Chronic mountain sickness (CMS) is
a high altitude complication
with high rates of morbidity and mortality. CMS is characterized by
high-altitude polycythemia (HAPC) and high-altitude pulmonary hypertension
(HAPH). In this study, macitentan, a dual endothelin receptor antagonist,
was used to treat CMS, and the induced metabolomics changes were studied.
CMS was induced in rats in a hypobaric hypoxia chamber (simulating
a 5500 m plateau) for 4 weeks. Macitentan was administered in the
third and fourth weeks (30 mg·kg–1·day–1). At the end of the follow-up period, we performed
echocardiography, measured hemodynamic parameters and hematocrit,
and performed histological staining. Furthermore, ultraperformance
liquid chromatography-mass spectrometry (UPLC–MS)-based metabolic
analysis was applied to explore metabolic changes associated with
hypobaric hypoxia, with or without macitentan. qRT-PCR and kits for
the determination of xanthine oxidase (XO) activity were used for
validation experiments. Macitentan was effective in attenuating CMS,
including CMS-induced right ventricle hypertrophy, HAPC, and HAPH.
The levels of 48 metabolites were significantly changed in the CMS
model group compared to the control group. Of these changes, 21 were
reversed by treatment with macitentan. Enrichment analysis revealed
that the purine metabolism pathway, as well as the arginine/proline
metabolism pathway, might be the key pathways adjusted by macitentan.
Furthermore, we verified macitentan played a beneficial role by directly
regulating the expression of arginine1 and arginine2 in the arginine/proline
metabolic pathway, and the activity of xanthine oxidase in the purine
metabolic pathway. In conclusion, this study demonstrated that macitentan
significantly ameliorated CMS in rats, and the mechanism was attributed
to the reversion of the disorder in purine and arginine/proline metabolism,
via direct regulation of XO activity and arginine1/2 expression. These
findings are expected to provide new insights into the therapeutics
and mechanism of macitentan in CMS.
The palladium-tetraethyl tetra-t-butylcalixarene-tetra(oxyacetate) complex, in the form of [NaL], exhibited high catalytic efficiency for the acylodeboronation reaction of arylboronic acids with benzoyl chloride or acetic anhydride, producing the corresponding ketones in good to excellent yields under mild reaction conditions. Various arylboronic acids, benzoyl chlorides and acetic anhydrides were tolerated in this method. Moreover, a typical method for synthesis of acetyl aryl ketones was obtained.
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