Genetic Medicine

About Us
About Us
The Department of Genetic Medicine at Weill Cornell leads a dynamic and innovative translational research program, advancing diverse fields such as Genetic Therapy and Personalized Medicine.
Contact Us
News
Genetic Medicine Community
Staff & Academic Opportunities
Research
About Our Research
Our translational research program aims to leverage our expertise in genetic therapies and personalized medicine to develop clinical solutions that target the molecular causes of human diseases.
Gene Therapy and Molecular Genetics
Personalized Medicine
Clinical Trials
About Clinical Trials
The Department of Genetic Medicine advances treatments and diagnostics through diverse clinical trials, including drug testing and research to better understand diseases.
Active Trials & Recruitment
Completed Trials & Publications
Faculty & Staff
Belfer Gene Therapy Core Facility
About Our Facility
The Belfer Gene Therapy Core Facility (BGTCF) is a cutting-edge genetic medicine research facility.
BGTCF Faculty & Staff
Contact Us
Crystal Clinic

Genetic Medicine

Urinary excretion of desmosine (elastin cross-links) in subjects with PiZZ alpha-1-antitrypsin deficiency, a phenotype associated with hereditary predisposition to pulmonary emphysema.

Publication Type	Academic Article
Authors	Pelham F, Wewers M, Crystal R, Buist A, Janoff A
Journal	Am Rev Respir Dis
Volume	132
Issue	4
Pagination	821-3
Date Published	10/01/1985
ISSN	0003-0805
Keywords	Amino Acids, Desmosine, Homozygote, Pulmonary Emphysema, alpha 1-Antitrypsin Deficiency
Abstract	To evaluate the concept that lung elastin degradation is accelerated in homozygous alpha-1-antitrypsin (AAT) deficient persons, we prepared acid hydrolysates of urine and used a radioimmunoassay for desmosine to measure urine concentrations of this elastin-specific cross-link in such persons and in control subjects. Excretion of desmosine in 17 homozygous AAT-deficient (PiZZ) patients with emphysema was compared with that in 27 patients with interstitial lung diseases (16 sarcoid, 5 idiopathic pulmonary fibrosis, 6 other interstitial lung diseases) and 26 healthy subjects. Both smokers and nonsmokers were present in all groups. Urinary desmosine concentration (microgram/100 mg creatinine) was 2.35 +/- 0.93 in the PiZZ patients, 2.49 +/- 1.01 in those with interstitial lung disease, and 2.05 +/- 0.54 in the healthy control subjects (p greater than 0.1, all comparisons). Because abnormal pulmonary elastolysis may be largely completed before symptoms of emphysema develop in AAT-deficient persons, we also tested 6 asymptomatic adults with homozygous AAT deficiency (PiZZ) and 5 PiZZ children. Urine desmosine (microgram/100 mg creatinine) was not significantly elevated in either group compared with that in the age-matched control subjects, although children (PiZZ and age-matched controls) showed higher excretions than did adults (6 asymptomatic PiZZ adults, 2.60 +/- 0.91; 5 PiZZ children, 3.27 +/- 0.62; 10 control children, 3.61 +/- 0.62). These data suggest that pathologic lung elastolysis in the PiZZ subject may constitute too small a fraction of total-body elastin turnover to be detected by this method.(ABSTRACT TRUNCATED AT 250 WORDS)
DOI	10.1164/arrd.1985.132.4.821
PubMed ID	3876794