Community-acquired pyogenic liver abscess (PLA) caused by Klebsiella pneumoniae has become an emerging infectious disease. Capsular serotypes K1 and K2 are predominant virulent strains of isolates in Taiwan. Phage therapy has several limitations before, but now it is one of potential therapeutic approaches due to antibiotic resistance. The phage has infection specificity and can be propagated in the presence of its host. Therefore, we evaluated the therapeutic potential of phage in PLA mice model. NTUH-K2044-K1-1 with full genome sequenced was chosen from different phage isolates covering all capsular types to do the pioneer study, which specifically infects K1 strains. Toxicity testing in animals revealed no rectal temperature rise. Pharmacokinetic analysis showed phage concentration reached its peak among different tissues at 6 h and retention of phage in spleen was still observed at 72 h. Moreover, phage potentially crossed blood-brain barrier. The level of TNF- The level of TNF-α and IL-6 in serum beared no difference after phage administration, however, the clearance rates among tissues significantly increased after repeated administrations. Intraperitoneal administration of a single dose of 108 PFU phage at 16 h or 24 h after intraperitoneal K. pneumonia infection was sufficient to improve 75% survival. The efficacy of phage therapy was evaluated in mice with image-documented abscess observed by animal MRI. The results of 8 phage-treated mice and 4 untreated mice illustrated that administration of 108 PFU phage twice a day for 2 weeks could prolong the life span of infected mice. These data suggested that phage therapy have the potential to become alternative or adjuvant agents in treating antibiotic-resistant or deep tissue infections.