DNA gyrase, an ATP-dependent enzyme, plays a critical role in DNA replication, transcription, and recombination in Mycobacterium tuberculosis (MTB). While fluoroquinolones are effective antibacterial agents targeting DNA gyrase, their clinical use is often limited due to side effects and the emergence of bacterial resistance. In this study, we developed a quantitative structure-activity relationship (QSAR) model to predict the anti-tubercular activity of Quinoline-Aminopiperidine derivatives targeting the DNA gyrase enzyme, using a dataset of 48 compounds obtained from the literature. The QSAR model was validated using both internal and external validation metrics. Model 4, the best predictive model, demonstrated a strong fit with an R² of 0.8393, an adjusted R² (R²adj) of 0.8010, and a lack of fit (LOF) parameter of 0.0626. The QSAR results revealed that DNA gyrase inhibition is significantly influenced by factors such as partition coefficient, molecular flexibility, hydrogen bonding potential, and the presence of fluorine atoms. Twelve quinoline-aminopiperidine derivatives were designed, and their anti-tubercular activity was predicted using QSAR model-4. These compounds were further assessed for pharmacokinetic properties, toxicity, and binding affinity to DNA gyrase. Pharmacophore modeling was also performed and validated using MOE software. The final pharmacophore model includes the features of two aromatic hydrophobic features, one hydrogen bond acceptor, and one hydrogen bond donor. The results indicated that designed compounds QA-3 and dataset compounds C-34 exhibit favorable drug-likeness properties. Molecular dynamics simulations confirmed the stable binding of compounds QA-3 and C-34 to the DNA gyrase protein, highlighting their potential as promising anti-tubercular agents. The developed QSAR Model-4 will facilitate the prediction of anti-tubercular activity in Quinoline-Aminopiperidine derivatives.