| Id |
Subject |
Object |
Predicate |
Lexical cue |
| T1 |
0-140 |
Sentence |
denotes |
Long-Term Expression of the Human CFTR Gene in Mouse Airway via Helper-Dependent Adenoviral Vector Delivery and Transient Immunosuppression. |
| T2 |
141-308 |
Sentence |
denotes |
Sustained expression of the CFTR gene is a major challenge to gene therapy with either viral or nonviral vectors with immune response to vector and transgene products. |
| T3 |
309-433 |
Sentence |
denotes |
One strategy to achieve sustained CFTR expression is to modulate the host immune system through transient immunosuppression. |
| T4 |
434-723 |
Sentence |
denotes |
In this study, we examined cyclophosphamide (cytoxan), dexamethasone (Dex), and a combination of cyclosporin, methylprednisolone, and azathioprine (combination) for their effects on long-term expression of the human CFTR delivered with helper-dependent adenoviral vectors in mouse airways. |
| T5 |
724-889 |
Sentence |
denotes |
We found that cyclophosphamide significantly enhanced long-term expression of the transgenic human CFTR and the reporter gene LacZ by reducing host immune responses. |
| T6 |
890-1000 |
Sentence |
denotes |
Dex administration greatly reduced neutralizing antibody production but had no effect on transgene expression. |
| T7 |
1001-1140 |
Sentence |
denotes |
Treatment with a combination of cyclosporin A, azathioprine, and methylprednisolone affected neither CFTR gene expression nor inflammation. |
| T8 |
1141-1259 |
Sentence |
denotes |
Our data suggest that transient immunosuppression might be a strategy to improve sustained expression in gene therapy. |
| T1 |
0-140 |
Sentence |
denotes |
Long-Term Expression of the Human CFTR Gene in Mouse Airway via Helper-Dependent Adenoviral Vector Delivery and Transient Immunosuppression. |
| T2 |
141-308 |
Sentence |
denotes |
Sustained expression of the CFTR gene is a major challenge to gene therapy with either viral or nonviral vectors with immune response to vector and transgene products. |
| T3 |
309-433 |
Sentence |
denotes |
One strategy to achieve sustained CFTR expression is to modulate the host immune system through transient immunosuppression. |
| T4 |
434-723 |
Sentence |
denotes |
In this study, we examined cyclophosphamide (cytoxan), dexamethasone (Dex), and a combination of cyclosporin, methylprednisolone, and azathioprine (combination) for their effects on long-term expression of the human CFTR delivered with helper-dependent adenoviral vectors in mouse airways. |
| T5 |
724-889 |
Sentence |
denotes |
We found that cyclophosphamide significantly enhanced long-term expression of the transgenic human CFTR and the reporter gene LacZ by reducing host immune responses. |
| T6 |
890-1000 |
Sentence |
denotes |
Dex administration greatly reduced neutralizing antibody production but had no effect on transgene expression. |
| T7 |
1001-1140 |
Sentence |
denotes |
Treatment with a combination of cyclosporin A, azathioprine, and methylprednisolone affected neither CFTR gene expression nor inflammation. |
| T8 |
1141-1259 |
Sentence |
denotes |
Our data suggest that transient immunosuppression might be a strategy to improve sustained expression in gene therapy. |
