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izvor podataka: crosbi

Role of B lymphocytes in new bone formation (CROSBI ID 87172)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Marušić, Ana ; Grčević, Danka ; Katavić, Vedran ; Kovačić, Nataša ; Lukić, Ivan Krešimir ; Kalajzić, Ivo ; Lorenzo, Joseph A. Role of B lymphocytes in new bone formation // Laboratory investigation, 80 (2000), 11; 1761-1774-x

Podaci o odgovornosti

Marušić, Ana ; Grčević, Danka ; Katavić, Vedran ; Kovačić, Nataša ; Lukić, Ivan Krešimir ; Kalajzić, Ivo ; Lorenzo, Joseph A.

engleski

Role of B lymphocytes in new bone formation

Although they may be a close relationship between B lymphocytes and osteoclasts, bone resorbing cells, little is known about the role of B lymphocytes in bone formation. We compared in vivo new bone induction in mice homozygous for the microMT gene knockout, which lack functional B lymphocytes, with that in control wild type (C57BL/6) mice, using two models of new bone induction in vivo: endochondral osteoinduction by subcutaneous implantation of recombinant human bone morphogenetic protein (rhBMP-2) and osteogenic regeneration after tibial bone marrow ablation. The expression of bone specific proteins (bone sialoprotein, osteopontin, and osteocalcin) and inflammatory/ immunomodulatory cytokines (interleukin-1alpha and -1beta, interleukin-6, and tumor necrosis factor-alpha ) was assessed by Northern blot analysis or reverse transcription – polymerase chain reaction, respectively. Ossicles induced by rhBMP-2 were larger in volume and mass in microMT knockout mice, but relative volumes of the newly induced bone, cartilage, and bone marrow were similar in the two groups. Six days after tibial bone marrow ablation, microMT knockout mice resorbed the initial blood clot faster and formed more trabecular bone, paralleled by greater levels of bone sialoprotein mRNA than in the wild type mice. microMT knockout and wild type mice also differed in the expression pattern of inflammatory/immunomodulatory cytokines during the development of the newly induced bone, suggesting that a genetic lack of B lymphocytes may create a change in the immunological milieu at the site of new bone induction, which stimulates the initial accumulation and proliferation of mesenchymal progenitor.

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Podaci o izdanju

80 (11)

2000.

1761-1774-x

objavljeno

0023-6837

Povezanost rada

Farmacija

Indeksiranost