Adiso Therapeutics, Concord, MA USA.
APC Microbiome Ireland, University College Cork, Cork, Ireland.
Brain Behav Immun. 2024 Oct;121:384-402. doi: 10.1016/j.bbi.2024.08.024. Epub 2024 Aug 13.
Neuroinflammation is a common component of neurological disorders. In the gut-brain-immune axis, bacteria and their metabolites are now thought to play a role in the modulation of the nervous and immune systems which may impact neuroinflammation. In this respect, commensal bacteria of humans have recently been shown to produce metabolites that mimic endogenous G-protein coupled receptor (GPCR) ligands. To date, it has not been established whether plant commensal bacteria, which may be ingested by animals including humans, can impact the gut-brain-immune axis via GPCR agonism. We screened an isopropanol (IPA) extract of the plant commensal Bacillus velezensis ADS024, a non-engrafting live biotherapeutic product (LBP) with anti-inflammatory properties isolated from human feces, against a panel of 168 GPCRs and identified strong agonism of the lysophosphatidic acid (LPA) receptor LPA3. The ADS024 IPA extracted material (ADS024-IPA) did not agonize LPA2, and only very weakly agonized LPA1. The agonism of LPA3 was inhibited by the reversible LPA1/3 antagonist Ki16425. ADS024-IPA signaled downstream of LPA3 through G-protein-induced calcium release, recruitment of β-arrestin, and recruitment of the neurodegeneration-associated proteins 14-3-3γ, ε and ζ but did not recruit the β isoform. Since LPA3 agonism was previously indirectly implicated in the reduction of pathology in models of Parkinson's disease (PD) and multiple sclerosis (MS) by use of the nonselective antagonist Ki16425, and since we identified an LPA3-specific agonist within ADS024, we sought to examine whether LPA3 might indeed be part of a broad underlying mechanism to control neuroinflammation. We tested oral treatment of ADS024 in multiple models of neuroinflammatory diseases using three models of PD, two models of MS, and a model each of amyotrophic lateral sclerosis (ALS), Huntington's disease (HD), and chemo-induced peripheral neuropathy (CIPN). ADS024 treatment improved model-specific functional effects including improvements in motor movement, breathing and swallowing, and allodynia suggesting that ADS024 treatment impacted a universal underlying neuroinflammatory mechanism regardless of the initiating cause of disease. We used the MOG-EAE mouse model to examine early events after disease initiation and found that ADS024 attenuated the increase in circulating lymphocytes and changes in neutrophil subtypes, and ADS024 attenuated the early loss of cell-surface LPA3 receptor expression on circulating white blood cells. ADS024 efficacy was partially inhibited by Ki16425 in vivo suggesting LPA3 may be part of its mechanism. Altogether, these data suggest that ADS024 and its LPA3 agonism activity should be investigated further as a possible treatment for diseases with a neuroinflammatory component.
神经炎症是许多神经疾病的共同特征。在肠道-大脑-免疫轴中,人们现在认为细菌及其代谢产物在调节神经系统和免疫系统方面发挥作用,这可能会影响神经炎症。在这方面,人类共生菌最近被证明可以产生模拟内源性 G 蛋白偶联受体 (GPCR) 配体的代谢产物。迄今为止,尚未确定植物共生菌是否可以通过 GPCR 激动作用来影响肠道-大脑-免疫轴,而这些共生菌可能会被包括人类在内的动物摄入。我们筛选了一种来自人粪便的非定植性活体生物治疗产品 (LBP) 植物共生菌 Bacillus velezensis ADS024 的异丙醇 (IPA) 提取物,该产品具有抗炎特性,针对 168 个 GPCR 进行了检测,并鉴定出溶血磷脂酸 (LPA) 受体 LPA3 的强烈激动作用。ADSO24IPA 提取材料(ADSO24-IPA)不会激动 LPA2,仅微弱激动 LPA1。LPA3 的激动作用可被可逆的 LPA1/3 拮抗剂 Ki16425 抑制。ADSO24-IPA 通过 G 蛋白诱导的钙释放、β-arrestin 募集和神经变性相关蛋白 14-3-3γ、ε和ζ募集来传递 LPA3 下游信号,但不募集β亚型。由于使用非选择性拮抗剂 Ki16425,LPA3 激动作用先前间接地参与了帕金森病 (PD) 和多发性硬化症 (MS) 模型中病理学的减少,并且我们在 ADS024 中鉴定出了一种 LPA3 特异性激动剂,因此我们试图研究 LPA3 是否确实是控制神经炎症的广泛潜在机制的一部分。我们使用三种 PD 模型、两种 MS 模型以及每种 ALS、HD 和 CIPN 模型,在多种神经炎症性疾病的动物模型中测试了 ADS024 的口服治疗。ADSO24 治疗改善了特定于模型的功能效果,包括运动运动、呼吸和吞咽功能的改善以及所有痛觉过敏,这表明 ADS024 治疗影响了普遍存在的潜在神经炎症机制,而与疾病的起始原因无关。我们使用 MOG-EAE 小鼠模型来研究疾病起始后的早期事件,发现 ADS024 可减轻循环淋巴细胞的增加和中性粒细胞亚型的变化,并可减轻循环白细胞表面 LPA3 受体表达的早期丧失。ADSO24 的功效在体内部分被 Ki16425 抑制,表明 LPA3 可能是其机制的一部分。总而言之,这些数据表明,ADSO24 及其 LPA3 激动活性应作为具有神经炎症成分的疾病的潜在治疗方法进一步研究。
