Effect of positive allosteric modulation and orthosteric agonism of dopamine D2-like receptors on respiration in mouse models of Rett syndrome

IF 1.9 4区 医学 Q3 PHYSIOLOGY
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Abstract

Rett syndrome (RTT) is an autism spectrum disorder caused by loss-of-function mutations in the methyl-CPG-binding protein 2 (Mecp2) gene. Frequent apneas and irregular breathing are prevalent in RTT, and also occur in rodent models of the disorder, including Mecp2Bird and Mecp2R168X mice. Sarizotan, a serotonin 5-HT1a and dopamine D2-like receptor agonist, reduces the incidence of apneas and irregular breathing in mouse models of RTT (Abdala et al., 2014). Targeting the 5HT1a receptor alone also improves respiration in RTT mice (Levitt et al., 2013). However, the contribution of D2-like receptors in correcting these respiratory disturbances remains untested. PAOPA, a dopamine D2-like receptor positive allosteric modulator, and quinpirole, a dopamine D2-like receptor orthosteric agonist, were used in conjunction with whole-body plethysmography to evaluate whether activation of D2-like receptors is sufficient to improve breathing disturbances in female heterozygous Mecp2Bird/+ and Mecp2R168X/+ mice. PAOPA did not significantly change apnea incidence or irregularity score in RTT mice. PAOPA also had no effect on the ventilatory response to hypercapnia (7 % CO2). In contrast, quinpirole reduced apnea incidence and irregularity scores and improved the hypercapnic ventilatory response in Mecp2R168X/+ and Mecp2Bird/+ mice, while also reducing respiratory rate. These results suggest that D2-like receptors could contribute to the positive effects of sarizotan in the correction of respiratory abnormalities in Rett syndrome. However, positive allosteric modulation of D2-like receptors alone was not sufficient to evoke these effects.

多巴胺 D2 类受体的正异位调节和正异位激动对雷特综合征小鼠模型呼吸的影响
雷特综合征(RTT)是一种自闭症谱系障碍,由甲基-氯化石蜡结合蛋白 2(Mecp2)基因的功能缺失突变引起。频繁的呼吸暂停和不规则呼吸在 RTT 中很常见,在该疾病的啮齿类动物模型中也会出现,包括 Mecp2Bird 和 Mecp2R168X 小鼠。Sarizotan 是一种血清素 5-HT1a 和多巴胺 D2 样受体激动剂,可降低 RTT 小鼠模型中呼吸暂停和呼吸不规则的发生率(Abdala 等人,2014 年)。单独靶向 5HT1a 受体也能改善 RTT 小鼠的呼吸(Levitt 等人,2013 年)。然而,D2样受体在纠正这些呼吸障碍方面的贡献仍有待检验。PAOPA 是一种多巴胺 D2 样受体正异位调节剂,喹吡罗是一种多巴胺 D2 样受体正异位激动剂,我们将其与全身褶压测定法结合使用,以评估激活 D2 样受体是否足以改善雌性杂合子 Mecp2Bird/+ 和 Mecp2R168X/+ 小鼠的呼吸紊乱。PAOPA 对 RTT 小鼠的呼吸暂停发生率或不规则性评分没有明显改变。PAOPA 对高碳酸血症(7% CO2)的通气反应也没有影响。相反,喹吡罗能降低呼吸暂停发生率和不规则性评分,改善 Mecp2R168X/+ 和 Mecp2Bird/+ 小鼠的高碳酸血症通气反应,同时还能降低呼吸频率。这些结果表明,D2 样受体可能有助于沙里佐坦在纠正 Rett 综合征呼吸异常方面的积极作用。然而,仅对D2样受体进行正性异位调节不足以诱发这些效应。
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来源期刊
CiteScore
4.80
自引率
8.70%
发文量
104
审稿时长
54 days
期刊介绍: Respiratory Physiology & Neurobiology (RESPNB) publishes original articles and invited reviews concerning physiology and pathophysiology of respiration in its broadest sense. Although a special focus is on topics in neurobiology, high quality papers in respiratory molecular and cellular biology are also welcome, as are high-quality papers in traditional areas, such as: -Mechanics of breathing- Gas exchange and acid-base balance- Respiration at rest and exercise- Respiration in unusual conditions, like high or low pressure or changes of temperature, low ambient oxygen- Embryonic and adult respiration- Comparative respiratory physiology. Papers on clinical aspects, original methods, as well as theoretical papers are also considered as long as they foster the understanding of respiratory physiology and pathophysiology.
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