Urinary bis(monacylglycerol) phosphate (BMP) levels are higher in LRRK2 and GBA1 variant carriers but do not predict disease progression in PPMI cohorts

Author:

Merchant Kalpana1ORCID,Simuni Tanya2ORCID,Fedler Janel3ORCID,Caspell-Garcia Chelsea4,Brumm Michael3,Nudelman Kelly5ORCID,Tengstrand Elizabeth6,Hsieh Frank6,Alcalay Roy7,Coffey Chris4,Chahine Lana8,Foroud Tatiana9,Singleton Andrew10ORCID,weintraub daniel11,Hutten Samantha12,Sherer Todd12,Siderowf Andrew13,Mollenhauer Brit14,Tanner Caroline15ORCID,Marek Ken16

Affiliation:

1. Northwestern University

2. Northwestern University Feinberg School of Medicine, Chicago, IL, USA

3. The University of Iowa

4. University of Iowa

5. National Cell Repository for Alzheimer's disease

6. Nextcea, Inc.

7. Columbia University

8. University of Pittsburgh

9. Indiana University

10. National Institute on Aging (NIA), NIH

11. Uni Pensylvannia

12. The Michael J. Fox Foundation for Parkinson’s Research

13. University of Pennsylvania

14. University Medical Centre Goettingen

15. University of California - San Francisco

16. Institute for Neurodegenerative Disorders

Abstract

Abstract We quantified concentrations of three isoforms of the endolysosomal lipid, bis(monoacylglycerol) phosphate (BMP) in urine of deeply phenotyped cohorts in the Parkinson’s Progression Markers Initiative: LRRK2 G2019S PD (N = 134) and non-manifesting carriers (NMC) (G2019S + NMC; N = 182), LRRK2 R1441G PD (N = 15) and R1441G + NMC (N = 15), GBA1 N409S PD (N = 76) and N409S + NMC (N = 178), sporadic PD (sPD, N = 379) and healthy controls (HC) (N = 190). Effects of each mutation and disease status were analyzed using nonparametric methods. Longitudinal changes in BMP levels were analyzed using linear mixed models. At baseline, all LRRK2 carriers had 3-7x higher BMP levels compared to HC, irrespective of the disease status. GBA1 N409S carriers also showed significant, albeit smaller, elevation (~ 30–40%) in BMP levels compared to HC. In LRRK2 G2019S PD, urinary BMP levels remained stable over two years. Furthermore, baseline BMP levels did not predict disease progression as measured by striatal DaT imaging, MDS-UPDRS III Off or MoCA in any of the cohorts. These data support the utility of BMP as a target modulation biomarker in therapeutic trials of genetic and sPD but not as a prognostic or disease progression biomarker.

Publisher

Research Square Platform LLC

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