Hisato Sakamoto scite author profile

To determine the immunolocalization of ClC-5 in the mouse kidney, we developed a ClC-5-specific rat monoclonal antibody. Immunoblotting demonstrated an 85-kDa band of ClC-5 in the kidney and ClC-5 transfected cells. Immunocytochemistry revealed significant labeling of ClC-5 in brush-border membrane and subapical intracellular vesicles of the proximal tubule. In addition, apical and cytoplasmic staining was observed in the type A intercalated cells in the cortical collecting duct. In contrast, the staining was minimal in the outer and inner medullary collecting ducts and the thick ascending limb. Western blotting of vesicles immunoisolated by the ClC-5 antibody showed the presence of H+-ATPase, strongly indicating that these two proteins were present in the same membranes. Double labeling with antibodies against ClC-5 and H+-ATPase and analysis by confocal images showed that ClC-5 and H+-ATPase colocalized in these ClC-5-positive cells. These findings suggest that ClC-5 might be involved in the endocytosis and/or the H+ secretion in the proximal tubule cells and the cortical collecting duct type A intercalated cells in mouse kidney.

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Identification of an acid-activated Cl⁻ channel from human skeletal muscles

Kawasaki

Fukuma

Yamauchi

et al. 1999

American Journal of Physiology-Cell Physiology

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ClC-4 gene was isolated as a putative Cl(-) channel. Due to a lack of functional expression of ClC-4, its physiological role remains unknown. We isolated a human ClC-4 clone (hClC-4sk) from human skeletal muscles and stably transfected it to Chinese hamster ovary cells. Whole cell patch-clamp studies showed that the hClC-4sk channel was activated by external acidic pH and inhibited by DIDS. It passed a strong outward Cl(-) current with a permeability sequence of I(-) > Cl(-) > F(-). The hClC-4sk has consensus sites for phosphorylation by protein kinase A (PKA); however, stimulation of PKA had no effect on the currents. hClC-4sk mRNA was expressed in excitable tissues, such as heart, brain, and skeletal muscle. These functional characteristics of hClC-4sk provide a clue to its physiological role in excitable cells.

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Identification of a New Outwardly Rectifying Cl− Channel That Belongs to a Subfamily of the ClC Cl− Channels

Sakamoto

Kawasaki

Uchida

et al. 1996

Journal of Biological Chemistry

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A new outwardly rectifying Cl- channels (ORCC) that belongs to ClC Cl- channel family has been identified from rat kidney and designated as ClC-5. ClC-5 cDNA encodes a polypeptide of 746 amino acids, which is indicated by hydrophobicity analysis to have structural features that are common of the ClC family. However, the amino acid sequence was weakly homologous to those of other ClC Cl- channels except for ClC-3, which we recently identified as a Ca2+-sensitive ORCC. Northern blot analysis of rat tissues showed that ClC-5 mRNA was predominantly expressed in the kidney and colon. To characterize the functional properties of ClC-5 by whole cell patch-clamp technique, we established the stably transfected CHO-K1 cell line using intranuclear microinjection technique. The transfected cells induced outwardly rectifying and 4,4'-diisothiocyanostilbene-2,2'-disulfonic acid-sensitive Cl- currents on whole cell configuration. Following the identification of two highly homologous ORCCs, ClC-3 and ClC-5, a new subfamily encoding ORCC has emerged in the ClC family. Furthermore, ClC-5 was almost identical to a partial sequence of human cDNA that is related to Dent's disease. The molecular structure and functional properties of ClC-5 will provide an important insight into ORCCs and the pathogenesis of Dent's disease.

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Effective Antibiotic Treatment of Methicillin-Resistant <i>Staphylococcus aureus</i>-Associated Glomerulonephritis

Nagaba

Hiki

Aoyama

et al. 2002

Nephron

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Background: A new type of glomerulonephritis following a methicillin-resistant Staphylococcus aureus (MRSA) infection has been reported. The purpose of this study is to elucidate the clinicopathological features and the responsiveness to treatment of the disease. Methods: We studied the treatment of 8 patients with glomerulonephritis related to MRSA infection. We observed the eight cases and analyzed clinical features, laboratory findings and histopathological data. Results: On admission, all patients had no renal abnormalities. One to four months after suffering from MRSA infection, severe proteinuria and hematuria developed. Renal biopsy specimens revealed moderate to severe mesangial proliferative glomerulonephritis with various degrees of crescent formation. Immunofluorescence studies showed IgA and C3. Antibiotic therapy was performed in six cases, resulting in successfully reducing the proteinuria in parallel with the decreased activity of MRSA infection in five cases. The other 2 cases received corticosteroid treatment after complete cessation of MRSA infection, but they had a relapse of MRSA infection and later died from sepsis. Conclusions: These results suggested that MRSA-associated glomerulonephritis might respond to antibiotic treatment in most cases. This also indicated that special care must be taken in the application of steroid therapy for the glomerulonephritis with crescents, even though the MRSA infection has gone into an inactive state.

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A highly sensitive radioimmunoassay of atrial natriuretic peptide (ANP) in human plasma and urine

Marumo

Sakamoto

Ando

et al. 1986

Biochemical and Biophysical Research Communications

104

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Hisato Sakamoto

Cellular and subcellular immunolocalization of ClC-5 channel in mouse kidney: colocalization with H⁺-ATPase

Identification of an acid-activated Cl⁻ channel from human skeletal muscles

Identification of a New Outwardly Rectifying Cl− Channel That Belongs to a Subfamily of the ClC Cl− Channels

Effective Antibiotic Treatment of Methicillin-Resistant <i>Staphylococcus aureus</i>-Associated Glomerulonephritis

A highly sensitive radioimmunoassay of atrial natriuretic peptide (ANP) in human plasma and urine

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Product

Resources

About

Hisato Sakamoto

Cellular and subcellular immunolocalization of ClC-5 channel in mouse kidney: colocalization with H+-ATPase

Identification of an acid-activated Cl− channel from human skeletal muscles

Identification of a New Outwardly Rectifying Cl− Channel That Belongs to a Subfamily of the ClC Cl− Channels

Effective Antibiotic Treatment of Methicillin-Resistant <i>Staphylococcus aureus</i>-Associated Glomerulonephritis

A highly sensitive radioimmunoassay of atrial natriuretic peptide (ANP) in human plasma and urine

Contact Info

Product

Resources

About

Cellular and subcellular immunolocalization of ClC-5 channel in mouse kidney: colocalization with H⁺-ATPase

Identification of an acid-activated Cl⁻ channel from human skeletal muscles