Recent perspectives on the association between osteonecrosis and bone mineral density decline in childhood acute lymphoblastic leukemia.

Faculty reviews Pub Date : 2021-06-23 eCollection Date: 2021-01-01 DOI:10.12703/r/10-57
Jenneke E van Atteveld, Demi Tc de Winter, Rob Pieters, Sebastian Jcmm Neggers, Marry M van den Heuvel-Eibrink
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引用次数: 1

Abstract

The attention to treatment-related toxicity has increased since the survival of children with acute lymphoblastic leukemia (ALL) has improved significantly over the past few decades. Intensive ALL treatment schedules including corticosteroids and asparaginase have been shown to give rise to skeletal abnormalities such as osteonecrosis and low bone mineral density (BMD), which may lead to debilitating sequelae in survivors. Although osteonecrosis and low BMD are different entities with suggested separate pathophysiological mechanisms, recent studies indicate that osteonecrosis is associated with accelerated BMD decline. Common underlying mechanisms for osteonecrosis and BMD decline are considered, such as an enhanced sensitivity to corticosteroids in children who suffer from both osteonecrosis and low BMD. In addition, restriction of weight-bearing activities, which is generally advised in patients with osteonecrosis, could aggravate BMD decline. This induces a clinical dilemma, since bone stimulation is important to maintain BMD but alternative interventions for osteonecrosis are limited. Furthermore, this recent finding of accelerated BMD decline in children with osteonecrosis emphasizes the need to develop effective preventive measures for osteonecrosis, which may include targeting BMD decline.

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儿童急性淋巴细胞白血病骨坏死与骨密度下降关系的最新研究进展。
在过去的几十年里,急性淋巴细胞白血病(ALL)儿童的生存率显著提高,因此对治疗相关毒性的关注也随之增加。包括皮质类固醇和天冬酰胺酶在内的强化ALL治疗方案已被证明会引起骨骼异常,如骨坏死和低骨密度(BMD),这可能导致幸存者的衰弱后遗症。虽然骨坏死和低骨密度是不同的实体,有不同的病理生理机制,但最近的研究表明骨坏死与骨密度加速下降有关。骨坏死和骨密度下降的共同潜在机制被考虑,例如骨密度低和骨坏死的儿童对皮质类固醇的敏感性增强。此外,骨坏死患者通常建议限制负重活动,这可能会加剧骨密度下降。这引起了临床困境,因为骨刺激对维持骨密度很重要,但骨坏死的替代干预措施有限。此外,最近发现骨密度在骨坏死儿童中加速下降,这强调了制定有效的骨密度预防措施的必要性,其中可能包括针对骨密度下降。
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