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Differentiation of sarcoidosis from tuberculosis by use of electron capture gas-liquid chromatography
Authors:P L Almenoff  J B Brooks  A Johnson  M Lesser
Institution:(1) Division of Pulmonary/Critical Care Medicine, Mount Sinai School of Medicine, 10029 New York;(2) Pulmonary/Critical Care Medicine Section, Veterans Affairs Medical Center, 10468 Bronx, New York;(3) Division of AIDS, STD, TB Laboratory Research, Tuberculosis/Mycobacteriology Branch, National Center for Infectious Diseases, 30333 Atlanta, Georgia;(4) Medical Research, Veterans Affairs Medical Center, Hampton, Virginia, USA;(5) Present address: Pulmonary/Critical Care, VA Medical Center, 130 West Kingsbridge Rd., 10468 Bronx, KY, USA
Abstract:To explore further the possible etiologic role of mycobacteria in the development of sarcoidosis, we measured free, nonbound tuberculostearic acid (TSA, 10-methyloctadecanoic), a component of mycobacteria, in the sera of subjects with sarcoidosis or active untreated pulmonary tuberculosis and in healthy controls by use of frequency-pulsed electron capture gas-liquid chromatography (FPEC-GLC). The selective analytic system is capable of measuring as little as 15-fmol quantities of free, nonbound TSA in serum and cerebral spinal fluid. We found that TSA was present in the sera of all subjects with Mycobacterium tuberculosis (n = 10) but was undetectable in subjects with sarcoidosis (n = 15) and in healthy controls (n = 15), thereby suggesting that if sarcoidosis is caused by a mycobacterial organism, TSA is not produced or does not gain access to the systemic circulation in quantities sufficient for measurement. However, in the course of the studies we found that a peak, designated p11, was elevated in the sera of all subjects with acute sarcoidosis (n = 4). Also, a peak designated p3 was reduced significantly in all subjects with acute and chronic sarcoidosis and absent in subjects with M. tuberculosis compared with healthy controls. Both peaks were later shown by chemical analysis and mass spectral studies to be carboxylic acids not previously associated with specific disease entities. Follow-up detailed studies will be needed to determine if quantitation of these unique carboxylic acids will be useful in differentiating sarcoidosis from other disorders.
Keywords:Sarcoidosis  Tuberculosis  TSA  FPEC  GLC
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