Regulation of <scp>LRRK2 mRNA</scp> stability by <scp>ATIC</scp> and its substrate <scp>AICAR</scp> through <scp>ARE</scp>‐mediated <scp>mRNA</scp> decay in Parkinson's disease

Liu, Qinfang; Zhu, Dong; Li, Naren; Chen, Shifan; Hu, Liang; Yu, Jianzhong; Xiong, Yulan

doi:10.15252/embj.2022113410

Cited by 6 publications

(2 citation statements)

References 79 publications

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“…2). We found that in G2019S L2PD a number of proteins expression was reduced namely, ATIC, which can repress LRRK2 and rescue neurodegeneration 48 (log2FC=-0.97, adj. P=1.92x10 -13 ); RAB9A, involved in phagocytic vesicle trafficking and lysosomal function (log2FC=-1.17, adj.…”

Section: Resultsmentioning

confidence: 98%

“…61 Thus, ATIC, the top protein down-regulated in G2019S carriers, catalyses the last two steps of mitochondria purine biosynthesis 62,63 and was also linked previously to LRRK2 toxicity. 48 Other deficits included KARS1, a tRNA synthetase; PSMC5, the proteasomal 26S subunit; or SCLY, seleno-cysteine lyase, an enzyme involved in peptide elongation that is also involved in neurodegeneration. 64 Our findings in LRRK2 PMBCs align with studies reporting transcriptional repression of proteostasis regulators in G2019S L2PD, 65 and proteostasis defects in PD substantia nigra.…”

Section: Discussionmentioning

confidence: 99%

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In-depth mass-spectrometry reveals phospho-RAB12 as a blood biomarker of G2019S LRRK2-driven Parkinson’s

Cortés,

Phung,

de Mena

et al. 2024

Preprint

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Leucine-rich repeat kinase 2 (LRRK2) inhibition is a promising disease-modifying therapy for LRRK2-associated Parkinson disease (L2PD) and idiopathic PD (iPD). Yet, pharmaco-dynamic readouts and progression biomarkers for disease modification clinical trials are insufficient. Employing phospho-/proteomic analyses we assessed the impact that LRRK2 activating mutations had in peripheral blood mononuclear cells (PBMCs) from a LRRK2 clinical cohort from Spain (n=174) encompassing G2019S L2PD patients (n=37), non-manifesting LRRK2 mutation carriers of G2019S, here, G2019S L2NMCs (n=27), R1441G L2PD patients (n=14), R1441G L2NMCs (n=11), iPD (n=40), and controls (n=45). We identified 207 differential proteins in G2019S L2PD compared to controls (39 up/ 168 down) and 67 in G2019S L2NMCs (10 up/ 57 down). G2019S down-regulated proteins affected the endolysosomal pathway, proteostasis and mitochondria, e.g., ATIC, RAB9A, or LAMP1. At the phospho-proteome level, we observed increases in endogenous phosphorylation levels of pSer106 RAB12 in G2019S carriers, which were validated by immunoblotting after 1 year of follow-up (n=48). Freshly collected PBMCs from 3 G2019S L2PD, 1 R1441G L2PD, 1 iPD, and 5 controls (n=10) showed strong diminishment of pSer106 RAB12 phosphorylation levels after in-vitro administration of the MLi-2 LRRK2 inhibitor. Using machine learning, we identified an 18-feature G2019S phospho-/protein signature capable of discriminating G2019S L2PD, L2NMCs, and controls with 96% accuracy that correlated with disease severity, i.e., UPDRS-III motor scoring. Our study identified pSer106 RAB12 as an endogenous biomarker in easily accessible PBMCs from G2019S carriers and suggests that phospho-/proteomic findings in human PBMCs such as pSer106 RAB12 can be deployed as a universal pharmaco-dynamic readout for L2PD, L2NMCs, and iPD. Future work may determine whether pSer106 RAB12 could help with patient enrichment and monitoring drug efficacy in LRRK2 clinical trials.

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Section: Resultsmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 99%

In-depth mass-spectrometry reveals phospho-RAB12 as a blood biomarker of G2019S LRRK2-driven Parkinson’s

Cortés,

Phung,

de Mena

et al. 2024

Preprint

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Roncoroni Re‐Visited: The Neuronal Intranuclear Rodlet Comes of Age

Woulfe,

Munoz

2024

J of Comparative Neurology

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Despite myriad technological advances in neuroscience, the nervous system harbors morphological phenomena that continue to defy explanation. First described by the classical microscopists, including Santiago Ramon y Cajal, at the end of the 19th century, the neuronal intranuclear rodlet (INR) has mystified neurohistologists and microscopists for centuries. In this review article, we will provide an overview of the discovery of the INR as well as the subsequent attempts to elucidate its nature and functional significance. We outline our own studies of this structure over the past three decades, focusing on its elusive nature, its interactions with other nuclear organelles, and on disease‐related quantitative changes in Alzheimer's disease. We then describe our somewhat serendipitous discovery that these structures are filamentous aggregates of the nucleotide‐synthesizing metabolic enzyme inosine monophosphate dehydrogenase. The filamentation of metabolic enzymes to form mesoscale cellular structures called “rods and rings” or “cytoophidia” (Greek for “cellular snakes”) is a recently described phenomenon that remains to be systematically investigated in the nervous system. Thus, this review provides an intriguing historical juxtaposition in neuroscience, inculcating the neuronal INR, once a mere morphological curiosity, into one of the most rapidly evolving fields in contemporary cell biology.

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LRRK2 in Parkinson's disease: upstream regulation and therapeutic targeting

Xiong,

2024

Trends in Molecular Medicine

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Regulation of LRRK2 mRNA stability by ATIC and its substrate AICAR through ARE‐mediated mRNA decay in Parkinson's disease

Cited by 6 publications

References 79 publications

In-depth mass-spectrometry reveals phospho-RAB12 as a blood biomarker of G2019S LRRK2-driven Parkinson’s

In-depth mass-spectrometry reveals phospho-RAB12 as a blood biomarker of G2019S LRRK2-driven Parkinson’s

Roncoroni Re‐Visited: The Neuronal Intranuclear Rodlet Comes of Age

LRRK2 in Parkinson's disease: upstream regulation and therapeutic targeting

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