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Oleic Acid-Containing Phosphatidylinositol Is a Blood Biomarker Candidate for SPG28
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Hereditary spastic paraplegia is a genetic neurological disorder characterized by spasticity of the lower limbs, and spastic paraplegia type 28 is one of its subtypes. Spastic paraplegia type 28 is a hereditary neurogenerative disorder with an autosomal recessive inheritance caused by loss of function of DDHD1. DDHD1 encodes phospholipase A1, which catalyzes phospholipids to lysophospholipids such as phosphatidic acids and phosphatidylinositols to lysophosphatidic acids and lysophoshatidylinositols. Quantitative changes in these phospholipids can be key to the pathogenesis of SPG28, even at subclinical levels. By lipidome analysis using plasma from mice, we globally examined phospholipids to identify molecules showing significant quantitative changes in Ddhd1 knockout mice. We then examined reproducibility of the quantitative changes in human sera including SPG28 patients. We identified nine kinds of phosphatidylinositols that show significant increases in Ddhd1 knockout mice. Of these, four kinds of phosphatidylinositols replicated the highest level in the SPG28 patient serum. All four kinds of phosphatidylinositols contained oleic acid. This observation suggests that the amount of oleic acid-containing PI was affected by loss of function of DDHD1. Our results also propose the possibility of using oleic acid-containing PI as a blood biomarker for SPG28.
Title: Oleic Acid-Containing Phosphatidylinositol Is a Blood Biomarker Candidate for SPG28
Description:
Hereditary spastic paraplegia is a genetic neurological disorder characterized by spasticity of the lower limbs, and spastic paraplegia type 28 is one of its subtypes.
Spastic paraplegia type 28 is a hereditary neurogenerative disorder with an autosomal recessive inheritance caused by loss of function of DDHD1.
DDHD1 encodes phospholipase A1, which catalyzes phospholipids to lysophospholipids such as phosphatidic acids and phosphatidylinositols to lysophosphatidic acids and lysophoshatidylinositols.
Quantitative changes in these phospholipids can be key to the pathogenesis of SPG28, even at subclinical levels.
By lipidome analysis using plasma from mice, we globally examined phospholipids to identify molecules showing significant quantitative changes in Ddhd1 knockout mice.
We then examined reproducibility of the quantitative changes in human sera including SPG28 patients.
We identified nine kinds of phosphatidylinositols that show significant increases in Ddhd1 knockout mice.
Of these, four kinds of phosphatidylinositols replicated the highest level in the SPG28 patient serum.
All four kinds of phosphatidylinositols contained oleic acid.
This observation suggests that the amount of oleic acid-containing PI was affected by loss of function of DDHD1.
Our results also propose the possibility of using oleic acid-containing PI as a blood biomarker for SPG28.
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