Nguyen Thi Ngoc Dao scite author profile

Nguyen Thi Ngoc Dao

5Publications

56Citation Statements Received

71Citation Statements Given

How they've been cited

153

How they cite others

Affiliations

Institute of Mathematics

Publications

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Release of Vasoactive Substances from Guinea-Pig Lungs by Slow-Reacting Substance C and Arachidonic Acid

Vargäftig¹,

Dao²

1971

Pharmacology

108

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Arachidonic acid and ‘slow-reacting substance C, perfused through isolated guinea-pig lungs, release a ‘rabbit aorta contracting substance C (RCS-C), indistinguishable from a RCS released under similar conditions by anaphylaxis, bradykinin and ‘slow-reacting substance A’. Release of RCS-C is blocked by previous perfusion of the lungs with aspirin or phenylbutazone. A role for ‘rabbit aorta contracting substances’, released during inflammation by a cascade of events initially evoked by phospholipase A activation, is suggested.

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Unequal Crossing-Over between Aldosterone Synthase and 11β-Hydroxylase Genes Causes Congenital Adrenal Hyperplasia

Hampf

Dao

Hoan

et al. 2001

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Congenital adrenal hyperplasia is one of the most frequently inherited diseases. It is characterized by a severe decline in cortisol secretion, which results in a compensatory increase in ACTH and consequent adrenal growth (hyperplasia). Here we describe the first case of 11beta-hydroxylase deficiency that is caused by an unequal cross-over of the genes encoding aldosterone synthase (CYP11B2) and 11beta-hydroxylase (CYP11B1). CYP11B1 and CYP11B2 are located on chromosome 8q24 approximately 45 kb apart from each other. The investigated genetic recombination deleted the normal alleles of the two genes and created a chimeric fusion gene, which consists of the promotor and exons 1 through 4 of the aldosterone synthase gene plus intron 4 through exon 9 of the 11beta-hydroxylase gene. This recombination event subordinates any remaining 11beta-hydroxylase activity of the chimeric enzyme to the control mechanisms of CYP11B2, the expression of which is mainly regulated by angiotensin II and K(+). Normally the 11beta-hydroxylase activity is controlled by ACTH. The existence of the CYP11B2/CYP11B1 chimera was discovered by means of a PCR method and was confirmed with a Southern blot. Furthermore, by applying a minigene expression method we demonstrated a point mutation in intron 3 (IVS3+16G-->T) of the patient's second 11beta-hydroxylase allele that radically diminishes proper splicing of the pre-mRNA by giving rise to a new, highly preferred donor splice site.

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Antagonism by anti-inflammatory drugs of tissue slow reacting substance C

Vargäftig¹,

Dao²

1970

Pharmacological Research Communications

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New Molecular Genetic Defects Causing 11β-Hydroxylase Deficiency (CAH)

Hampf¹,

Dao

Hoan

et al. 2000

Endocrine Research

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Purification and identification of some characters of the fibrinolytic enzyme isolated from the earthwom Perionyx excavatus

Thủy¹,

Tuyến²,

Dao³

2014

V J Bio

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