关于婴儿期膳食牛骨质素安全数据的充分性和生理作用的专家小组会议

Stephen A. Fleming, Sarah M. Reyes, Sharon M. Donovan, O. Hernell, Rulan Jiang, Bo Lönnerdal, Josef Neu, Lawrence Steinman, Esben S. Sørensen, Christina E. West, Ronald Kleinman, J. Wallingford
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摘要

母乳因其独特的成分而成为婴儿营养的最佳标准。人乳中含有丰富的骨生成素(OPN),而牛乳中却没有。在配方奶中添加牛乳骨生成素(bmOPN)可能会复制人乳中 OPN 的浓度和功能。为了解决安全性问题,我们召集了一个专家小组,以评估婴儿期膳食中 bmOPN 的安全性数据和生理作用是否充分。母乳喂养婴儿暴露于人乳 OPN(hmOPN)的情况已经得到了很好的描述,在哺乳期的前 6 个月会明显减少。膳食中的 bmOPN 不易被胃肠消化,可在 8-24 小时内被吸收并从血液循环中清除,仅占血浆 OPN 总量的一小部分(<5%)。对 hmOPN 的标签研究表明,3 小时后,完整或消化的 OPN 被胴体(62%)、小肠(23%)、胃(5%)和小肠灌流物(4%)吸收,在盲肠、肝脏、大脑、心脏和脾脏中发现的 OPN 各占 <2%。虽然有关 bmOPN 生理影响的研究结果各不相同,但在生长、胃肠道、免疫或大脑相关结果方面均未发现不良影响。重组牛型和人型在血浆中的吸收与 bmOPN 相似,对认知和免疫也有影响。专家小组建议优先考虑对免疫力和认知能力的临床相关结果进行全面测定的试验,以确认 bmOPN 的安全性,而不是进一步研究其吸收、分布、代谢和排泄情况。本综述就现有数据是否足以评估婴儿配方奶粉中使用的 bmOPN 的安全性达成了专家共识,有助于就婴儿配方奶粉的配方做出循证决策。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
An expert panel on the adequacy of safety data and physiological roles of dietary bovine osteopontin in infancy
Human milk, due to its unique composition, is the optimal standard for infant nutrition. Osteopontin (OPN) is abundant in human milk but not bovine milk. The addition of bovine milk osteopontin (bmOPN) to formula may replicate OPN’s concentration and function in human milk. To address safety concerns, we convened an expert panel to assess the adequacy of safety data and physiological roles of dietary bmOPN in infancy. The exposure of breastfed infants to human milk OPN (hmOPN) has been well-characterized and decreases markedly over the first 6 months of lactation. Dietary bmOPN is resistant to gastric and intestinal digestion, absorbed and cleared from circulation within 8–24 h, and represents a small portion (<5%) of total plasma OPN. Label studies on hmOPN suggest that after 3 h, intact or digested OPN is absorbed into carcass (62%), small intestine (23%), stomach (5%), and small intestinal perfusate (4%), with <2% each found in the cecum, liver, brain, heart, and spleen. Although the results are heterogenous with respect to bmOPN’s physiologic impact, no adverse impacts have been reported across growth, gastrointestinal, immune, or brain-related outcomes. Recombinant bovine and human forms demonstrate similar absorption in plasma as bmOPN, as well as effects on cognition and immunity. The panel recommended prioritization of trials measuring a comprehensive set of clinically relevant outcomes on immunity and cognition to confirm the safety of bmOPN over that of further research on its absorption, distribution, metabolism, and excretion. This review offers expert consensus on the adequacy of data available to assess the safety of bmOPN for use in infant formula, aiding evidence-based decisions on the formulation of infant formula.
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