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与ADNP缺陷相关的微生物群变化:NAP(CP201)治疗ADNP综合征及其他疾病的快速指标。

Microbiota changes associated with ADNP deficiencies: rapid indicators for NAP (CP201) treatment of the ADNP syndrome and beyond.

作者信息

Kapitansky Oxana, Giladi Eliezer, Jaljuli Iman, Bereswill Stefan, Heimesaat Markus M, Gozes Illana

机构信息

The First Lily and Avraham Gildor Chair for the Investigation of Growth Factors, Dr. Diana and Zelman Elton (Elbaum) Laboratory for Molecular Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Sagol School of Neuroscience and Adams Super Center for Brain Studies, Tel Aviv University, 69978, Tel Aviv, Israel.

Department of Statistics and Operations Research, School of Mathematical Sciences, Raymond and Beverly Sackler Faculty of Exact Sciences, Tel-Aviv University, 69978, Tel Aviv, Israel.

出版信息

J Neural Transm (Vienna). 2020 Feb;127(2):251-263. doi: 10.1007/s00702-020-02155-5. Epub 2020 Feb 18.

Abstract

Activity-dependent neuroprotective protein (ADNP) and its protein snippet NAP (drug candidate CP201) regulate synapse formation and cognitive as well as behavioral functions, in part, through microtubule interaction. Given potential interactions between the microbiome and brain function, we now investigated the potential effects of the ADNP-deficient genotype, mimicking the ADNP syndrome on microbiota composition in the Adnp mouse model. We have discovered a surprising robust sexually dichotomized Adnp genotype effect and correction by NAP (CP201) as follows. Most of the commensal bacterial microbiota tested were affected by the Adnp genotype and corrected by NAP treatment in a male sex-dependent manner. The following list includes all the bacterial groups tested-labeled in bold are male Adnp-genotype increased and corrected (decreased) by NAP. (1) Eubacteriaceae (EubV3), (2) Enterobacteriaceae (Entero), (3) Enterococcus genus (gEncocc), (4) Lactobacillus group (Lacto), (5) Bifidobacterium genus (BIF), (6) Bacteroides/Prevotella species (Bac), (7) Clostridium coccoides group (Coer), (8) Clostridium leptum group (Cluster IV, sgClep), and (9) Mouse intestinal Bacteroides (MIB). No similarities were found between males and females regarding sex- and genotype-dependent microbiota distributions. Furthermore, a female Adnp genotype associated decrease (contrasting male increase) was observed in the Lactobacillus group (Lacto). Significant correlations were discovered between specific bacterial group loads and open-field behavior as well as social recognition behaviors. In summary, we discovered ADNP deficiency associated changes in commensal gut microbiota compositions, a sex-dependent biomarker for the ADNP syndrome and beyond. Strikingly, we discovered rapidly detected NAP (CP201) treatment-dependent biomarkers within the gut microbiota.

摘要

活性依赖的神经保护蛋白(ADNP)及其蛋白片段NAP(候选药物CP201)部分通过与微管相互作用来调节突触形成、认知及行为功能。鉴于微生物群与脑功能之间存在潜在相互作用,我们现在研究了在Adnp小鼠模型中,模拟ADNP综合征的ADNP缺陷基因型对微生物群组成的潜在影响。我们发现了一个令人惊讶的、强大的性别二分法Adnp基因型效应以及NAP(CP201)的校正作用,具体如下。所检测的大多数共生细菌微生物群受到Adnp基因型的影响,并以雄性性别依赖的方式通过NAP治疗得到校正。以下列表包括所有检测的细菌组——加粗标记的是雄性Adnp基因型增加并通过NAP校正(减少)的细菌组。(1)真杆菌科(EubV3),(2)肠杆菌科(Entero),(3)肠球菌属(gEncocc),(4)乳杆菌属(Lacto),(5)双歧杆菌属(BIF),(6)拟杆菌/普雷沃氏菌属(Bac),(7)球状梭菌组(Coer),(8)纤细梭菌组(第四簇,sgClep),以及(9)小鼠肠道拟杆菌(MIB)。在性别和基因型依赖的微生物群分布方面,未发现雄性和雌性之间存在相似性。此外,在乳杆菌属(Lacto)中观察到雌性Adnp基因型相关的减少(与雄性增加相反)。在特定细菌组负荷与旷场行为以及社会识别行为之间发现了显著相关性。总之,我们发现ADNP缺乏与共生肠道微生物群组成的变化有关,这是ADNP综合征及其他相关疾病的性别依赖性生物标志物。引人注目的是,我们在肠道微生物群中发现了快速检测到的依赖于NAP(CP201)治疗的生物标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ef41/7035218/8a586c6ed905/702_2020_2155_Fig1_HTML.jpg

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