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Abstract

Low molecular weight phenotype of Apo(a) is a risk factor of corticosteroid-induced osteonecrosis of the femoral head after renal transplant.

Tetsurou Hirata, Mikihiro Fujioka, Kenji A Takahashi, Takeshi Asano, Masashi Ishida, Kiyokazu Akioka, Masahiko Okamoto, Norio Yoshimura, Yoshiko Satomi, Hoyoku Nishino, Yoshio Hirota, Shigeo Nakajima, Shigeaki Kato and Toshikazu Kubo
The Journal of Rheumatology March 2007, 34 (3) 516-522;
Tetsurou Hirata
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Mikihiro Fujioka
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Kenji A Takahashi
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Takeshi Asano
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Masashi Ishida
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Kiyokazu Akioka
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Masahiko Okamoto
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Norio Yoshimura
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Yoshiko Satomi
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Hoyoku Nishino
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Yoshio Hirota
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Shigeo Nakajima
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Shigeaki Kato
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Toshikazu Kubo
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Abstract

OBJECTIVE: Osteonecrosis of the femoral head (ONF) is a necrosis due to disruption of the blood flow. The disease often occurs in association with corticosteroid treatment. The pathology of corticosteroid-induced ONF is unclear, although abnormalities in the coagulation and fibrinolytic systems or in the lipid metabolism have been reported to be involved. We examined the relationships between development of ONF and genetic variations and plasma level of lipoprotein(a) (Lp(a)), which is closely involved in the coagulation and fibrinolytic systems and lipid metabolism. METHODS: The study population consisted of 112 renal transplant patients undergoing corticosteroid treatment. Their apolipoprotein (a) [apo(a)] isoform was determined by Western blotting, and patients were classified into low molecular weight (LMW) or high molecular weight (HMW) groups. The plasma Lp(a) level was measured. Patients were also examined for 3 single-nucleotide polymorphisms (SNP), -773 (G/A), +93 (C/T), and +121 (G/A). Relationships between these 3 genetic factors of Lp(a) and ONF development were examined using statistical methods including multivariate analysis. RESULTS: A strong relationship was observed between the apo(a) molecular weight phenotype and ONF development, with an increased risk of ONF development for the LMW group (adjusted odds ratio 5.75, 95% CI 1.76-18.74, p = 0.0038). No significant relationships were observed between ONF and plasma Lp(a) level and SNP. CONCLUSION: Apo(a) molecular weight phenotype would be a useful predictor of ONF that develops after corticosteroid treatment.

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The Journal of Rheumatology
Vol. 34, Issue 3
1 Mar 2007
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Low molecular weight phenotype of Apo(a) is a risk factor of corticosteroid-induced osteonecrosis of the femoral head after renal transplant.
Tetsurou Hirata, Mikihiro Fujioka, Kenji A Takahashi, Takeshi Asano, Masashi Ishida, Kiyokazu Akioka, Masahiko Okamoto, Norio Yoshimura, Yoshiko Satomi, Hoyoku Nishino, Yoshio Hirota, Shigeo Nakajima, Shigeaki Kato, Toshikazu Kubo
The Journal of Rheumatology Mar 2007, 34 (3) 516-522;

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Low molecular weight phenotype of Apo(a) is a risk factor of corticosteroid-induced osteonecrosis of the femoral head after renal transplant.
Tetsurou Hirata, Mikihiro Fujioka, Kenji A Takahashi, Takeshi Asano, Masashi Ishida, Kiyokazu Akioka, Masahiko Okamoto, Norio Yoshimura, Yoshiko Satomi, Hoyoku Nishino, Yoshio Hirota, Shigeo Nakajima, Shigeaki Kato, Toshikazu Kubo
The Journal of Rheumatology Mar 2007, 34 (3) 516-522;
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