- Mandel-Brehm, Caleigh;
- Vazquez, Sara E;
- Liverman, Christopher;
- Cheng, Mickie;
- Quandt, Zoe;
- Kung, Andrew F;
- Parent, Audrey;
- Miao, Brenda;
- Disse, Emmanuel;
- Cugnet-Anceau, Christine;
- Dalle, Stéphane;
- Orlova, Elizaveta;
- Frolova, Elena;
- Alba, Diana;
- Michels, Aaron;
- Oftedal, Bergithe E;
- Lionakis, Michail S;
- Husebye, Eystein S;
- Agarwal, Anil K;
- Li, Xilong;
- Zhu, Chengsong;
- Li, Quan;
- Oral, Elif;
- Brown, Rebecca;
- Anderson, Mark S;
- Garg, Abhimanyu;
- DeRisi, Joseph L
Acquired lipodystrophy is often characterized as an idiopathic subtype of lipodystrophy. Despite suspicion of an immune-mediated pathology, biomarkers such as autoantibodies are generally lacking. Here, we used an unbiased proteome-wide screening approach to identify autoantibodies to the adipocyte-specific lipid droplet protein perilipin 1 (PLIN1) in a murine model of autoimmune polyendocrine syndrome type 1 (APS1). We then tested for PLIN1 autoantibodies in human subjects with acquired lipodystrophy with two independent severe breaks in immune tolerance (including APS1) along with control subjects using a specific radioligand binding assay and indirect immunofluorescence on fat tissue. We identified autoantibodies to PLIN1 in these two cases, including the first reported case of APS1 with acquired lipodystrophy and a second patient who acquired lipodystrophy as an immune-related adverse event following cancer immunotherapy. Lastly, we also found PLIN1 autoantibodies to be specifically enriched in a subset of patients with acquired generalized lipodystrophy (17 of 46 [37%]), particularly those with panniculitis and other features of autoimmunity. These data lend additional support to new literature that suggests that PLIN1 autoantibodies represent a marker of acquired autoimmune lipodystrophies and further link them to a break in immune tolerance.