Exploratory study reveals far reaching systemic and cellular effects of verapamil treatment in subjects with type 1 diabetes.
| Citation | Xu, Guanlan, et al. “Exploratory Study Reveals Far Reaching Systemic and Cellular Effects of Verapamil Treatment in Subjects With Type 1 Diabetes”. 2022. Nature Communications, vol. 13, no. 1, 2022, p. 1159.  | 
       
| Center | University of Alabama at Birmingham | 
| Featured | 
   Featured 
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| Author | Guanlan Xu, Tiffany D Grimes, Truman B Grayson, Junqin Chen, Lance A Thielen, Hubert M Tse, Peng Li, Matt Kanke, Tai-Tu Lin, Athena A Schepmoes, Adam C Swensen, Vladislav A Petyuk, Fernando Ovalle, Praveen Sethupathy, Wei-Jun Qian, Anath Shalev | 
| Abstract | 
   Currently, no oral medications are available for type 1 diabetes (T1D). While our recent randomized placebo-controlled T1D trial revealed that oral verapamil had short-term beneficial effects, their duration and underlying mechanisms remained elusive. Now, our global T1D serum proteomics analysis identified chromogranin A (CHGA), a T1D-autoantigen, as the top protein altered by verapamil and as a potential therapeutic marker and revealed that verapamil normalizes serum CHGA levels and reverses T1D-induced elevations in circulating proinflammatory T-follicular-helper cell markers. RNA-sequencing further confirmed that verapamil regulates the thioredoxin system and promotes an anti-oxidative, anti-apoptotic and immunomodulatory gene expression profile in human islets. Moreover, continuous use of oral verapamil delayed T1D progression, promoted endogenous beta-cell function and lowered insulin requirements and serum CHGA levels for at least 2 years and these benefits were lost upon discontinuation. Thus, the current studies provide crucial mechanistic and clinical insight into the beneficial effects of verapamil in T1D.  | 
        
| Year of Publication | 
   2022 
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| Journal | 
   Nature communications 
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| Volume | 
   13 
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| Issue | 
   1 
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| Number of Pages | 
   1159 
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| Date Published | 
   03/2022 
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| ISSN Number | 
   2041-1723 
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| DOI | 
   10.1038/s41467-022-28826-3 
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| Alternate Journal | 
   Nat Commun 
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| PMCID | 
   PMC8894430 
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| PMID | 
   35241690 
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