long time, this elevated norepinephrine induces the down-regulation of -adrenergic receptors and contributes to desensitization. 33 Such alteration of -adrenergic receptors may provide an explanation for the attenuation of the effects of epinephrine observed in class III patients. In contrast to our results, Hirota et al 34 reported that greater hemodynamic changes were observed in class III patients than in patients in other groups. However, their subjects were so few (n = 2) that their findings were unreliable. When excessive concentration or dose of epinephrine is administered in patients with a normal heart, SV and cardiac output are further elevated because of the 1 effect of epinephrine, leading to a prominent rise in blood pressure. 35 Consequently, rate pressure product, indexes of myocardial oxygen consumption, and left ventricular stroke work (the product of MAP and SV), representing the level of work by the left ventricle, also increase. Although a normal heart can apparently with- stand these great demands, in failing or ischemic heart, cardiac functions may be impaired by these changes. 36 The possibility of adverse interactions between epinephrine and nonselective -blocking agents has been suggested. 37,38 Epinephrine production may lead to an exaggerated increase in blood pressure in patients taking a nonspecific -blocking agent such as propran- olol. As shown in Fig 1, the response to the low dose of epinephrine in patients taking nonselective -blocking agents differed from that in patients not taking such medication. Little 39 suggested, on the basis of clinical experience, that 1:100,000 epinephrine (no more than 0.036 mg of epinephrine) in a local anesthetic could safely be used for patients receiving nonselective - blocking agents. However, the possibility of a hyper- tensive interaction occurring with epinephrine should be considered when epinephrine is used in patients taking a nonspecific -blocking agent. This study provides documentation that 1.8 mL of L-E is safe and has few, if any, hemodynamic conse- quences in patients with cardiovascular disease. We concluded that a low dose of epinephrine (22.5 g) in local dental anesthesia was well tolerated by cardiovas- cular patients who were in NYHA classes I through III. REFERENCES 1. Hasse AL, Heng MK, Garrett NR. Blood pressure and electro- cardiographic response to dental treatment with use of local anesthesia. J Am Dent Assoc 1986;113:639-42. 2. Massalha R, Valdman S, Farkash P, Merkin L, Herishanu Y. Fatal intracerebral hemorrhage during dental treatment. Isr J Med Sci 1996;32:774-6. ORAL SURGERY ORAL MEDICINE ORAL PATHOLOGY Niwa et al 615 Volume 92, Number 6 616 Niwa et al ORAL SURGERY ORAL MEDICINE ORAL PATHOLOGY December 2001 3. Murakawa T, Koh H, Tsubo T, Ishihara H, Matsuki A. Two cases of circulatory failure after local infiltration of epinephrine during tonsillectomy. Masui 1998;47:955-62. 4. 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Reprint requests: Hitoshi Niwa, DDS, PhD Department of Dental Anesthesiology Osaka University Faculty of Dentistry 1-8 Yamadaoka, Suita Osaka 565-0871 Japan niwa@dent.osaka-u.ac.jp