Defective cellular trafficking of missense NPR-B mutants is the major mechanism underlying Acromesomelic Dysplasia type Maroteaux

doi:10.1093/hmg/ddn354

Human Molecular Genetics Advance Access published online on October 22, 2008
Human Molecular Genetics, doi:10.1093/hmg/ddn354

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Defective cellular trafficking of missense NPR-B mutants is the major mechanism underlying Acromesomelic Dysplasia type Maroteaux

Alistair N. Hume³, Jens Buttgereit⁴^,5, Aydah M. Al-Awadhi¹, Sarah S. Al-Suwaidi¹, Anne John¹, Michael Bader⁴, Miguel C. Seabra³, Lihadh Al-Gazali² and Bassam R. Ali¹^,*

¹ Department of Pathology ² Department of Pediatrics, Faculty of Medicine and Health Sciences, United Arab Emirates University, Al-Ain, United Arab Emirates ³ Molecular Medicine, National Heart and Lung Institute, Imperial College London, London SW7 2AZ, UK ⁴ Max Delbrück Centrum for Molecular Medicine, Berlin-Buch, Berlin, Germany ⁵ Medical Faculty of the Charité, Experimental and Clinical Research Center, Franz-Volhard-Clinic, Berlin, Germany

^* Correspondence should be addressed to: Dr. Bassam R. Ali; Department of Pathology, Faculty of Medicine and Health Sciences, UAE University, P.O. Box 17666, Al-Ain, United Arab Emirates. Tel. +971 3 7137470 Fax. +971 3 7671966 E.Mail. bassam.ali{at}uaeu.ac.ae or br_ali{at}hotmail.com

Received July 12, 2008; Revised October 9, 2008; Accepted October 20, 2008

The natriuretic peptides (NPs) comprise a family of structurallyrelated but genetically distinct hormones that regulate a varietyof physiological processes such as cardiac growth, blood pressure,axonal path-finding and endochondral ossification leading tothe formation of vertebrae and long bones. The biological actionsof NP are mediated by natriuretic peptide receptors (NPRs) –A,-B and -C that are located on the cell surface. Mutations inNPR-B have been shown to cause Acromesomelic Dysplasia typeMaroteaux (AMDM), a growth disorder in humans and severe dwarfismin mice. We hypothesized that missense mutations of NPR-B associatedwith AMDM primarily affect NPR-B function by the arrest of receptortrafficking at the ER, due to conformational change, ratherthan an impairment of ligand binding, transmission of signalthrough the membrane or catalytic activity. Twelve missensemutations found in AMDM patients and cn/cn mice were generatedby site-directed mutagenesis and transiently over-expressedin HeLa cells. Confocal microscopy revealed that 11 out of 12mutants were retained in the ER. Determination of the ligand-dependentcGMP response confirmed that ER-retained NPR-B mutants are non-functional.Meanwhile the only cell surface targeted NPR-B missense mutant(D176E) displayed greatly reduced enzymatic activity due toimpaired ligand binding. Thus in the majority of cases of AMDMassociated with missense NPR-B mutation, disease appears toresult from defects in targeting of the ER receptor to the plasmamembrane.

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