TY - JOUR
T1 - Evaluation of endogenous nitric oxide synthesis in congenital urea cycle enzyme defects
AU - Nagasaka, Hironori
AU - Tsukahara, Hirokazu
AU - Yorifuji, Tohru
AU - Miida, Takashi
AU - Murayama, Kei
AU - Tsuruoka, Tomoko
AU - Takatani, Tomozumi
AU - Kanazawa, Masaki
AU - Kobayashi, Kunihiko
AU - Okano, Yoshiyuki
AU - Takayanagi, Masaki
N1 - Funding Information:
This work was supported by a research grant from the Japanese Ministry of Education, Culture, Sports, Science, and Technology.
PY - 2009/3
Y1 - 2009/3
N2 - Nitric oxide (NO) is synthesized from arginine and O2 by nitric oxide synthase (NOS). Citrulline, which is formed as a by-product of the NOS reaction, can be recycled to arginine by the 2 enzymes acting in the urea cycle: argininosuccinate synthetase (ASS) and argininosuccinate lyase (ASL). Although the complete urea cycle is expressed only in the liver, ASS and ASL are expressed in other organs including the kidney and vascular endothelium. To examine possible alterations of the NO pathway in urea cycle defects, we measured plasma concentrations of arginine and citrulline and serum concentrations of nitrite/nitrate (NOx-, stable NO metabolites) and asymmetric dimethylarginine (ADMA, an endogenous NOS inhibitor) in patients with congenital urea cycle disorders of 3 types: ornithine transcarbamylase (OTC) deficiency, ASS deficiency, and ASL deficiency. All were receiving oral arginine replacement at the time of this study. The same parameters were also measured in healthy subjects, who participated as controls. The OTC-deficient patients had significantly high NOx- and nonsignificantly high ADMA concentrations. Their NOx- was significantly positively correlated with arginine. The ASS-deficient patients had significantly low NOx- and significantly high ADMA concentrations. The ASL-deficient patients had normal NOx- and nonsignificantly high ADMA concentrations. In ASS-deficient and ASL-deficient patients, the NOx- was significantly inversely correlated with citrulline. These results suggest that NO synthesis is enhanced in OTC-deficient patients while receiving arginine but that NO synthesis remains low in ASS-deficient patients despite receiving arginine. They also suggest that endogenous NO synthesis is negatively affected by citrulline and ADMA in ASS-deficient and ASL-deficient patients. Although the molecular mechanisms remain poorly understood, we infer that the NO pathway might play a role in the pathophysiology related to congenital urea cycle disorders.
AB - Nitric oxide (NO) is synthesized from arginine and O2 by nitric oxide synthase (NOS). Citrulline, which is formed as a by-product of the NOS reaction, can be recycled to arginine by the 2 enzymes acting in the urea cycle: argininosuccinate synthetase (ASS) and argininosuccinate lyase (ASL). Although the complete urea cycle is expressed only in the liver, ASS and ASL are expressed in other organs including the kidney and vascular endothelium. To examine possible alterations of the NO pathway in urea cycle defects, we measured plasma concentrations of arginine and citrulline and serum concentrations of nitrite/nitrate (NOx-, stable NO metabolites) and asymmetric dimethylarginine (ADMA, an endogenous NOS inhibitor) in patients with congenital urea cycle disorders of 3 types: ornithine transcarbamylase (OTC) deficiency, ASS deficiency, and ASL deficiency. All were receiving oral arginine replacement at the time of this study. The same parameters were also measured in healthy subjects, who participated as controls. The OTC-deficient patients had significantly high NOx- and nonsignificantly high ADMA concentrations. Their NOx- was significantly positively correlated with arginine. The ASS-deficient patients had significantly low NOx- and significantly high ADMA concentrations. The ASL-deficient patients had normal NOx- and nonsignificantly high ADMA concentrations. In ASS-deficient and ASL-deficient patients, the NOx- was significantly inversely correlated with citrulline. These results suggest that NO synthesis is enhanced in OTC-deficient patients while receiving arginine but that NO synthesis remains low in ASS-deficient patients despite receiving arginine. They also suggest that endogenous NO synthesis is negatively affected by citrulline and ADMA in ASS-deficient and ASL-deficient patients. Although the molecular mechanisms remain poorly understood, we infer that the NO pathway might play a role in the pathophysiology related to congenital urea cycle disorders.
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U2 - 10.1016/j.metabol.2008.09.025
DO - 10.1016/j.metabol.2008.09.025
M3 - Article
C2 - 19217439
AN - SCOPUS:59649120881
SN - 0026-0495
VL - 58
SP - 278
EP - 282
JO - Metabolism: Clinical and Experimental
JF - Metabolism: Clinical and Experimental
IS - 3
ER -
