Glucocorticoid regulation and glycosylation of mouse intestinal type IIb Na-P<sub>i</sub>cotransporter during ontogeny

Arima, Kayo; Hines, Eric R.; Kiela, Pawel R.; Drees, Jason B.; Collins, James F.

doi:10.1152/ajpgi.00319.2001

Cited by 67 publications

(55 citation statements)

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“…Tissue sections (6-10 m) from both tissues were prepared by the Histopathology Core Service at the University of Arizona (Tucson, AZ). Immunohistochemical staining and detection was performed as previously described (2). NaPi-IIb antiserum was reacted with sections for 60 min at a 1:500 (for intestinal sections) or a 1:4,000 (for lung sections) dilution in PBS.…”

Section: Methodsmentioning

confidence: 99%

“…Intestinal Pi absorption through the NaPi-IIb cotransporter is regulated by various physiological effectors. Epidermal growth factor (EGF) and glucocorticoids inhibit intestinal sodium-dependent Pi (Na/Pi) absorption and NaPi-IIb gene expression (2,31), whereas 1,25(OH) 2 vitamin D 3 and dietary Pi deprivation stimulate intestinal Na/Pi absorption and NaPi-IIb gene expression (17,30).…”

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confidence: 99%

“…Estrogen is involved not only in the regulation of Ca 2ϩ absorption (3,13) but also in the maintenance of bone density (3,8) and in the modulation of 1,25(OH) 2 vitamin D 3 synthesis (4,8,20,23,27). Although 1,25(OH) 2 vitamin D 3 is known to regulate intestinal Pi absorption, there is no evidence to date demonstrating estrogen regulation via NaPi-IIb cotransporter expression. Thus the current studies were designed to investigate the possible link between estrogen and intestinal NaPi-IIb gene expression.…”

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confidence: 99%

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Regulation of intestinal NaPi-IIb cotransporter gene expression by estrogen

Uno

Inouye

et al. 2003

American Journal of Physiology-Gastrointestinal and Liver Physi

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The current experiments were designed to study the effect of β-estradiol on type IIb sodium-coupled phosphate (NaPi-IIb) cotransporter gene expression. Uptake studies with intestinal brush-border membrane vesicles (BBMV) showed that estrogen treatment increased sodium-dependent phosphate absorption by ∼45% in rat intestine. Northern blot analysis indicated that NaPi-IIb mRNA expression was increased by ∼50% after estrogen treatment. Western blot analysis also detected an increase in BBMV NaPi-IIb protein expression in estrogen-treated rats. In human intestinal Caco-2 cells, NaPi-IIb mRNA abundance was increased ∼60% after estrogen treatment, and this increase could be abolished by inhibition of gene transcription. Transfection studies with human NaPi-IIb promoter reporter constructs showed that the promoter was responsive to estrogen treatment. These studies demonstrate for the first time that estrogen stimulates intestinal sodium-dependent phosphate absorption in female rats. This stimulation is associated with increased NaPi-IIb mRNA and protein expression. Thus the effect of estrogen on intestinal Pi absorption may be partially due to activation of NaPi-IIb gene transcription.

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Section: Methodsmentioning

confidence: 99%

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confidence: 99%

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Regulation of intestinal NaPi-IIb cotransporter gene expression by estrogen

Uno

Inouye

et al. 2003

American Journal of Physiology-Gastrointestinal and Liver Physi

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“…Type II Na ϩ -P i cotransporters (NaPi-II) are largely responsible for renal and intestinal transport of P i in the human body, with the IIa and IIb isoforms being most important in the kidney and intestine, respectively. The NaPiIIa cotransporter is localized on the brush-border membrane of the renal proximal tubules and is regulated by dietary P i levels (6,28,30), parathyroid hormone (15,21), and 1,25(OH) 2 -vitamin D 3 (27). The NaPi-IIb cotransporter is localized on the apical membrane of intestinal enterocytes and is also regulated by dietary P i levels and vitamin D 3 (11,12,32).…”

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“…In addition, recent studies have shown that other physiological factors influence intestinal P i uptake by altering NaPi-IIb cotransporter gene expression. For example, EGF and glucocorticoids decrease NaPi-IIb gene expression, which corresponds to a decrease in intestinal Na-dependent P i absorption (3,34). Conversely, vitamin D 3 (11,32) and estrogen (36) stimulate NaPiIIb gene expression, which corresponds to an increase in intestinal Na-dependent P i absorption.…”

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confidence: 99%

NF1 transcriptional factor(s) is required for basal promoter activation of the human intestinal NaPi-IIb cotransporter gene

