Inherited Disorders of Coenzyme A Biosynthesis: Models, Mechanisms, and Treatments

Cavestro, Chiara; Diodato, Daria; Tiranti, Valeria; Meo, Ivano Di

doi:10.3390/ijms24065951

Cited by 7 publications

(7 citation statements)

References 141 publications

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“…It is clear that brain iron accumulation is a characteristic of many neurodegenerative pathologies, including the most widespread disorders, such as Alzheimer’s disease and Parkinson’s disease [ 9 , 36 ]; however, the specific mechanism of iron deposition and its contribution to neuronal death are not yet fully understood [ 9 ]. In particular, the relationship between CoA biosynthesis defects and brain iron accumulation in PKAN disorders has not yet been elucidated [ 37 ].…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial iron deficiency triggers cytosolic iron overload in PKAN hiPS-derived astrocytes

Santambrogio,

Cozzi,

Balestrucci

et al. 2024

Cell Death Dis

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Disease models of neurodegeneration with brain iron accumulation (NBIA) offer the possibility to explore the relationship between iron dyshomeostasis and neurodegeneration. We analyzed hiPS-derived astrocytes from PANK2-associated neurodegeneration (PKAN), an NBIA disease characterized by progressive neurodegeneration and high iron accumulation in the globus pallidus. Previous data indicated that PKAN astrocytes exhibit alterations in iron metabolism, general impairment of constitutive endosomal trafficking, mitochondrial dysfunction and acquired neurotoxic features. Here, we performed a more in-depth analysis of the interactions between endocytic vesicles and mitochondria via superresolution microscopy experiments. A significantly lower number of transferrin-enriched vesicles were in contact with mitochondria in PKAN cells than in control cells, confirming the impaired intracellular fate of cargo endosomes. The investigation of cytosolic and mitochondrial iron parameters indicated that mitochondrial iron availability was substantially lower in PKAN cells compared to that in the controls. In addition, PKAN astrocytes exhibited defects in tubulin acetylation/phosphorylation, which might be responsible for unregulated vesicular dynamics and inappropriate iron delivery to mitochondria. Thus, the impairment of iron incorporation into these organelles seems to be the cause of cell iron delocalization, resulting in cytosolic iron overload and mitochondrial iron deficiency, triggering mitochondrial dysfunction. Overall, the data elucidate the mechanism of iron accumulation in CoA deficiency, highlighting the importance of mitochondrial iron deficiency in the pathogenesis of disease.

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Section: Discussionmentioning

confidence: 99%

Mitochondrial iron deficiency triggers cytosolic iron overload in PKAN hiPS-derived astrocytes

Santambrogio,

Cozzi,

Balestrucci

et al. 2024

Cell Death Dis

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“…Although clinical trials with several compounds are in progress, PKAN treatments primarily aim to control the main disease symptoms: spasticity, seizures, dystonia, or psychiatric disorders [124]. Nevertheless, several promising therapeutic approaches are currently in progress [12,91]. These treatments can be summarized in four categories: (1) iron chelation to eliminate iron accumulation in the brain; (2) metabolite supplementation to correct metabolic deficits in the CoA pathway; (3) PANK isoforms activation to restore CoA biosynthesis; and (4) gene therapy by introducing the wild-type PANK2 gene.…”

Section: Therapeutic Strategies For Pkanmentioning

confidence: 99%

“…However, some of these therapies have not been successful, whereas others are under evaluation. For a detailed updated of current PKAN treatment approaches see [12,91,124,125].…”

Section: Therapeutic Strategies For Pkanmentioning

confidence: 99%

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Patient-Derived Cellular Models for Polytarget Precision Medicine in Pantothenate Kinase-Associated Neurodegeneration

Álvarez-Córdoba,

Talaverón-Rey,

Povea-Cabello

et al. 2023

Pharmaceuticals

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The term neurodegeneration with brain iron accumulation (NBIA) brings together a broad set of progressive and disabling neurological genetic disorders in which iron is deposited preferentially in certain areas of the brain. Among NBIA disorders, the most frequent subtype is pantothenate kinase-associated neurodegeneration (PKAN) caused by pathologic variants in the PANK2 gene codifying the enzyme pantothenate kinase 2 (PANK2). To date, there are no effective treatments to stop the progression of these diseases. This review discusses the utility of patient-derived cell models as a valuable tool for the identification of pharmacological or natural compounds for implementing polytarget precision medicine in PKAN. Recently, several studies have described that PKAN patient-derived fibroblasts present the main pathological features associated with the disease including intracellular iron overload. Interestingly, treatment of mutant cell cultures with various supplements such as pantothenate, pantethine, vitamin E, omega 3, α-lipoic acid L-carnitine or thiamine, improved all pathophysiological alterations in PKAN fibroblasts with residual expression of the PANK2 enzyme. The information provided by pharmacological screenings in patient-derived cellular models can help optimize therapeutic strategies in individual PKAN patients.

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“…As critical components in cellular metabolism, COA-SH and ATP are strongly linked to cell growth, death, and energy provision. 19,20 Abnormal levels of these molecules in the body closely correlate with various diseases, 21 such as cardiovascular diseases, 22 Parkinson's disease, 23 and Alzheimer's disease. 24 Therefore, the development of point-of-care testing (POCT) sensors capable of directly and accurately detecting COA-SH and ATP holds significant importance.…”

Section: Introductionmentioning

confidence: 99%

Direct single-molecule detection of CoA-SH and ATP by the membrane proteins TMEM120A and TMEM120B

Zhao,

Chen,

Liu

et al. 2024

Nanoscale

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Inherited Disorders of Coenzyme A Biosynthesis: Models, Mechanisms, and Treatments

Cited by 7 publications

References 141 publications

Mitochondrial iron deficiency triggers cytosolic iron overload in PKAN hiPS-derived astrocytes

Mitochondrial iron deficiency triggers cytosolic iron overload in PKAN hiPS-derived astrocytes

Patient-Derived Cellular Models for Polytarget Precision Medicine in Pantothenate Kinase-Associated Neurodegeneration

Direct single-molecule detection of CoA-SH and ATP by the membrane proteins TMEM120A and TMEM120B

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