Elevated Serum GAD65 and GAD65-GADA Immune Complexes in Stiff Person Syndrome

Glutamic acid decarboxylase 65 (GAD65) and autoantibodies specific for GAD65 (GADA) are associated with autoimmune diseases including Stiff Person Syndrome (SPS) and Type 1 diabetes (T1D). GADA is recognized as a biomarker of value for clinical diagnosis and prognostication in these diseases. Nonetheless, it remains medically interesting to develop sensitive and specific assays to detect GAD65 preceding GADA emergence, and to monitor GADA-GAD65 immune complexes in blood samples. In the present study, we developed a highly sensitive proximity ligation assay to measure serum GAD65. This novel assay allowed detection of as little as 0.65 pg/ml GAD65. We were also able to detect immune complexes involving GAD65 and GADA. Both free GAD65 and GAD65-GADA levels were significantly higher in serum samples from SPS patients compared to healthy controls. The proximity ligation assays applied for detection of GAD65 and its immune complexes may thus enable improved diagnosis and better understanding of SPS. Autoantibodies against glutamic acid decarboxylase 65 (GAD65) are found in a majority of patients with Stiff Person Syndrome (SPS) Detection of GAD65 and GAD65-GADA complexes in blood may enable earlier diagnosis, as well as monitoring of the ongoing destruction of targeted cells, provided sufficiently sensitive assays can be developed. In recent years, several relatively sensitive methods have been developed in attempts to detect endogenous GAD65 in blood. The most sensitive immunoassay allowed detection of GAD65 in human plasma spiked with as little as 31 pg/ml recombinant human GAD6

Integrative Personal Omics Profiles during Periods of Weight Gain and Loss

Advances in omics technologies now allow an unprecedented level of phenotyping for human diseases, including obesity, in which individual responses to excess weight are heterogeneous and unpredictable. To aid the development of better understanding of these phenotypes, we performed a controlled longitudinal weight perturbation study combining multiple omics strategies (genomics, transcriptomics, multiple proteomics assays, metabolomics, and microbiomics) during periods of weight gain and loss in humans. Results demonstrated that: (1) weight gain is associated with the activation of strong inflammatory and hypertrophic cardiomyopathy signatures in blood; (2) although weight loss reverses some changes, a number of signatures persist, indicative of long-term physiologic changes; (3) we observed omics signatures associated with insulin resistance that may serve as novel diagnostics; (4) specific biomolecules were highly individualized and stable in response to perturbations, potentially representing stable personalized markers. Most data are available open access and serve as a valuable resource for the community. Cell Syst 2018 Feb 28; 6(2):157-170.e8