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Pregled bibliografske jedinice broj: 194862

Immunotherapeutic potential of peptidoglycan-monomer linked with zinc in old mice


Mrakovčić-Šutić, Ines; Jakovac, Hrvoje; Grebić, Damir; Radošević-Stašić, Biserka
Immunotherapeutic potential of peptidoglycan-monomer linked with zinc in old mice // The international journal of artificial organs, 28 (2005), 4; 400-400 (podatak o recenziji nije dostupan, kongresno priopcenje, znanstveni)


CROSBI ID: 194862 Za ispravke kontaktirajte CROSBI podršku putem web obrasca

Naslov
Immunotherapeutic potential of peptidoglycan-monomer linked with zinc in old mice

Autori
Mrakovčić-Šutić, Ines ; Jakovac, Hrvoje ; Grebić, Damir ; Radošević-Stašić, Biserka

Izvornik
The international journal of artificial organs (0391-3988) 28 (2005), 4; 400-400

Vrsta, podvrsta i kategorija rada
Radovi u časopisima, kongresno priopcenje, znanstveni

Ključne riječi
peptidoglycan-monomer with Zn ; very old mice ; liver ; spleen ; YAC-1 ; syngeneic thymocytes

Sažetak
Although different theories try to explain the aging process, it is generally accepted that there is a correlation between the aging and the accumulation of oxidatively damaged proteins, lipids and nucleic acids, as well as reactive nitrogen species (RNS), which are widely implicated in the inflammatory process and responsible for a variety of age-related dysfunction. The elimination of deleterious effects of ROS/RNS are dependent on their concentration and the microenvironment in which ROS/RNS are released, while in the processes of the recognition and elimination of potentially harmful altered macromolecules, and general coping with stress are involved the cells of innate and adaptive immune system. Owing to the presence of immunosenescence in elderly and our previous findings that peptidoglycan monomer (PGM), originally prepared by biosynthesis from culture fluids of Gram (+) Brevibacterium divaricatum and its new analog PGM-Zn have marked immunocorrective and hepatoprotective properties in experimental models of immunodeficiency (halothane anesthesia and obstructive jaundice) in this study we attempted to investigate the effects of in vivo application of PGM-Zn in very old mice (aged 2 years) estimating the phenotypic and functional characteristic of intrahepatic and splenic mononuclear lymphatic cells (MNLC), and comparing the data with similarly treated young (2 month old) C57BL6 mice. For this purpose both age groups of mice were treated during the 6 days (every second day) with 3 injections of PGM-Zn (10 mg/kg i.p.) or with the same amount of the solvent. Two days after the last injection, the phenotype of lymphatic cells was determined by FACS staining, and the spontaneous cytotoxic activity of freshly isolated intrahepatic and splenic MNLC was measured against NK-sensitive (YAC-1) and against NKT-sensitive targets (syngeneic thymocytes). The results have shown that in the control-old mice very significant changes occur particularly in the liver. Thus, the proportion of intrahepatic CD3+, CD8+, CD122+ (IL-2Rb+) and CD3+/CD122+ cells was found to be significantly greater, and the proportion of NK1.1+ cells lower than in the control-young mice. Treatment with PGM-Zn in both age groups significantly increased the proportion of NK1.1+, CD69+ and CD3+/NK1.1+ cells, but this increase was less expressed in very old mice. On the contrary, PGM-Zn in old mice markedly decreased the percentage of hepatic CD8+ T cells, and CD122+ NKT cells. Similar changes were not found in the spleen, where, in the control-old group was found a significantly less proportion of CD8+ cells and a greater inhibitory effects of PGM-Zn on CD19+ cells. Simultaneously, we noticed that hepatic MNLCs obtained from control-very old mice were markedly less cytotoxic against YAC-1 than those obtained from young mice (p<0.0001). Splenic MNLC obtained from very old mice in comparison to “ young” cells were, however, significantly more cytotoxic against the syngeneic thymocytes (p<0.0001), suggesting the effects of auto reactive clones of cells. Furthermore, in very old mice this type of cytotoxicity might be additionally stimulated by in vivo application of PGM-Zn. On the contrary, in young mice PGM-Zn more stimulated the NK-dependent cytotoxicity against YAC-1 target. The data emphasize the role of the liver in immunosenescence and TLR-mediated control of cell-mediated cytotoxicities, orchestrated by dendritic cells and distinct types of NKT cells.

Izvorni jezik
Engleski

Znanstvena područja
Temeljne medicinske znanosti



POVEZANOST RADA


Projekti:
0062018

Ustanove:
Medicinski fakultet, Rijeka


Citiraj ovu publikaciju:

Mrakovčić-Šutić, Ines; Jakovac, Hrvoje; Grebić, Damir; Radošević-Stašić, Biserka
Immunotherapeutic potential of peptidoglycan-monomer linked with zinc in old mice // The international journal of artificial organs, 28 (2005), 4; 400-400 (podatak o recenziji nije dostupan, kongresno priopcenje, znanstveni)
Mrakovčić-Šutić, I., Jakovac, H., Grebić, D. & Radošević-Stašić, B. (2005) Immunotherapeutic potential of peptidoglycan-monomer linked with zinc in old mice. The international journal of artificial organs, 28 (4), 400-400.
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@article{article, author = {Mrakov\v{c}i\'{c}-\v{S}uti\'{c}, Ines and Jakovac, Hrvoje and Grebi\'{c}, Damir and Rado\v{s}evi\'{c}-Sta\v{s}i\'{c}, Biserka}, year = {2005}, pages = {400-400}, keywords = {peptidoglycan-monomer with Zn, very old mice, liver, spleen, YAC-1, syngeneic thymocytes}, journal = {The international journal of artificial organs}, volume = {28}, number = {4}, issn = {0391-3988}, title = {Immunotherapeutic potential of peptidoglycan-monomer linked with zinc in old mice}, keyword = {peptidoglycan-monomer with Zn, very old mice, liver, spleen, YAC-1, syngeneic thymocytes} }

Časopis indeksira:


  • Current Contents Connect (CCC)
  • Web of Science Core Collection (WoSCC)
    • Science Citation Index Expanded (SCI-EXP)
    • SCI-EXP, SSCI i/ili A&HCI
  • Scopus
  • MEDLINE


Uključenost u ostale bibliografske baze podataka::


  • Biological Abstracts
  • Chemical Abstracts
  • Excerpta Medica
  • Index Medicus
  • EMBASE
  • BIOSIS
  • Metal Abstracts /METADEX





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