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Literature DB >> 4127163

A hereditary alteration in kidneys of mice with Chediak-Higashi syndrome.

Abstract

The beige mouse is considered to be a homologue of Chediak-Higashi syndrome (CHS). Cytochemical and electron microscopic studies have revealed an inherited lesion in the kidneys of these mice. The alteration was confined to the distal segments (S3) of the proximal tubules and was characterized by the accumulation of numerous massive polysaccharide-rich granules. These granules were reactive for acid phosphatase and beta-glucuronidase activities and were therefore considered to be lysosomes. Small numbers of lymphocytes were also observed in the perivascular spaces and within the tubules of the S3 segment. The fine structure of S3 cells was also markedly altered. In addition to the massive lysosomes, dense material was found associated with the brush border and was present in pinocytotic vesicles at the base of the brush border and between basal invaginations of the plasma membranes. Despite these changes, reabsorption of exogeneous peroxidase by S3 cells appeared to be normal. The presence of a congenital defect in the kidney of the beige mouse appears to provide a useful model for studying the morphology and function of the S3 region of the nephron.

Entities: Chemical Disease Gene Species

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Year: 1973 PMID： 4127163 PMCID： PMC1904055

Source DB: PubMed Journal: Am J Pathol ISSN： 0002-9440 Impact factor: 4.307

22 in total

1. The Chediak-Higashi syndrome: studies in four patients and a review of the literature.

Authors: R S Blume; S M Wolff
Journal: Medicine (Baltimore) Date: 1972-07 Impact factor: 1.889

2. Ultrastructure of cells in bone marrow and peripheral blood of normal mink and mink with the homologue of the Chediak-Higashi trait of humans. II. Cytoplasmic granules in eosinophils, basophils, mononuclear cells and platelets.

Authors: W C Davis; S S Spicer; W B Greene; G A Padgett
Journal: Am J Pathol Date: 1971-06 Impact factor: 4.307

3. Observations on the segmentation of the proximal tubule in the rat kidney. Comparison of results from phase contrast, fluorescence and electron microscopy.

Authors: A B Maunsbach
Journal: J Ultrastruct Res Date: 1966-10

4. The influence of different fixatives and fixation methods on the ultrastructure of rat kidney proximal tubule cells. I. Comparison of different perfusion fixation methods and of glutaraldehyde, formaldehyde and osmium tetroxide fixatives.

Authors: A B Maunsbach
Journal: J Ultrastruct Res Date: 1966-06

5. Characterization and significance of abnormal leukocyte granules in the beige mouse: a possible homologue for Chediak-Higashi Aleutian trait.

Authors: J M Bennett; R S Blume; S M Wolff
Journal: J Lab Clin Med Date: 1969-02

6. Giant granules and widespread cytoplasmic inclusions in a genetic syndrome of Aleutian mink. An electron microscopic study.

Authors: M A Lutzner; J H Tierney; E P Benditt
Journal: Lab Invest Date: 1965-12 Impact factor: 5.662

A hereditary alteration in kidneys of mice with Chediak-Higashi syndrome.

1. The Chediak-Higashi syndrome: studies in four patients and a review of the literature.

2. Ultrastructure of cells in bone marrow and peripheral blood of normal mink and mink with the homologue of the Chediak-Higashi trait of humans. II. Cytoplasmic granules in eosinophils, basophils, mononuclear cells and platelets.

3. Observations on the segmentation of the proximal tubule in the rat kidney. Comparison of results from phase contrast, fluorescence and electron microscopy.

4. The influence of different fixatives and fixation methods on the ultrastructure of rat kidney proximal tubule cells. I. Comparison of different perfusion fixation methods and of glutaraldehyde, formaldehyde and osmium tetroxide fixatives.

5. Characterization and significance of abnormal leukocyte granules in the beige mouse: a possible homologue for Chediak-Higashi Aleutian trait.

6. Giant granules and widespread cytoplasmic inclusions in a genetic syndrome of Aleutian mink. An electron microscopic study.

7. Giant granules in leukocytes of the beige mouse.

8. Defective function of renal lysosomes in mice with the Chediak-Higashi syndrome.

9. Distribution of peroxisomes (microbodies) in the nephron of the rat: a cytochemical study.

10. The fine structural localization of endogenous and exogenous peroxidase activity in Kupffer cells of rat liver.

1. Characterization of lysosomes and lysosomal enzymes from Chediak-Higashi-syndrome cultured fibroblasts.

2. Turnover of kidney beta-glucuronidase in normal and Chédiak-Higashi (beige) mice.

3. Mast cell degranulation in beige mice with the Chédiak-Higashi defect.

4. Alterations in the proximal nephron of beige mice with the Chédiak-Higashi syndrome.

5. Giant dense bodies in fibroblasts cultured from beige mice with the Chédiak-Higashi syndrome.

6. Fate of exogenous peroxidase in renal lysosomes of mice with Chediak-Higashi syndrome.

7. Defective lysosomal enzyme secretion in kidneys of Chediak-Higashi (beige) mice.