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A recent genome‐wide association study has determined that the Niemann‐Pick C1 (NPC1) gene is associated with early‐onset and morbid adult obesity. However, what effects of the nonsynonymous variation in NPC1 on protein function result in weight gain remains unknown. The NPC1 heterozygous mouse model (Npc1+/−), which expresses one‐half the normal amounts of functional Npc1 protein compared to the homozygous normal (Npc1+/+) mouse, was used to determine whether decreased Npc1 gene dosage was associated with weight gain when fed either a low‐fat (10% kcal fat) or high‐fat (45% kcal fat) diet beginning at 4 weeks of age until 20 weeks of age. The results indicated that Npc1+/− mice had significantly increased weight gain beginning at 13 weeks of age when fed a high‐fat diet, but not when fed a low‐fat diet, compared to the Npc1+/+ mice fed the same diet. With respect to mice fed a high‐fat diet, the Npc1+/− mice continued to have significantly increased weight gain to 30 weeks of age. At this age, the Npc1+/− mice were found to have increased liver and inguinal adipose weights compared to the Npc1+/+ mice. Therefore, decreased Npc1 gene dosage resulting in decreased Npc1 protein function, promoted weight gain in mice fed a high‐fat diet consistent with a gene–diet interaction.