Mg In Cases Research Articles

Role of serum magnesium level as an indicator of glycemic control in type 2 diabetes mellitus

Background: Diabetes mellitus (DM) is caused by various etiological factors that lead to different metabolic dysregulations. Magnesium (Mg) is supposed to have some role in glycemic control in Type 2 diabetes and also with the disease progression. This study was taken up to estimate the level of serum Mg and correlate the same with glycated hemoglobin (HbA1c). Aim and Objective: The present study was conducted to estimate serum Mg level in type 2 DM patients and find out if there is any correlation with HbA1c. Materials and Methods: Blood samples from 50 patients of type 2 diabetes were taken and levels of different parameters – fasting blood sugar, postprandial blood sugar, HbA1c, and serum Mg were estimated and analyzed statistically. Results: The mean serum Mg in cases is 1.64 ± 0.15 mg/dl and mean serum Mg in controls is 1.9 ± 0.16 mg/dl. Mean HbA1c in cases is 7.49 ± 1.22% and mean HbA1c in controls is 4.64 ± 0.36%. There is a negative correlation between serum Mg levels and HbA1c. Conclusion: In this study, inverse correlation was found between serum Mg level and HbA1c. Further larger study will be needed to strengthen the results revealed.

Serious postoperative complications induced by medical glue: three case reports

BackgroundVarious types of medical glues/adhesives/topical coagulants’ (referred to as MG hereinafter) have widespread application as surgical adhesives, and have been shown to be safe and effective for a broad range of usage, such as in hemostasis, reinforcement of intestinal anastomoses or sites of potential fluid leakage, adhesion of two surfaces, wound closure, and vascular embolization. However, inappropriate application of MG may sometimes lead to serious complications. Herein, we describe three cases of serious postoperative complications induced by a possible inappropriate use of N-butyl-2-cyanoacrylate MG (NBCA MG).Case presentationThree patients presented with abdominal pain (chronic pain in cases 1 and 2, and acute pain in Case 3), hematochezia (Case 2), and intestinal obstruction (Case 3). All patients had a history of abdominal surgery and intraoperative use of NBCA MG. Abdominal computed tomography and gastroenterological endoscopy revealed foreign bodies (solidified MG in cases 1 and 2) and intestinal obstruction related to a mass of residual non-absorbed MG causing an internal hernia from a dense adhesion (Case 3). All patients underwent exploratory laparotomy, which revealed duodenal perforation, colonic erosion, and an internal hernia, all of which was related to MG use. We undertook removal of the foreign bodies (cases 1 and 2), surgical closure of the site of duodenal erosion (Case 1), partial colectomy (Case 2), and partial enterectomy (Case 3).ConclusionInappropriate application of MG may induce serious complications. We emphasize the importance of careful evaluation of the indications, dosage, and spraying thickness of MG in clinical practice. Serious complications caused by inappropriate application of MG should be reported to raise awareness in the surgical fraternity.

Retrospective Nested Case Control Study of the Impact of Immunosuppression on Post Transplant Malignancy among Adult Heart Transplant Patients

Purpose Post-transplant malignancy is diagnosed in approximately 18% of heart transplant (HTx) recipients and is a leading long-term cause of death among these patients. The association between exposure to rabbit anti-thymocyte globulin (rATG), a polyclonal depleting antibody used for its immunomodulatory activity, and incidence of malignancy in HTx is unclear. Methods This is a single-center, retrospective chart review of all HTx recipients who received rATG induction between October 1, 2008 and December 31, 2015. ICD-9 codes were used to identify HTx patients who were diagnosed with any malignancy post-transplant (cases). A nested, case-control study design was used to determine the relative risk of rATG exposure with the incidence of malignancy post-transplant. Cancer cases were matched to controls in a 1:2 method based on age, sex, Epstein Barr Virus donor/recipient status, and year of transplant. Secondary analyses amongst 1:2 matches examined the impact of maintenance immunosuppression exposure on cancer risk using a weighted equation composed of the drug dose, duration, and trough values when applicable. Results Of the 126 patients included in the study, 25 developed malignancy. These 25 patient cases were matched to 50 control patients. The primary endpoint was to evaluate the association of rATG on the risk of malignancy. The median cumulative rATG dose in milligrams (mg) between groups was 365mg in cases and 465mg in controls (OR 0.94, 95% CI 0.79 - 1.11, p=0.46). The cumulative dose of rATG in mg/kg was 4.7 mg/kg in cases vs. 5.7 mg/kg in controls (OR 0.96, 95% CI 0.82 - 1.12, p=0.59). By both univariate and multivariate analyses, there were no statistically significant differences in malignancyassociated with the usage of or quantified exposure to tacrolimus, sirolimus, cyclosporine, or mycophenolate mofetil, although sirolimus showed anti-oncotic trends. Conclusion The results of this study demonstrate current rATG dosing strategies may not singularly be associated with malignancy development as previous dosing strategies suggested. Additional investigations are needed to explore the multiple factors associated with post-transplant malignancy as well as the possible modulating effect of sirolimus.