Uno

Inouye

et al. 2005

American Journal of Physiology-Gastrointestinal and Liver Physi

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. NF1 transcriptional factor(s) is required for basal promoter activation of the human intestinal NaPi-IIb cotransporter gene. Am J Physiol Gastrointest Liver Physiol 288: G175-G181, 2005; First published September 30, 2004; doi:10.1152/ ajpgi.00396.2004.-The human intestinal type IIb Na ϩ -Pi cotransporter (hNaPi-IIb) gene promoter lacks a TATA box and has a high GC content in the 5Ј-flanking region. To understand the mechanism of hNaPi-IIb gene transcription, the current study was performed to characterize the minimal promoter region and transcriptional factor(s) necessary to activate gene expression in human intestinal cells . With the use of progressively shorter promoter constructs, a minimal promoter extending from bp Ϫ58 to ϩ15 was identified and shown to direct high levels of hNaPi-IIb cotransporter expression in Caco-2 cells. Gel mobility shift assays (GMSAs) indicated that two regions could be bound by nuclear proteins from Caco-2 cells: region A at bp Ϫ26/Ϫ23 and region B at bp Ϫ44/Ϫ35. The introduction of mutations in region A abolished promoter activity, whereas mutations in region B had no effect. Deletion mutants of the same regions showed identical results. Furthermore, DNase I footprinting experiments confirmed the observation made by GMSAs. Additional studies, which used a specific nuclear factor 1 (NF1) antiserum, demonstrated that NF1 protein(s) binds to the minimal promoter at region A. These results indicated that the NF1 protein(s) is required to activate the basal transcription of hNaPi-IIb gene under normal growth conditions. This study has thus identified a new target gene in the small intestinal epithelium that is directly regulated by NF1 transcriptional factor(s).type IIb sodium-phosphate cotransporter; Slc34a2; Caco-2 cells; nuclear factor 1 REGULATION OF P i homeostasis is vital for maintaining optimal physiological conditions for body development and maintenance of bone health. Type II Na ϩ -P i cotransporters (NaPi-II) are largely responsible for renal and intestinal transport of P i in the human body, with the IIa and IIb isoforms being most important in the kidney and intestine, respectively. The NaPiIIa cotransporter is localized on the brush-border membrane of the renal proximal tubules and is regulated by dietary P i levels (6, 28, 30), parathyroid hormone (15, 21), and 1,25(OH) 2 -vitamin D 3 (27). The NaPi-IIb cotransporter is localized on the apical membrane of intestinal enterocytes and is also regulated by dietary P i levels and vitamin D 3 (11,12,32). In addition, recent studies have shown that other physiological factors influence intestinal P i uptake by altering NaPi-IIb cotransporter gene expression. For example, EGF and glucocorticoids decrease NaPi-IIb gene expression, which corresponds to a decrease in intestinal Na-dependent P i absorption (3, 34). Conversely, vitamin D 3 (11,32) and estrogen (36) stimulate NaPiIIb gene expression, which corresponds to an increase in intestinal Na-dependent P i absorption.We recently (34) cloned the human NaPi-IIb (hNaPi-IIb) ...

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Mechanisms and Regulation of Intestinal Phosphate Absorption

Hernando¹,

Wagner²

2018

Comprehensive Physiology

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States of hypo- and hyperphosphatemia have deleterious consequences including rickets/osteomalacia and renal/cardiovascular disease, respectively. Therefore, the maintenance of appropriate plasma levels of phosphate is an essential requirement for health. This control is executed by the collaborative action of intestine and kidney whose capacities to (re)absorb phosphate are regulated by a number of hormonal and metabolic factors, among them parathyroid hormone, fibroblast growth factor 23, 1,25(OH) vitamin D , and dietary phosphate. The molecular mechanisms responsible for the transepithelial transport of phosphate across enterocytes are only partially understood. Indeed, whereas renal reabsorption entirely relies on well-characterized active transport mechanisms of phosphate across the renal proximal epithelia, intestinal absorption proceeds via active and passive mechanisms, with the molecular identity of the passive component still unknown. The active absorption of phosphate depends mostly on the activity and expression of the sodium-dependent phosphate cotransporter NaPi-IIb (SLC34A2), which is highly regulated by many of the factors, mentioned earlier. Physiologically, the contribution of NaPi-IIb to the maintenance of phosphate balance appears to be mostly relevant during periods of low phosphate availability. Therefore, its role in individuals living in industrialized societies with high phosphate intake is probably less relevant. Importantly, small increases in plasma phosphate, even within normal range, associate with higher risk of cardiovascular disease. Therefore, therapeutic approaches to treat hyperphosphatemia, including dietary phosphate restriction and phosphate binders, aim at reducing intestinal absorption. Here we review the current state of research in the field. © 2017 American Physiological Society. Compr Physiol 8:1065-1090, 2018.

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Glucocorticoid regulation and glycosylation of mouse intestinal type IIb Na-P_icotransporter during ontogeny

Cited by 67 publications

References 45 publications

Regulation of intestinal NaPi-IIb cotransporter gene expression by estrogen

Regulation of intestinal NaPi-IIb cotransporter gene expression by estrogen

NF1 transcriptional factor(s) is required for basal promoter activation of the human intestinal NaPi-IIb cotransporter gene

Mechanisms and Regulation of Intestinal Phosphate Absorption

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Glucocorticoid regulation and glycosylation of mouse intestinal type IIb Na-Picotransporter during ontogeny

Cited by 67 publications

References 45 publications

Regulation of intestinal NaPi-IIb cotransporter gene expression by estrogen

Regulation of intestinal NaPi-IIb cotransporter gene expression by estrogen

NF1 transcriptional factor(s) is required for basal promoter activation of the human intestinal NaPi-IIb cotransporter gene

Mechanisms and Regulation of Intestinal Phosphate Absorption

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Glucocorticoid regulation and glycosylation of mouse intestinal type IIb Na-P_icotransporter during ontogeny