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Potential application of neogalactosylalbumin in positron emission tomography evaluation of liver function. | LitMetric

Potential application of neogalactosylalbumin in positron emission tomography evaluation of liver function.

World J Gastroenterol

Shun-Da Du, Shao-Hua Li, Bao Jin, Xin Lu, Xin-Ting Sang, Hua-Yu Yang, Shou-Xian Zhong, Yi-Lei Mao, Department of Liver Surgery, Peking Union Medical College Hospital, Chinese Academy of Medical Sciences and Peking Union Medical College, Beijing 100730, China.

Published: June 2017

AI Article Synopsis

  • The study aimed to evaluate neogalactosylalbumin (NGA) as a method to assess liver function using positron emission tomography technology in a mouse model.
  • Female Kunming mice were divided into fibrosis and normal control groups, with fibrosis induced by carbon tetrachloride injection; NGA was administered to assess its distribution and liver uptake.
  • Results indicated that NGA accumulated primarily in the liver and kidneys, and significant differences in its uptake between healthy and fibrotic livers were observed, suggesting NGA's potential as a liver function indicator.

Article Abstract

Aim: To investigate the evaluation of neogalactosylalbumin (NGA) for liver function assessment based on positron emission tomography technology.

Methods: Female Kunming mice were assigned randomly to two groups: fibrosis group and normal control group. A murine hepatic fibrosis model was generated by intraperitoneal injection of 10% carbon tetrachloride (CCl) at 0.4 mL every 48 h for 42 d. F-labeled NGA ([F]FNGA) was synthesized and administered at a dosage of 3.7 MBq/mouse to both fibrosis mice and normal control mice. Distribution of [F]FNGA amongst organs was examined, and dynamic scanning was performed. Parameters were set up to compare the uptake of tracers by fibrotic liver and healthy liver. Serologic tests for liver function were also performed.

Results: The liver function of the fibrosis model mice was significantly impaired by the use of CCl. In the fibrosis model mice, hepatic fibrosis was verified by naked eye assessment and pathological analysis. [F]FNGA was found to predominantly accumulate in liver and kidneys in both control group ( = 21) and fibrosis group ( = 23). The liver uptake ability (LUA), peak time (T), and uptake rate (LUR) of [F]FNGA between healthy liver ( = 8) and fibrosis liver ( = 10) were significantly different ( < 0.05, < 0.01, and < 0.05, respectively). LUA was significantly correlated with total serum protein level (TP) ( < 0.05). T was significantly correlated with both TP and glucose (Glu) concentration ( < 0.05 both), and LUR was significantly correlated with both total bile acid and Glu concentration ( < 0.01 and < 0.05, respectively).

Conclusion: [F]FNGA mainly accumulated in liver and remained for sufficient time. Functionally-impaired liver showed a significant different uptake pattern of [F]FNGA compared to the controls.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5483502PMC
http://dx.doi.org/10.3748/wjg.v23.i23.4278DOI Listing

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