- Tsao, Tasha;
- Qiu, Longhui;
- Bharti, Reena;
- Shemesh, Avishai;
- Hernandez, Alberto M;
- Cleary, Simon J;
- Greenland, Nancy Y;
- Santos, Jesse;
- Shi, Ruoshi;
- Bai, Lu;
- Richardson, Jennifer;
- Dilley, Kimberley;
- Will, Matthias;
- Tomasevic, Nenad;
- Sputova, Tereza;
- Salles, Adam;
- Kang, Jeffrey;
- Zhang, Dongliang;
- Hays, Steve R;
- Kukreja, Jasleen;
- Singer, Jonathan P;
- Lanier, Lewis L;
- Looney, Mark R;
- Greenland, John R;
- Calabrese, Daniel R
Background
Pulmonary ischaemia-reperfusion injury (IRI) is a major contributor to poor lung transplant outcomes. We recently demonstrated a central role of airway-centred natural killer (NK) cells in mediating IRI; however, there are no existing effective therapies for directly targeting NK cells in humans.Methods
We hypothesised that a depleting anti-CD94 monoclonal antibody (mAb) would provide therapeutic benefit in mouse and human models of IRI based on high levels of KLRD1 (CD94) transcripts in bronchoalveolar lavage samples from lung transplant patients.Results
We found that CD94 is highly expressed on mouse and human NK cells, with increased expression during IRI. Anti-mouse and anti-human mAbs against CD94 showed effective NK cell depletion in mouse and human models and blunted lung damage and airway epithelial killing, respectively. In two different allogeneic orthotopic lung transplant mouse models, anti-CD94 treatment during induction reduced early lung injury and chronic inflammation relative to control therapies. Anti-CD94 did not increase donor antigen-presenting cells that could alter long-term graft acceptance.Conclusions
Lung transplant induction regimens incorporating anti-CD94 treatment may safely improve early clinical outcomes.