Niikura Kazuaki, Takeshita Nobuaki, Takano Mikiko
Pharmacology Research Laboratories, Astellas Pharma Inc., Ibaraki, Japan.
J Bone Miner Res. 2005 Sep;20(9):1579-88. doi: 10.1359/JBMR.050517. Epub 2005 May 31.
FR167356, a novel inhibitor of vacuolar ATPase, has high potency against osteoclast V-ATPase and low potency against lysosomal V-ATPase. FR167356 is the first compound of this nature to be tested. It has the potential to be useful for clinical application.
It has been suggested that the key issue regarding the therapeutic usefulness of V-ATPase inhibitors is their selectivity.
In in vitro and in vivo studies, we compared FR167356 with other vacuolar ATPase (V-ATPase) inhibitors, bafilomycin A1 and SB242784. H+ transport by various membrane vesicles was assayed by measuring uptake of acridine orange. Inhibitory activity against in vitro bone resorption was examined by measuring the Ca2+ release from cultured calvariae. In vivo, hypercalcemia was induced by retinoic acid in thyroparathyroidectomized-ovariectomized rats, and the effect on serum Ca2+ level was assessed. Ovariectomized rats were treated with FR167356 or SB242784. One week after surgery, free deoxypyridinoline levels in 24-h urine samples, which were collected from 6 h after administration of FR167356, were measured by ELISA. After 4 weeks of treatment, plasma biochemical parameters were analyzed. BMD of the distal femur metaphysis was measured with pQCT. Histomorphometric analysis of the proximal tibias was performed. Blood gases of rats treated with FR167356 were measured with a blood gas analyzer for estimating the effect of FR167356 on in vivo function of renal V-ATPase.
FR167356, which is distinctly different from other V-ATPase inhibitors, has a high potency against osteoclast V-ATPase and low potency against lysosomal V-ATPase. Similarly, FR167356 inhibited bone resorption in vitro when stimulated by PTH, IL-1, and IL-6. FR167356 reduced retinoic acid-induced hypercalcemia in thyroparathyroidectomized-ovariectomized rats in a dose-dependent manner. Moreover, FR167356 was shown to restore BMD of ovariectomized rats caused by the inhibition of bone resorption. Ovariectomized rats treated with FR167356 did not show adverse symptoms, whereas SB242784 caused a decrease in body weight gain and significant changes in two plasma biochemical parameters. Interestingly, FR167356 treatment did not affect blood acid-base balance; however, FR167356 inhibited renal V-ATPase with a similar potency as for osteoclast V-ATPase inhibition.
Comparison of FR167356 with SB242784 implies that the characteristics of FR167356 may be more appropriate for clinical application as a V-ATPase inhibitor.
新型液泡型ATP酶抑制剂FR167356对破骨细胞V-ATP酶具有高效力,而对溶酶体V-ATP酶效力较低。FR167356是首个被测试的此类化合物。它具有临床应用的潜力。
有人提出,V-ATP酶抑制剂治疗效用的关键问题在于其选择性。
在体外和体内研究中,我们将FR167356与其他液泡型ATP酶(V-ATP酶)抑制剂巴弗洛霉素A1和SB242784进行了比较。通过测量吖啶橙摄取量来测定各种膜囊泡的H⁺转运。通过测量培养颅骨中Ca²⁺释放来检测对体外骨吸收的抑制活性。在体内,用维甲酸诱导甲状旁腺切除-卵巢切除大鼠出现高钙血症,并评估对血清Ca²⁺水平的影响。给卵巢切除大鼠用FR167356或SB242784治疗。手术后一周,通过ELISA测量从给予FR167356后6小时开始收集的24小时尿液样本中的游离脱氧吡啶啉水平。治疗4周后,分析血浆生化参数。用pQCT测量股骨远端干骺端的骨密度。对近端胫骨进行组织形态计量分析。用血气分析仪测量用FR167356治疗的大鼠的血气,以评估FR167356对肾V-ATP酶体内功能的影响。
FR167356与其他V-ATP酶抑制剂明显不同,对破骨细胞V-ATP酶具有高效力,而对溶酶体V-ATP酶效力较低。同样,FR167356在受到甲状旁腺激素、白细胞介素-1和白细胞介素-6刺激时,能在体外抑制骨吸收。FR167356以剂量依赖性方式降低了甲状旁腺切除-卵巢切除大鼠中维甲酸诱导的高钙血症。此外,FR167356显示可恢复因骨吸收抑制导致的卵巢切除大鼠的骨密度。用FR167356治疗的卵巢切除大鼠未出现不良症状,而SB242784导致体重增加减少和两个血浆生化参数发生显著变化。有趣的是,FR167356治疗不影响血液酸碱平衡;然而,FR167356抑制肾V-ATP酶的效力与抑制破骨细胞V-ATP酶的效力相似。
将FR167356与SB242784进行比较表明,FR167356的特性可能更适合作为V-ATP酶抑制剂用于临床应用。
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