Validation of noninvasive morphological and diffusion imaging in mouse emphysema by micro-computed tomography and hyperpolarized (129)Xe magnetic resonance imaging

Validation of noninvasive morphological and diffusion imaging in mouse emphysema by micro-computed tomography and hyperpolarized (129)Xe magnetic resonance imaging

Animal disease models are pivotal in investigating the pathogenesis of emphysema and developing novel drugs, but the modalities to evaluate murine emphysema models have been of limited validity and sensitivity. In this study, we evaluated hyperpolarized (129)Xe magnetic resonance imaging (MRI) and m...

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Published in:American journal of respiratory cell and molecular biology Vol. 49; no. 4; pp. 592 - 600
Main Authors: Tetsumoto, Satoshi, Takeda, Yoshito, Imai, Hirohiko, Kimura, Atsuomi, Jin, Yingji, Nakanishi, Kaori, Maeda, Yohei, Kuhara, Hanako, Tsujino, Kazuyuki, Iwasaki, Takeo, Shigeta, Hiroshi, Kondo, Yasushi, Ito, Mari, Minami, Toshiyuki, Hirata, Haruhiko, Takahashi, Ryo, Kohmo, Satoshi, Nagatomo, Izumi, Inoue, Koji, Kida, Hiroshi, Kijima, Takashi, Tachibana, Isao, Maeda, Norikazu, Funahashi, Toru, Shimomura, Iichiro, Fujiwara, Hideaki, Kumanogoh, Atsushi
Format: Journal Article
Language:English
Published: United States 01-10-2013
Subjects:
Animals
Disease Models, Animal
Magnetic Resonance Imaging - methods
Male
Mice
Mice, Inbred C57BL
Pulmonary Alveoli - diagnostic imaging
Pulmonary Alveoli - pathology
Pulmonary Emphysema - diagnostic imaging
Pulmonary Emphysema - pathology
Tomography, X-Ray Computed - methods
Xenon Isotopes - analysis
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Summary:Animal disease models are pivotal in investigating the pathogenesis of emphysema and developing novel drugs, but the modalities to evaluate murine emphysema models have been of limited validity and sensitivity. In this study, we evaluated hyperpolarized (129)Xe magnetic resonance imaging (MRI) and micro-computed tomography (micro-CT) compared with traditional methods, such as plethysmography and histology. Elastase-treated mice and adiponectin knockout mice were used as murine emphysema models to evaluate these modalities. Three weeks after elastase administration, significant and heterogeneous emphysema was evaluated according to the mean linear intercept and plethysmography parameters. Notably, the distribution of low-density areas, as examined by micro-CT, correlated with the mean linear intercept and plethysmography parameters in whole lungs. These correlations were also observed in regional areas. Furthermore, we introduced hyperpolarized (129)Xe MRI, which can evaluate gas exchange between the alveoli and blood during spontaneous breathing. Parameters of gas exchange (fD) and alveolar size (Vs/Va) were significantly decreased in elastase-treated mice, and moderately correlated with the plethysmography parameters. Of importance, we could detect a decrease of the fD value in low-density areas with micro-CT, suggesting that gas exchange decreased in emphysematous lesions. Likewise, these parameters (fD and Vs/Va) were also decreased in adiponectin knockout mice, which exhibit emphysema with a homogeneous distribution. We demonstrated the feasibility of (129)Xe MRI and micro-CT in combination with traditional modalities. These noninvasive modalities provide complementary data that can be used for repeated estimations of regional gas exchange and lung morphology.
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ISSN:1535-4989
DOI:10.1165/rcmb.2012-0350OC