Cytoplasmic sulfate for sulfation reactions may be derived either from extracellular fluids or from catabolism of sulfur-containing amino acids and other thiols. In vitro studies have pointed out the potential relevance of sulfur-containing amino acids as sources for sulfation when extracellular sulfate concentration is low or when its transport is impaired such as in DTDST [DTD (diastrophic dysplasia) sulfate transporter] chondrodysplasias. In the present study, we have considered the contribution of cysteine and cysteine derivatives to in vivo macromolecular sulfation of cartilage by using the mouse model of DTD we have recently generated [Forlino, Piazza, Tiveron, Della Torre, Tatangelo, Bonafe, Gualeni, Romano, Pecora, Superti-Furga et al. (2005) Hum. Mol. Genet. 14, 859–871]. By intraperitoneal injection of [35S]cysteine in wild-type and mutant mice and determination of the specific activity of the chondroitin 4-sulfated disaccharide in cartilage, we demonstrated that the pathway by which sulfate is recruited from the intracellular oxidation of thiols is active in vivo. To check whether cysteine derivatives play a role, sulfation of cartilage proteoglycans was measured after treatment for 1 week of newborn mutant and wild-type mice with hypodermic NAC (N-acetyl-L-cysteine). The relative amount of sulfated disaccharides increased in mutant mice treated with NAC compared with the placebo group, indicating an increase in proteoglycan sulfation due to NAC catabolism, although pharmacokinetic studies demonstrated that the drug was rapidly removed from the bloodstream. In conclusion, cysteine contribution to cartilage proteoglycan sulfation in vivo is minimal under physiological conditions even if extracellular sulfate availability is low; however, the contribution of thiols to sulfation becomes significant by increasing their plasma concentration.
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Research Article|
August 29 2006
In vivo contribution of amino acid sulfur to cartilage proteoglycan sulfation Available to Purchase
Fabio Pecora;
Fabio Pecora
*Dipartimento di Biochimica ‘Alessandro Castellani’, Università di Pavia, via Taramelli 3/B, I-27100 Pavia, Italy
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Benedetta Gualeni;
Benedetta Gualeni
*Dipartimento di Biochimica ‘Alessandro Castellani’, Università di Pavia, via Taramelli 3/B, I-27100 Pavia, Italy
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Antonella Forlino;
Antonella Forlino
*Dipartimento di Biochimica ‘Alessandro Castellani’, Università di Pavia, via Taramelli 3/B, I-27100 Pavia, Italy
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Andrea Superti-Furga;
Andrea Superti-Furga
†Center for Pediatrics and Adolescent Medicine, Freiburg University Hospital, Mathildenstr. 1, D-79106 Freiburg, Germany
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Ruggero Tenni;
Ruggero Tenni
*Dipartimento di Biochimica ‘Alessandro Castellani’, Università di Pavia, via Taramelli 3/B, I-27100 Pavia, Italy
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Giuseppe Cetta;
Giuseppe Cetta
*Dipartimento di Biochimica ‘Alessandro Castellani’, Università di Pavia, via Taramelli 3/B, I-27100 Pavia, Italy
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Antonio Rossi
Antonio Rossi
1
*Dipartimento di Biochimica ‘Alessandro Castellani’, Università di Pavia, via Taramelli 3/B, I-27100 Pavia, Italy
1To whom correspondence should be addressed (email [email protected]).
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Publisher: Portland Press Ltd
Received:
April 13 2006
Revision Received:
May 23 2006
Accepted:
May 23 2006
Accepted Manuscript online:
May 23 2006
Online ISSN: 1470-8728
Print ISSN: 0264-6021
The Biochemical Society, London
2006
Biochem J (2006) 398 (3): 509–514.
Article history
Received:
April 13 2006
Revision Received:
May 23 2006
Accepted:
May 23 2006
Accepted Manuscript online:
May 23 2006
Citation
Fabio Pecora, Benedetta Gualeni, Antonella Forlino, Andrea Superti-Furga, Ruggero Tenni, Giuseppe Cetta, Antonio Rossi; In vivo contribution of amino acid sulfur to cartilage proteoglycan sulfation. Biochem J 15 September 2006; 398 (3): 509–514. doi: https://doi.org/10.1042/BJ20060566
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