Soluble HLA in human body fluids

Soluble HLA in human body fluids

There is a growing body of information about the soluble forms of HLA in serum but there are only a few reports discussing sHLA in other body fluids. We quantitated sHLA-I and sHLA-II concentrations in sweat, saliva and tear samples from five normal individuals with known HLA-phenotypes. We also stu...

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Veröffentlicht in:Human immunology 1999-03, Vol.60 (3), p.239-244
Hauptverfasser: Aultman, Donnie, Adamashvili, Irena, Yaturu, Kamalakar, Langford, Marlyn, Gelder, Frank, Gautreaux, Michael, Ghali, G.E, McDonald, John
Format: Artikel
Sprache:eng
Schlagworte:
Disease
ELISA
Histocompatibility Antigens Class I - isolation & purification
Histocompatibility Antigens Class II - isolation & purification
HLA Antigens - cerebrospinal fluid
HLA Antigens - isolation & purification
Humans
major histocompatibility complex
Saliva - immunology
Solubility
soluble HLA Class I
soluble HLA Class II
Sweat - immunology
Tears - immunology
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Zusammenfassung:There is a growing body of information about the soluble forms of HLA in serum but there are only a few reports discussing sHLA in other body fluids. We quantitated sHLA-I and sHLA-II concentrations in sweat, saliva and tear samples from five normal individuals with known HLA-phenotypes. We also studied sweat samples from an additional 12 normal nonphenotyped subjects, as well as in CSF of 20 subjects with different illnesses, using solid phase enzyme linked immunoassay. Sweat, saliva and tears from normal subjects were found to contain very low or nondetectable amounts of sHLA-I. In contrast, sHLA-II molecules were found in each of these body fluids, although, with considerable variation between individuals. The presence of sHLA-II in saliva was further confirmed by Western-blotting. It was observed that sHLA-II having molecular mass of 43,900 and 18,100 daltons was comparable with that found in serum from normal individuals. In addition, no association of sHLA-II levels with allospecificities in either body fluid or in serum was apparent. The results of CSF sHLA concentrations in different diseases were as follows: (1) High CSF SHLA-I levels were measured during viral encephylitis ( n = 3), while none of these patients contained sHLA-II in CSF; (2) The levels of sHLA-II, but not sHLA-I were elevated in CSF of patients during seizure ( n = 6) and of patients with neonatal hepatitis (1 of 2) or with connective tissue disease accompanied with viral infection ( n = 2); (3) No CSF sHLA-I or sHLA-II could be detected at polyneuropathy ( n = 2), or in patients with syphilis ( n = 3), or leukemia ( n = 2) with evidence of neurologic involvement of central nervous system. Taken together, it may be concluded that the presence of sHLA in several body fluids is physiologically normal. It appears that sHLA-II is the predominant class of HLA molecules present in different body fluids. We propose that the system responsible for sHLA-II production in various body fluids must involve different mechanisms than those responsible for sHLA-I synthesis in serum.
ISSN:0198-8859
1879-1166
DOI:10.1016/S0198-8859(98)00122-0