原发性和继发性甲状旁腺功能亢进状态模型中的代谢性碱中毒。
Metabolic alkalosis in models of primary and secondary hyperparathyroid states.
作者信息
Hulter H N, Toto R D, Ilnicki L P, Halloran B, Sebastian A
出版信息
Am J Physiol. 1983 Oct;245(4):F450-61. doi: 10.1152/ajprenal.1983.245.4.F450.
Hyperchloremic metabolic acidosis has been reported in clinical states of primary and secondary hyperparathyroidism (HPT). Acute administration of parathyroid hormone (PTH) decreases renal acidification in humans and dogs, but the renal and systemic acid-base effects of chronic HPT have not been extensively investigated. In chronically thyroparathyroidectomized (TPTX) dogs (group I), bPTH 1-5 U/kg twice daily resulted in sustained hypophosphatemia, hypercalcemia, and Cl- -resistant metabolic alkalosis that was of renal origin at least in part: delta [HCO3-]p + 4.1 +/- 0.8 meq/liter, P less than 0.01; delta [H+]p -4 +/- 1 neq/liter, P less than 0.001, days 10-12. The cumulative change (sigma delta) in net acid excretion (NAE) was +44 meq (day 9, P less than 0.05). Similarly, metabolic alkalosis of renal origin, at least in part, occurred when PTH was administered by chronic continuous intravenous infusion (group II). Since chronic administration of calcitriol in dogs results in metabolic alkalosis, plasma calcitriol concentration was measured and found not to be increased by chronic intravenous PTH administration. In intact dogs (group III), a continuous chronic intravenous infusion of the Ca2+ chelator, Na4EGTA (3.0 mmol/kg daily), substituted for an equimolar amount of prechelated EGTA (CaNa2EGTA), resulted in a model of hypocalcemic HPT and severe Cl- -resistant metabolic alkalosis: delta [HCO3-]p +9.1 +/- 1.9 meq/liter, P less than 0.05; delta [H+]p -5 +/- 1 neq/liter, P less than 0.01, days 6-8. NAE decreased significantly. Thus, whereas metabolic alkalosis induced by PTH administration could be accounted for by increased NAE (group I), EGTA-induced metabolic alkalosis was accounted for by an extrarenal mechanism of base input to extracellular fluid (group III). Neutralization of the extrarenal base input by chronic administration of HCl during the period of EGTA-induced HPT did not preclude the development of metabolic alkalosis (group V), suggesting that a renal component was present in EGTA-induced metabolic alkalosis as well as in models of primary HPT (groups I and II). During the steady state, in this group as in the groups administered PTH, the net endogenous load of acid to the systemic circulation requiring renal excretion was unchanged from control, as indicated by stable values of NAE not significantly different from control. Yet metabolic alkalosis persisted in the steady state.(ABSTRACT TRUNCATED AT 400 WORDS)
高氯性代谢性酸中毒已在原发性和继发性甲状旁腺功能亢进(HPT)的临床状态中被报道。急性给予甲状旁腺激素(PTH)会降低人和犬的肾脏酸化功能,但慢性HPT对肾脏和全身酸碱平衡的影响尚未得到广泛研究。在慢性甲状腺甲状旁腺切除(TPTX)的犬(第一组)中,每日两次给予bPTH 1 - 5 U/kg导致持续的低磷血症、高钙血症和对Cl⁻抵抗的代谢性碱中毒,其至少部分源于肾脏:[HCO₃⁻]p变化量 + 4.1 ± 0.8 meq/升,P < 0.01;[H⁺]p变化量 -4 ± 1 nmol/升,P < 0.001,第10 - 12天。净酸排泄(NAE)的累积变化(∑δ)为 +44 meq(第9天,P < 0.05)。同样,当通过慢性持续静脉输注给予PTH时(第二组),至少部分出现了源于肾脏的代谢性碱中毒。由于在犬中慢性给予骨化三醇会导致代谢性碱中毒,因此测量了血浆骨化三醇浓度,发现慢性静脉给予PTH并未使其升高。在完整的犬(第三组)中,持续慢性静脉输注Ca²⁺螯合剂Na₄EGTA(每日3.0 mmol/kg)替代等摩尔量的预先螯合的EGTA(CaNa₂EGTA),导致了低钙血症性HPT和严重的对Cl⁻抵抗的代谢性碱中毒模型:[HCO₃⁻]p变化量 +9.1 ± 1.9 meq/升,P < 0.05;[H⁺]p变化量 -5 ± 1 nmol/升,P < 0.01,第6 - 8天。NAE显著降低。因此,虽然给予PTH诱导的代谢性碱中毒可由NAE增加来解释(第一组),但EGTA诱导的代谢性碱中毒是由碱输入细胞外液的肾外机制引起的(第三组)。在EGTA诱导的HPT期间通过慢性给予HCl中和肾外碱输入并不能阻止代谢性碱中毒的发生(第五组),这表明在EGTA诱导的代谢性碱中毒以及原发性HPT模型(第一组和第二组)中都存在肾脏因素。在稳态时,与给予PTH的组一样,该组中需要肾脏排泄的全身循环中酸的净内源性负荷与对照相比没有变化,这由与对照无显著差异的稳定NAE值表明。然而,代谢性碱中毒在稳态时持续存在。(摘要截断于400字)
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