Orygen Youth Health Research Centre, University of Melbourne, Melbourne, Australia.
Psychiatry Res. 2012 Aug 30;199(1):8-11. doi: 10.1016/j.psychres.2012.03.010. Epub 2012 Apr 14.
Reports suggesting that schizophrenia participants are more likely to be phenylthiocarbamide (PTC) non-tasters when compared to controls have recently been controversial. If supported, a genetic-based phenotypic variation in PTC taster status is implicated, suggesting a greater illness risk for those participants with recessive alleles for the TAS2R38 receptor. Should PTC insensitivity be a schizophrenia endophenotype, then it would be expected in follow-up of ultra high-risk for psychosis participants who later develop schizophrenia (UHR-S). UHR-S was hypothesised to show reduced PTC sensitivity compared to those who were previously at risk, but did not transition (UHR-NP). PTC perception was assessed in 219 UHR participants at long-term follow-up, of whom 53 had transitioned to psychosis (UHR-P) during the follow-up period. Fifteen of the 219 participants were diagnosed with schizophrenia. Seventy-eight had a family history of psychotic disorder. No differences in PTC taster status were found in UHR participants based upon transition to psychosis status, schizophrenia diagnosis, or family history of schizophrenia. This report indicates that schizophrenia development among UHR participants is not associated with PTC tasting deficits and fails to support previous findings that inability to detect the bitter taste of PTC is a schizophrenia endophenotype.
有报道称,与对照组相比,精神分裂症患者更有可能无法尝出苯硫脲(PTC),这一观点最近引起了争议。如果这一观点得到证实,那么 PTC 味觉状态的遗传表型变异就暗示了那些 TAS2R38 受体隐性等位基因的参与者患病风险更高。如果 PTC 不敏感是精神分裂症的一个内表型,那么在精神病超高风险(UHR)参与者中进行随访时,预计会出现这种情况,这些参与者后来发展为精神分裂症(UHR-S)。UHR-S 被假设为与那些以前有风险但没有转变的参与者相比,PTC 敏感性降低(UHR-NP)。在长期随访中,对 219 名 UHR 参与者进行了 PTC 感知评估,其中 53 名参与者在随访期间发展为精神病(UHR-P)。219 名参与者中有 15 人被诊断为精神分裂症。78 人有精神障碍家族史。在 UHR 参与者中,根据向精神病状态、精神分裂症诊断或精神分裂症家族史的转变,无法发现 PTC 味觉状态的差异。本报告表明,UHR 参与者的精神分裂症发展与 PTC 味觉缺陷无关,也不支持先前无法检测到 PTC 苦味是精神分裂症内表型的发现。
