Chemoattraction activity for cells expressing specific receptors in vitro induced by transfection of Ad-RGD-chemokines into A549 cells. Chemoattractant activity of culture supernatants of A549 cells transfected with each chemokine gene-carrying Ad-RGD against the stable specific chemokine receptor-expressing cells. The culture supernatants of intact A549 cells, Ad-RGD-Luc-transfected A549 (Luc/A549) cells, and chemokine gene-transduced A549 cells were prepared and diluted with the assay medium. The fractional values within the parentheses in each panel express the dilution factor. These samples and recombinant chemokines dissolved with the assay medium were added to a 24-well culture plate. Cells expressing specific receptors for CCL17 and CCL22 (L1.2/CCR4), CCL20 (L1.2/CCR6), CCL19 and CCL21 (L1.2/CCR7), CCL27 (L1.2/CCR10), XCL1 (L1.2/XCR1), or CX3CL1 (L1.2/CX3CR1) were suspended with the assay medium and placed in a Chemotaxicell-24 installed in each well at 1 × 10⁶ cells /well. Likewise, parental L1.2 cells for these transfectants were prepared and added to the Chemotaxicell-24. Cell migration was allowed for 2 h at 37°C in a 5% CO₂ atmosphere. The cells that migrated to the lower well were lysed and quantified using a PicoGreen double-stranded DNA quantification reagent. The data are expressed as the mean±SE of the triplicate results. (Reproduced from Okada et al. [40]).

Enhancement of DC migration to lymphoid tissues by chemokine receptor expression on DCs. Increasing the migratory ability of a DC vaccine toward lymphoid tissue would remarkably improve the efficacy of DC-based immunotherapy. The chemokine receptor (CCR7) facilitates DC migration to lymphoid tissues. Superior lymphoid tissue-accumulation of DCs transduced with the CCR7 gene (CCR7/DCs) is advantageous as a vaccine carrier because it efficiently activates immune effector cells in regional lymph nodes.

Accumulation of immune cells in ovarian carcinoma in vivo by transfection of chemokine-encoding adenovirus vectors. Left: CD3-positive lymphocytes infiltrated into OV-HM tumors infected with Ad-RGD-mCCL27 and Ad-RGD-mCX₃CL1. a–d Representative immunohistochemical appearance of tumor nodules from mice inoculated intradermally with 1 × 10⁶ OV-HM cells infected with a none, b Ad-RGD, c Ad-RGD-mCCL27, or d Ad-RGD-mCX₃CL1. Right: NK cells infiltrated into OV-HM tumors infected with Ad-RGD-mCCL27 and Ad-RGD-mCX₃CL1. e–h Representative immunohistochemical appearance of tumor nodules from mice inoculated intradermally with 1 × 10⁶ OV-HM cells infected with e none, f Ad-RGD, g Ad-RGD-mCCL27, or h Ad-RGD-mCX₃CL1. (Reproduced from Gao et al. [39]).