Dietary isoflavone intake is associated with a reduced risk of myelodysplastic syndromes.

Isoflavones have been suggested to have protective effects on certain cancers. However, the association of soya foods or dietary isoflavones with the risk of myelodysplastic syndromes (MDS) has not been examined. Thus, the aim of this hospital-based case-control study undertaken in China in 2012-2013 was to investigate the association between dietary isoflavone intake and MDS risk. The analysis included 208 cases aged 19-85 years with MDS and 208 controls individually matched to the cases by sex, birth quinquennium and residential locality. Information on habitual food intakes, including nine items of soya foods, was sought from in-person interviews using a validated 107-item FFQ. Dietary intakes of daidzein, genistein, glycitein and total isoflavones were estimated using the 2008 US Department of Agriculture Isoflavone Database. OR were calculated from conditional logistic regression after adjustment for potential confounding by demographics, lifestyle and dietary factors. The mean daily intake of total isoflavones was 19·0 mg in cases and 23·0 mg in controls. Dietary intake of isoflavones was inversely associated with the risk of MDS. The adjusted OR in the highest tertile compared with the lowest tertile of intake were 0·43 (95 % CI 0·21, 0·85) for daidzein, 0·36 (95 % CI 0·18, 0·74) for genistein, 0·49 (95 % CI 0·25, 0·97) for glycitein and 0·40 (95 % CI 0·20, 0·81) for total isoflavones. The findings suggest that higher dietary intake of isoflavones is associated with a reduced risk of MDS in a Chinese population.

Dexamethasone Perioperative Coanalgesia in Lumbar Spine Fusion: A Controlled Cohort Study of Efficacy and Safety.

A 48-hour trial of dexamethasone coanalgesia became our standard practice in May 2008. This is our research Ethics Board-approved review of this experience to date with attention to perioperative narcotics use and pain scores for the first 48 hours after surgery as well as length of stay (LOS), wound healing complications, and infections in the first 6 months, compared with the historical precedent control cohort. Surgical case logs identified cases of 1- and 2-level elective lumbar decompression and fusion surgery performed since protocol initiation (cases) and for a like period beforehand (controls). Minimum of 6 months follow-up (sufficient to identify acute and subacute wound healing problems and perioperative infections) information was required. Hospital, Pain Service, and office records were reviewed for the extraction of outcomes data. We identified 132 cases and 146 controls. In 41 additional cases records were deficient. Baseline characteristics were equivalent. Cases included 70 males (53%) and 62 females (47%) of mean age 54 years (range, 18-84 y). Seventy-five (57%) cases were narcotics dependant (mean of 79.5 mg-morphine-equivalent daily). Controls included 78 males (53%) and 68 females (47%) of mean age 55 years (range, 27-85 y). Eighty-nine (61%) controls were narcotics dependant (mean 101.2 mg-morphine-equivalents daily). Mean morphine-equivalents narcotic consumption for 48 hours after surgery was 262.9 mg in cases and 280.7 mg in controls. VAS pain scores at 48 hours after surgery averaged 4.4 and 6.9 during rest and activity in the cases, and 3.7 and 6.3 during rest and activity in the controls. LOS averaged 3.9 days in cases and 5.2 days in controls. Delayed wound healing and surgical site infections were not observed in either group. Systemic dexamethasone after 1- and 2-level lumbar fusion surgery demonstrated minimal impact on 48 hours perioperative narcotics use with no detriment to pain control, wound healing, or infections. LOS was shortened by 25%.

