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首页> 外文期刊>Thyroid: official journal of the American Thyroid Association >Extensions, validation, and clinical applications of a feedback control system simulator of the hypothalamo-pituitary-thyroid axis.
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Extensions, validation, and clinical applications of a feedback control system simulator of the hypothalamo-pituitary-thyroid axis.

机译:下丘脑-垂体-甲状腺轴反馈控制系统模拟器的扩展,验证和临床应用。

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摘要

BACKGROUND: We upgraded our recent feedback control system (FBCS) simulation model of human thyroid hormone (TH) regulation to include explicit representation of hypothalamic and pituitary dynamics, and updated TH distribution and elimination (D&E) parameters. This new model greatly expands the range of clinical and basic science scenarios explorable by computer simulation. METHODS: We quantified the model from pharmacokinetic (PK) and physiological human data and validated it comparatively against several independent clinical data sets. We then explored three contemporary clinical issues with the new model: combined triiodothyronine (T(3))/thyroxine (T(4)) versus T(4)-only treatment, parenteral levothyroxine (L-T(4)) administration, and central hypothyroidism. RESULTS: Combined T(3)/T(4) therapy--In thyroidectomized patients, the L-T(4)-only replacement doses needed to normalize plasma T(3) or average tissue T(3) were 145 microg L-T(4)/day or 165 microg L-T(4)/day, respectively. The combined T(4) + T(3) dosing needed to normalize both plasma and tissue T(3) levels was 105 microg L-T(4) + 9 microg T(3) per day. For all three regimens, simulated mean steady-state plasma thyroid-stimulating hormone (TSH), T(3), and T(4) was within normal ranges (TSH: 0.5-5 mU/L; T(4): 5-12 microg/dL; T(3): 0.8-1.9 ng/mL). Parenteral T(4) administration--800 microg weekly or 400 microg twice weekly normalized average tissue T(3) levels both for subcutaneous (SC) and intramuscular (IM) routes of administration. TSH, T(3), and T(4) levels were maintained within normal ranges for all four of these dosing schemes (1x vs. 2x weekly, SC vs. IM). Central hypothyroidism--We simulated steady-state plasma T(3), T(4), and TSH concentrations in response to varying degrees of central hypothyroidism, reducing TSH secretion from 50% down to 0.1% of normal. Surprisingly, TSH, T(3), and T(4) plasma concentrations remained within normal ranges for TSH secretion as low as 25% of normal. CONCLUSIONS: Combined T(3)/T(4) treatment--Simulated standard L-T(4)-only therapy was sufficient to renormalize average tissue T(3) levels and maintain normal TSH, T(3), and T(4) plasma levels, supporting adequacy of standard L-T(4)-only treatment. Parenteral T(4) administration-TSH, T(3), and T(4) levels were maintained within normal ranges for all four of these dosing schemes (1x vs. 2x weekly, SC vs. IM), supporting these therapeutic alternatives for patients with compromised L-T(4) gut absorption. Central hypothyroidism--These results highlight how highly nonlinear feedback in the hypothalamic-pituitary-thyroid axis acts to maintain normal hormone levels, even with severely reduced TSH secretion.
机译:背景:我们升级了人类甲状腺激素(TH)调节的最新反馈控制系统(FBCS)仿真模型,以包括下丘脑和垂体动力学的明确表示,并更新了TH分布和消除(D&E)参数。这种新模型极大地扩展了可通过计算机仿真探索的临床和基础科学场景的范围。方法:我们从药代动力学(PK)和人体生理数据对模型进行了量化,并针对几个独立的临床数据集进行了比较验证。然后,我们使用新模型探索了三个当代临床问题:三碘甲状腺素(T(3))/甲状腺素(T(4))与仅T(4)的治疗,肠胃外左甲状腺素(LT(4))的给药和甲状腺功能减退。结果:T(3)/ T(4)联合治疗-在甲状腺切除的患者中,使血浆T(3)或平均组织T(3)正常化所需的仅LT(4)替代剂量为145 microg LT(4) /天或165微克LT(4)/天。标准化血浆和组织T(3)水平所需的总T(4)+ T(3)剂量为每天105微克L-T(4)+ 9微克T(3)。对于这三种方案,模拟的平均稳态血浆促甲状腺激素(TSH),T(3)和T(4)均在正常范围内(TSH:0.5-5 mU / L; T(4):5- 12 microg / dL; T(3):0.8-1.9 ng / mL)。肠胃外T(4)给药-皮下(SC)和肌内(IM)给药途径每周800微克或每周两次400微克标准化平均组织T(3)水平。对于所有这四种给药方案,TSH,T(3)和T(4)的水平均维持在正常范围内(每周1次vs. 2x,SC vs. IM)。中枢甲状腺功能减退症-我们模拟了稳态血浆T(3),T(4)和TSH的浓度,以响应不同程度的中枢甲状腺功能减退症,将TSH分泌从正常的50%降低到0.1%。令人惊讶的是,TSH,TS(3)和T(4)的血浆浓度保持在正常范围内,TSH的分泌量仅为正常水平的25%。结论:T(3)/ T(4)联合治疗-仅模拟标准LT(4)疗法足以使平均组织T(3)水平正常化并维持正常的TSH,T(3)和T(4)血浆水平,支持仅LT(4)标准治疗的充分性。所有这四种给药方案的肠胃外T(4)给药-TSH,T(3)和T(4)的水平均维持在正常范围内(每周1次vs. 2x,SC vs. IM),支持这些治疗方案LT(4)肠道吸收受损的患者。中枢甲状腺功能减退症-这些结果凸显了下丘脑-垂体-甲状腺轴的高度非线性反馈如何维持正常的激素水平,即使TSH分泌严重减少。

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