摘要: Motivation: Polygenic risk scores and other genomic analyses require large individual-level genotype datasets, yet strict data access restrictions impede sharing. Synthetic genotype generation offers a privacy-preserving alternative, but most existing methods operate unconditionally—producing samples without phenotype alignment—or rely on unsupervised compression, creating a gap between statistical fidelity and downstream task utility. Results: We present SNPgen, a two-stage conditional latent diffusion framework for generating phenotype-supervised synthetic genotypes. SNPgen combines GWAS-guided variant selection (1,024–2,048 trait-associated SNPs) with a variational autoencoder for genotype compression and a latent diffusion model conditioned on binary disease labels via classifier-free guidance. Evaluated on 458,724 UK Biobank individuals across four complex diseases (coronary artery disease, breast cancer, type 1 and type 2 diabetes), models trained on synthetic data matched real-data predictive performance in a train-on-synthetic, test-on-real protocol, approaching genome-wide PRS methods that use 2–6× more variants. Privacy analysis confirmed zero identical matches, near-random membership inference (AUC ≈ 0.50), preserved linkage disequilibrium structure, and high allele frequency correlation (r≥0.95) with source data. A controlled simulation with known causal effects verified faithful recovery of the imposed genetic association structure. Availability and implementation: Code available at https://github.com/ht-diva/SNPgen. Contact: andrea.lampis@polimi.it Supplementary information: Supplementary data are available in the Appendix.