Anticoagulant Managements of Left Ventricular Assist Device Implantation in Two Patients with Heparin-Induced Thrombocytopenia (HIT): Use of Argatroban as an Anticoagulant for Cardiopulmonary Bypass

Heparin-induced thrombocytopenia (HIT) can cause fatal arterial or venous thrombosis/thromboembolism. In high-risk cases, heparin should be immediately discontinued and an alternative administered; the only alternative permitted in Japan is argatroban, a direct thrombin inhibitor. Anticoagulation in patients with recent HIT requiring cardiopulmonary bypass (CPB) surgery is challenging, because it is sometimes difficult to find out appropriate dosage of argatroban using ACT based monitoring calculation. Two dilated cardiomyopathy patients with HIT were administered argatroban as the anticoagulant for the CPB in left ventricular assist device (LVAD) implantation. After discontinuing argatroban, blood coagulopathy persisted beyond its expected half-life, leading to abnormal haemostasis. Because of severe intraoperative and postoperative bleeding, both patients required massive transfusion support, despite the case 2 performed plasmapheresis to eliminate argatroban at the weaning from CPB. However, blood loss in case 2 (18,159 ml) was significantly lower than that in case 1 (31,292 ml), which might be contributed by the smaller dosage of argatroban (242 mg in case 2 vs. 489 mg in case 1) and plasmapheresis. Prolongation of ACT is multifactorial and affected by platelet count, fibrinogen concentration and, particularly total dose of argatroban. Furthermore, literatures and our experienses revealed that the recovery time to baseline ACT after stopping argatroban was significantly correlated with the total dose of argatroban (r=0.927). But, we could not authenticate the potency of plasmapheresis to eliminate argatroban and HIT antibodies. Because no specific antidotes are available for argatroban, surgical teams should carefully monitor timing of argatroban administration and the total dosage.

3,4-Diaminopyridine may improve neuromuscular block during botulism

In September 2011, two outbreaks of botulism toxemia (toxin A) incriminating the same artisanal product were responsible for nine cases of botulism in France. Among these cases, three women (Cases 1, 2, and 3) aged 27, 29, and 23 years, respectively, were hospitalized in our ICU for mechanical ventilation support. They rapidly received a trivalent botulism antitoxin serum. Two weeks later, Case 3 passed a spontaneous breathing trial but needed new ventilator support 24 hours after extubation. Association between respiratory failure and low compound muscle action potential (CMAP) amplitude measured at the forearm was reported in a study performed during a large outbreak in 2006 in Thailand [1]. CMAPs measured in the current Case 3 at the time of reintubation were <50% of theoretical values. Botulism could be considered a presynaptic myasthenia [2]. To reverse the effect of toxins, experimental models explored the effects of 3,4-diaminopyridine (3,4-DAP) [3]. In Europe, 3,4-DAP is used to treat symptoms of Lambert–Eaton myasthenic syndrome [4,5]. We conducted a pilot study to evaluate the electrophysiological effects of 3,4-DAP (Clinical Trials Registration: {type:clinical-trial,attrs:{text:NCT01441557,term_id:NCT01441557}}NCT01441557). The clinical trial protocol was accepted by the local ethics committee and the French Agency for the Safety of Health Products (agence francaise de securite sanitaire des produits de sante). Patients signed an informed consent. Experiments were conducted 21 days after the patients’ admissions. Electrophysiological measures were collected before and after the oral administration of a single dose of 3,4-DAP (20 mg for Cases 1 and 2, 10 mg for Case 3). The plasma concentration 90 minutes after administration was measured by liquid chromatography–tandem mass spectrometry. Cases 1 and 2 showed increase of CMAP amplitude after administration (Figure 1a) with a plasma concentration of 27 ng/ml and 18 ng/ml, respectively. The absence of effect in Case 3 was associated with lower serum concentration (5 ng/ml). These results suggest that the intensity of paralysis was different between the cases and was clinically associated with the quantity of poisoned food ingested (from a single toast to the leftovers on a knife). These different intensities of paralysis may explain the discrepant effects observed as higher plasma concentration was not associated with better CMAP improvement. Interestingly, Case 2 who answered the best to the treatment was weaned earlier from mechanical ventilation. Figure 1 Low compound muscle action potential amplitudes. Surface electromyograms were recorded bilaterally from right and left abductor pollicis brevis (ABP) and abductor digiti minimi (ADM) muscles following median and ulnar nerves supramaximal stimulation at ... In all cases, during the study period of 1 day, the CMAP amplitude concomitant to drug administration was higher than the later one, confirming the consistency of presynaptic block. Finally, weaning was successful at day 38, day 28, and day 35 in Cases 1, 2, and 3, respectively, following a prolonged spontaneous T-piece trial. Moreover, basic CMAPs at day 21 reflected the time to extubation (Figure 1b). In the perspective of bioterrorism, adjunctive treatment of botulism could be of a special interest in as much as stocks of antitoxin are limited. In this context, rapid onset of 3,4-DAP therapy may delay the evolution of paralysis to fatal respiratory failure. Although our results are encouraging, the observed effects of oral 3,4-DAP were modest and may be related to low blood concentration [5].

