The study does not isolate the mitochondrial pool of Par3 as necessary and sufficient for the metabolic and growth phenotypes because all manipulations alter total Par3 rather than using mitochondria-restricted or import-defective rescues (Figures 1, 4, 5). Given Par3's extensive non-mitochondrial functions in cortical signaling and tight junction formation [1], global knockdown/overexpression can rewire proliferation and metabolism via established cortical pathways independent of OGDH. While established methods exist for mitochondrial-specific protein targeting and rescue experiments [2], these approaches were not employed. Without compartment-specific genetics, the link from mitochondrial Par3–OGDH (Figure 3) to OCR/metabolite shifts (Figure 4) and xenograft outcomes (Figure 5) remains inferential.
线粒体Par3功能验证:为何需要区室特异性靶向实验?
本文分析Par3线粒体功能验证的技术缺陷,指出缺乏特异性靶向实验导致功能关联性推断不足,详解线粒体特异性蛋白验证方法及其在代谢表型与异种移植研究中的关键作用。
与梅斯小智对话
