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More on renal salt wasting without cerebral disease: response to saline infusion [Case Report]
Bitew, Solomon; Imbriano, Louis; Miyawaki, Nobuyuki; Fishbane, Steven; Maesaka, John K
BACKGROUND AND OBJECTIVES/OBJECTIVE:The existence and prevalence of cerebral salt wasting (CSW) or the preferred term, renal salt wasting (RSW), and its differentiation from syndrome of inappropriate antidiuretic hormone (SIADH) have been controversial. This controversy stems from overlapping clinical and laboratory findings and an inability to assess the volume status of these patients. The authors report another case of RSW without clinical cerebral disease and contrast it to SIADH. DESIGN, SETTING, PARTICIPANTS, & MEASUREMENTS/METHODS:Three patients with hyponatremia, hypouricemia, increased fractional excretion (FE) of urate, urine sodium >20 mmol/L, and concentrated urines were infused with isotonic saline after collection of baseline data. RESULTS:One patient with RSW had pneumonia without cerebral disease and showed increased plasma aldosterone and FEphosphate, and two patients with SIADH had increased blood volume, low plasma renin and aldosterone, and normal FEphosphate. The patient with RSW responded to isotonic saline by excretion of dilute urines, prompt correction of hyponatremia, and normal water loading test after volume repletion. Hypouricemia and increased FEurate persisted after correction of hyponatremia. Two patients with SIADH failed to dilute their urines and remained hyponatremic during 48 and 110 h of saline infusion. CONCLUSIONS:The authors demonstrate appropriate stimulation of ADH in RSW. Differences in plasma renin and aldosterone levels and FEphosphate can differentiate RSW from SIADH, as will persistent hypouricemia and increased FEurate after correction of hyponatremia in RSW. FEphosphate was the only contrasting variable at baseline. The authors suggest an approach to treat the hyponatremic patient meeting criteria for SIADH and RSW and changing CSW to the more appropriate term, RSW
PMID: 19201917
ISSN: 1555-905x
CID: 3464592
SLE and rapidly progressive glomerulonephritis [Case Report]
Masani, Naveed N; Imbriano, Louis J; D'Agati, Vivette D; Markowitz, Glen S
PMID: 15861363
ISSN: 1523-6838
CID: 3535332
High-dose intravenous gadolinium for renal computed tomographic angiography [Letter]
Rosioreanu, Alex; Hon, Man; Imbriano, Louis; Mueller, Richard; Katz, Douglas S
PMID: 15126665
ISSN: 1051-0443
CID: 3002032
Prolonged postpartum proteinuria after early preeclampsia [Case Report]
Durham, John H C; Desnick, Robert J; Imbriano, Louis; Wasserstein, Melissa; D'Agati, Vivette D; Markowitz, Glen S
PMID: 14712456
ISSN: 1523-6838
CID: 4591012
Treating interdialytic hyperkalemia with fludrocortisone [Editorial]
Imbriano, Louis J; Durham, John H; Maesaka, John K
Hyperkalemia is a frequent and dangerous problem in dialysis patients. Many factors contribute to potentially life-threatening potassium elevation and most remedies used to treat hyperkalemia are handicapped by the consequences of the separate pools of intra- and extracellular potassium. Besides the kidney, the colon has the ability to excrete potassium, which can help lower total body potassium. Several prior authors have addressed the colon's ability to up-regulate potassium secretion, including the effect of aldosterone on fecal potassium content. Potentially dangerous intradialytic maneuvers to lower potassium levels may be avoidable with the use of the mineralocorticoid agonist fludrocortisone.
PMID: 12535291
ISSN: 0894-0959
CID: 3464622