O3-005 - Phase 1 and 2 Trials of Combination Therapy with Gemcitabine and Candesartan in Advanced Pancreatic Cancer

ABSTRACT Background Inhibition of renin-angiotensin (RA) system is one of the attractive targets in the treatment of pancreatic cancer (PaC). Our retrospective analysis showed the association of inhibition of RA system with better prognosis in advanced PaC (Br J Cancer. 2010;103: 1644–8). Here we reported the results of phase 1 and 2 trials of gemcitabine and candesartan (GECA) therapy in advanced PaC. Patients In phase 1 trial in normotensive patients, candesartan was administered orally at escalating dose (4, 8, 16 and 32 mg) qd daily and gemcitabine was administered 1000 mg/m2 30 min i.v. day 1, 8, 15, repeated every 4 weeks. DLT was defined as grade 4 hematological toxic effects, Grade 2 hypotension, abnormal creatinine or potassium and grade 3 or 4 other non-hematological toxic effects. In phase 2 trial, candesartan was administered 16 mg in normotensive patients and 8 mg in patients with hypertension, followed by increase up to 16 mg in cases without adverse events. Eligible criteria were unresectable locally advanced or metastatic PaC without any prior treatment, ECOG PS 0-2, normal renal function and without hypotension. Results In phase 1 trial, 14 patients (locally advanced/metastatic 7/7, candesartan 4 mg: 3 patients, 8 mg: 3 patients, 16 mg: 6 patients, 32 mg: 2 patients) were enrolled between July 2009 and October 2010. One of six patients at 16 mg demonstrated DLT of grade 4 neutropenia and two of two patients at 32 mg demonstrated DLT of grade 2 hypotension. The response rate (RR) and the disease control rate (DCR) were 0% and 79%. Progression-free survival and overall survival were 7.6 and 22.9 months. In phase 2 trial, 35 patients (locally advanced/metastatic 9/26) were enrolled between May 2011 and December 2011. Major severe adverse events were neutropenia 24% and thrombocytopenia 18%. Grade 2 hypotension was seen in three patients. RR and DCR were 11% and 63%. Median PFS and OS were 4.3 and 7.7 months. Conclusion GECA in advanced PaC appeared safe and promising, though a phase 2 study failed to meet our primary objective of 5-month median PFS.

Postoperative Global Amnesia Reversed With Flumazenil

Global postoperative amnesia (profound anterograde and retrograde amnesia) is rare and usually attributed to transient global amnesia-a poorly understood condition with no broadly accepted mechanism. We report an incident of probable transient global amnesia in a patient after endoscopic retrograde cholangiopancreatogram under general anesthesia, which was successfully treated with flumazenil. On the basis of the results of flumazenil administration in this and a previous case report, we would recommend a trial dose of 0.2 mg for cases of global postoperative amnesia, repeated if the first dose seems effective.

Individualised strategy of warfarin treatment for deep vein thromboembolism – case reports

Individualised strategy of warfarin treatment for deep vein thromboembolism – case reports

Impact of Imatinib Dose Escalation in Chronic Myeloid Leukemia Patients in Chronic Phase with Sub-Optimal Response or Failure with Imatinib 400 Mg.

