Pleural effusion is a common medical problem in the chest and involves accumulation of an abnormal amount of pleural fluid in the pleural space. The severity of these symptoms depends on the volume and composition of the fluid, while the final outcome usually depends on the underlying disease responsible for the effusion. Pleural serosal inflammation on the surface of mesothelial cells and recruitment of leukocyte into the pleural cavity were considered related to the pleural effusion formation. In addition, a local tissue-based RAS has also been described and appears to play a key role in injury/repair responses. The known angiotensin converting enzyme (ACE)/angiotensin II (Ang II) /AT1R axis of RAS system and angiotensin converting enzyme II (ACE2)/Ang- (1-7) / Mas receptor axis were closely related to tissue structural maintenance, fibrosis of lung disease, and pulmonary fibrosis progression. Also, the performance of matrix metalloproteinases (MMPs) and its endogenous inhibition factor (tissue inhibitors of MMPs; TIMPs) are often used as the indicators of assessing extracellular matrix (ECM) structural remodeling. In this proposal, we tried to explore the correlation between ACE/Ang II/AT1R axis, ACE2/Ang-(1-7)/Mas axis, MMPs/TIMPs and pleural diseases. This study also investigated the frequency of the polymorphisms of MMP-2 and MMP-9 genes in the patients with pleural effusions. In the first part of experiment, we had analyzed the activity of ACE/ACE2 and MMPs in human pleural effusions in order to explore the connections between ACE/ACE2 and MMPs/TIMPs balance in the pleural effusion and pulmonary fibrosis. The −1059G/A MMP-2, −735C/T MMP-2 and −1562C/T MMP-9 polymorphisms were analyzed in the patients with different disease. In the second part, we successfully established a mouse model of pulmonary fibrosis to investigate the pathogenesis of pulmonary fibrosis, and the balancing activity ACE/ACE2 as well as MMPs/TIMPs. There were several results of our study. First of all, we found (1) a significant higher ACE activity resulting a significantly higher ratio of ACE/ACE2, in the exudative effusions; (2) an increased MMP-9 activity was found in the exudates; (3) in the tuberculous effusions, a significantly higher ADA activity combined with elevated MMP-9 and ACE levels, and reduced ACE2 activity were detected. Second, None of the polymorphisms, including genotypes distribution and allele frequency in −1059G/A MMP-2, −735C/T MMP-2 and −1562C/T MMP-9 was significantly associated with either adenocarcinoma or pneumonia exudates compared with transudates. Pleural MMP-2 activity was higher in homozygous −735CC MMP-2 patients. Pleural MMP-9 activity was higher in heterozygous −1562CT MMP-9 patients. Third, in the animal study, ACE, MMP-9 activities and TIMP-1 concentration in the lung tissue were significantly increased in wild-type (WT) mice injected bleomycin at 7-day and the histological sections showed significant leukocyte infiltration and collagen accumulation. The lung tissue MMP-9 activity is significantly higher in heterozygous, homozygous and hemizygous ACE2 KO mice than Control in early stage (3-day), and TIMP-1 concentration is significantly decreased. Those findings implied that the important role of ACE2 on bleomycin-induced pulmonary fibrosis may be via the regulation of MMP-9/TIMP-1 expression.