Publications by authors named "Aisyah Rahmawati"

Article Synopsis
  • Glycerophosphocholine (GPC) is a metabolite related to choline in cells and has been considered a potential supplement for brain health, but high choline intake may lead to TMAO production, linked to atherosclerosis.
  • This study investigates how GPC is absorbed and metabolized by the intestine, showing that it converts to choline and is transported into cells.
  • Researchers highlighted the enzyme Gpcpd1, which regulates this conversion and TMAO levels, with experiments indicating that its absence alters GPC metabolism and lowers TMAO in the bloodstream.
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Aims: Streptozotocin (STZ) is widely used to study diabetic complications. Owing to the nonspecific cytotoxicity of high-dose STZ, alternative models using moderate-dose or a combination of low-dose STZ and a high-fat diet have been established. This study aimed to investigate the effects of these models on muscle function.

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This study aims to analyze the mediating role of employee engagement and the green work environment in the relationship between motivation and the performance of logistics company employees in Jakarta, Indonesia. Employing a causal quantitative research approach, we distributed 222 questionnaires among logistics employees from four surrounding cities in Jakarta, namely Bogor, Depok, Tangerang, and Bekasi. These questionnaires were adapted from past studies.

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Early detection of drug-induced kidney injury is essential for drug development. In this study, multiple low-dose aristolochic acid (AA) and cisplatin (Cis) injections increased renal mRNA levels of inflammation, fibrosis, and renal tubule injury markers. We applied a serum amyloid A3 (Saa3) promoter-driven luciferase reporter (Saa3 promoter-luc mice) to these two tubulointerstitial nephritis models and performed bioluminescence imaging to monitor early renal pathologies.

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Glycerophosphocholine (GPC) is an important precursor for intracellular choline supply in phosphatidylcholine (PC) metabolism. GDE5/Gpcpd1 hydrolyzes GPC into choline and glycerol 3-phosphate; this study aimed to elucidate its physiological function in vivo. Heterozygous whole-body GDE5-deficient mice reveal a significant GPC accumulation across tissues, while homozygous whole-body knockout results in embryonic lethality.

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