Abstract 3289Poster Board III-1Imatinib dose escalation has been used in sub-optimal response and therapeutic failure to imatinib in conventional doses. The aim of this study was to evaluate the efficacy of imatinib dose increase in CML patients in CP who did not achieve the best response to imatinib 400 mg QID. Patients and methods:All CML patients in CP treated in our institution with imatinib 400mg between March 2002 and December 2008 were evaluated. Imatinib was escalated to 600–800mg in cases with sub-optimal response or failure, according to Leukemia Net or IRIS Trial criteria. All survival curves were calculated from date of dose increase: overall survival (OS) until death or last follow-up, event free survival (EFS) until loss of complete hematological response (CHR) or major cytogenetic response (MCyR), progression to accelerated phase (AP) or blast crisis (BC) or death from any cause. Transformation free survival (TFS) was calculated from dose increase until progression to AP, BC or death. Results:137 patients in CP were treated with imatinib 400 mg. Dose was escalated in 55 (40%) patients due to loss or failure to achieve CRH (13 = 24%); progression to BC (2 = 3.5%); no CCR (11 = 20%); loss of RCC (5 = 9%); CCR without major molecular response (MMR) after 18 months of imatinib (24 = 43.5%). Males: 37, females 18 cases. Median age: 44 (16–74) years. Twenty-eight patients (49%) were treated with imatinib as first line therapy and 51% had used IFN previously. Median time between diagnosis and imatinib start was 4.5 (0–94) months. Responses: 94% achieved CHR; 58% CCR and 34% MMR. After dose increase, 31 (56%) responded: 58% of the patients with previous sub-optimal molecular response achieved MMR. Among those who benefited from dose increase, only 3 cases lost the response: one with hematological resistance and two with cytogenetic resistance (2 lost CCR and one CHR). Seven out of 16 patients who increased dose due to cytogenetic failure (loss of response, failure and sub-optimal response) achieved response: one had partial cytogenetic response (PCyR) and 6 CCR. Five patients with hematological failure presented response: CHR (2), CCR (1), PCyR (1) and MMR (1). Patients with BC (2 cases) did not respond to dose escalation. TFS was 89% and 67% in 2 and 5 years, respectively. EFS was 71% and 64% in 2 and 5 years respectively. When stratified by the type of failure, EFS was 100%, 49% and 34% in the group with molecular sub-optimal response with median time of 22 (4–41) months, cytogenetic 17 (1.2–42) and hematological failure 7.7 (0.2–57), respectively (P<0.03). Conclusions:imatinib dose escalation was successful in molecular sub-optimal response. However, the patients who do not achieve MMR might be candidates to second line treatment. Patients who did not achieve cytogenetic or hematological response did worse with imatinib dose escalation. Disclosures:No relevant conflicts of interest to declare.

PLEURODESIS WITH CARBOPLATIN IN ELDERLY PATIENTS WITH MALIGNANT PLEURAL EFFUSION AND LUNG ADENOCARCINOMA

PLEURODESIS WITH CARBOPLATIN IN ELDERLY PATIENTS WITH MALIGNANT PLEURAL EFFUSION AND LUNG ADENOCARCINOMA

原発性肺クリプトコックス症に対するfluconazoleによる治療の検討

We treated two cases of primary pulmonary cryptococcosis with fluconazole (FLCZ), the clinical usefulness of FLCZ was evaluated. FLCZ was administered orally in doses of 300 mg daily for about six months. Concentrations of FLCZ were measured in the serum of the two cases and in the bronchoalveolar lavage (BAL) fluid in one case. The following results were obtained: 1. Clinical cures were obtained in the two cases. 2. The serum levels of FLCZ was 15.1 microliters/ml, 13.6 micrograms/ml two hours after administration of 100 mg in case 1, that of levels were 11.1 micrograms/ml, 8.9 micrograms/ml one hour and 4.5 hours, respectively, after administration of 100 mg in case 2. BAL was performed 4.5 hours after administration of 100 mg in case 2, the BAL fluid level of FLCZ was 0.7 microgram/ml. 3. The minimal inhibitory concentration of FLCZ against one strain obtained from the cytology brush in case 1 was 4.0 micrograms/ml. 4. The cryptococcal antigen titer decreased with the improvement of clinical signs and the resolution of chest X-ray abnormalities within about six months, and there was no relapse. From these results, we consider that FLCZ is a useful antifungal agent for primary pulmonary cryptococcosis, and we therefore recommend a six month treatment.

