G. W. K. Ching scite author profile

The incidence of heart failure (HF) is increasing and it remains the only area in cardiovascular disease wherein hospitalization rates and mortalities have worsened in the past 25 years. This review is provided to assess the role of radionuclide imaging in HF. The focus is on three aspects: the value of nuclear imaging to distinguish ischemic from non-ischemic etiologies; risk stratification of patients with HF with evaluation of candidates for specific treatment strategies; and the role of cardiac neuronal imaging in patients with HF. Distinguishing ischemic from non-ischemic cardiomyopathy is important because patients with ischemic cardiomyopathy can potentially have dramatic improvement with revascularization. Single photon emission computed tomography (SPECT) has excellent reported sensitivity and negative predictive value in the detection of coronary artery disease in HF patients. SPECT imaging is also useful in establishing treatment strategies in patients with HF, including those with new onset CHF. Cardiac neuronal imaging of mIBG is particularly helpful in risk stratification of patients with HF. The modality can be used to monitor the response to therapy as dysfunctional mIBG uptake may show improvement with pharmacological treatment.

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Hypertension

Ching

Beevers

1991

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An oral treatment for lead toxicity

Ching

Rogers

Braithwaite

et al. 1991

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An oral treatment for lead toxicity Sir, We read with interest the paper by Thomas and Ashton' which described a patient with lead poisoning in whom comparison was made between the efficacy ofintravenous sodium calciumedetate and oral DMSA. The authors claim that 'an equal amount of the lead is excreted by the two drugs'. Although both chelating agents produced similar falls in the blood lead concentration, the limited data given in Figure I by the authors' suggest that the excretion of lead during treatment with sodium calciumedetate was approximately five times greater than with oral DMSA, notwithstanding the fact that both treatments were continued for a similar period.The efficacy of chelation therapy in lead poisoning cannot bejudged by estimating blood lead concentrations alone; determination of urine lead excretion is mandatory. A critical review of the two comparative clinical studies published in the English literature2'3 does not support the view that DMSA is superior to sodium calciumedetate in promoting urinary lead excretion. Even though only 12-16 mg/kg/day sodium calciumedetate was given to intoxicated smelter workers,2 lead excretion was significantly greater than after DMSA administration (18-42 mg/kg/day). In a paediatric study,3 sodium calciumedetate (29 mg/kg/day) also produced greater urinary lead excretion than DMSA (30 mg/kg/day). Our own data (to be published) demonstrate that intravenous sodium calciumedetate (75 mg/kg/day) is approximately four times more effective in promoting lead excretion than DMSA (30 mg/kg/day). Taking into consideration not only 'therapeutic' dose but molar equivalents, we conclude that oral DMSA is less effective than intravenous sodium calciumedetate in promoting urinary lead excretion. Urea and electrolytes, electrocardiogram and chest radiograph on admission were normal. The patient was given intravenous plasma protein substitute at a rate of 1 litre per hour over 8 hours. A bolus (10 mg) and infusion (0.04 mg/min) of naloxone was given over 1 hour with no effect on conscious level or hypotension. After 8 hours a systolic blood pressure of 90 mmHg was maintained with a concomitant improvement in conscious level.There are 6 reports of angiotension converting enzyme inhibitor overdose'-6 with variable severity of hypotension and altered conscious level. The duration and severity of the hypotension was unexpected in view of the pharmacokinetics of the drug. Supportive therapy has been advocated with intravenous fluid and, rarely, inotropic support and renal-vasodilator therapy. It is unlikely that in our patient a concomitant intravenous narcotic overdose may have contributed to the hypotension and the altered conscious level. There was no clinical improvement with intravenous naloxone. Naloxone pre-treatment has been used to block the hypotensive response associated with captopril treatment7 and we report that, in our patient, naloxone did not reverse captopril-induced hypotension.

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G. W. K. Ching

Clinical outcomes after neurogenic stress induced cardiomyopathy in aneurysmal sub-arachnoid hemorrhage: A prospective cohort study

Functional significance of coronary collateral vessels in patients with previous ‘Q’ wave infarction: relation to aneurysm, left ventricular end diastolic pressure and ejection fraction

The role of radionuclide imaging in heart failure

Hypertension

An oral treatment for lead toxicity

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