A Case-Control Study of Caffeine and Methylxanthines in Benign Breast Disease

A dietary case-control study of 854 histologically diagnosed cases of benign breast disease (BBD), 755 matched surgical controls, and 723 matched neighborhood controls was conducted in Israel between 1977 and 1980. No association between coffee consumption and BBD was found. Analyses by histological type, degree of ductal atypia, age, sex, and ethnic origin, controlling for several confounding factors, confirmed the lack of association. The estimated mean intake of methylxanthines was also similar for cases and controls (302, 312, and 313 mg for cases, surgical controls, and neighborhood controls, respectively). No evidence of a dose-response was noted. Our results suggest that there is no association between coffee or methylxanthine consumption and BBD, although we had a 70% chance of finding a risk ratio of 1.5 with an error of 5%.

Oral Ketoconazole Therapy for Keratomycosis

Two patients, a 48-year-old woman and a 44-year-old man, with fungal keratitis were treated with orally administered ketoconazole, a new antifungal agent. In both cases healing and regression of the corneal ulcer began four or five days after initiation of ketoconazole treatment (300 mg/day). The clinical signs of corneal infection disappeared after eight (Case 1) and three (Case 2) weeks and visual acuities improved markedly (from counting fingers at 5 cm to 20/30 in Case 1 and from 20/30 to 20/16 in Case 2). The levels of serum glutamic oxaloacetic transaminase and serum glutamic pyruvic transaminase increased slightly during the course of treatment (total dosages: 13,000 mg in Case 1 and 4,700 mg in Case 2), but no other systemic or topical signs of toxicity or adverse reactions were noted in either case.

Dietary vitamin C and uterine cervical dysplasia.

A case-control study of women with cervical abnormalities identified through Pap smears, was conducted in the Bronx, New York, to explore the relationship between nutritional intake and cervical dysplasia. Nutrient intake was estimated from computer analysis of three-day food records and 24-hour recall for 169 study participants (87 cases, 82 controls), including a subset of 49 pairs matched for age, race and parity. Mean vitamin C intake per day from three-day food record for controls was 107 mg, compared to 80 mg for cases (p less than 0.01). Analysis of matched pairs showed similar results; 29% of cases compared to 3% of controls in matched subset had vitamin C intake less than 50% of the recommended daily allowance, yielding a ten-fold increase in risk of cervical dysplasia as estimated by odds ratio (p less than 0.05). Younger age, greater frequency of sexual intercourse and younger age at first intercourse were associated with higher risk of cervical dysplasia. Multiple logistic analyses indicated that low vitamin C intake is an independent contributor to risk of severe cervical dysplasia when age and sexual activity variables are controlled. Approximately 35% of US women in their reproductive years have daily vitamin C intake below 30 mg, and 68% have vitamin C intake below 88 mg. If other studies confirm these findings, it may be important to explore a possible protective role of supplementary vitamin C for women at high risk of cervical cancer.

TREATMENT AND FOLLOW-UP OF NEONATAL MEPIVACAINE INTOXICATION

6 Infants with mepivacaine intoxication secondary to accidental injection into the infant during paracervical and pudendal blocks were studied. All had depression at birth, tonic seizures with apnea in the first 6 hrs., and often unreactive dilated pupils. Two required respiratory support. Peak serum mepivacaine conc. were 9 to 25 μg/ml within the first 12 hrs. with a post-natal increase from cord and maternal conc. documented in 3 cases. CSF conc. was similar to simultaneous serum conc. Exchange transfusions in cases 3, 4, and 5 produced no significant changes in clinical status or serum conc., and the total removed by exchange was 3.5 mg in case 4 and 1.07 mg in case 5. Although gastric conc. on drainage reached 229 μg/ml in case 5 and 82 μg/ml in case 6, gastric lavage in case 6 recovered only 0.3 mg total. Urinary excretion under forced diuresis in cases 4, 5, and 6 produced 12.7 mg, 37.4 mg and 12.1 mg in the first 24 hrs. (80-96% of the total excreted in urine over 90 hrs). Thus, forced diuresis is the treatment of choice with gastric lavage and exchange transfusion used only when forced diuresis is contraindicated.All 5 survivors were followed, 4 for 2 to 4 yrs, and are neurologically and developmentally normal. Anticonvulsants were discontinued in all, 3 at discharge. Early recognition, seizure control, and prompt resuscitation with carefully monitored respiratory support were key. If severe perinatal hypoxia can be avoided the prognosis from intoxication per se is excellent.