Department of Biomedical Genetics, University of Rochester Medical Center, 601 Elmwood Avenue, Rochester, NY, 14642, USA.
MURTI Centre and Department of Biotechnology, School of Technology, Gandhi Institute of Technology and Management (GITAM), Visakhapatnam, Andhra Pradesh, 530045, India.
Geroscience. 2024 Oct;46(5):4827-4854. doi: 10.1007/s11357-024-01197-x. Epub 2024 Jun 15.
Dietary restriction (DR), the process of decreasing overall food consumption over an extended period of time, has been shown to increase longevity across evolutionarily diverse species and delay the onset of age-associated diseases in humans. In Caenorhabditis elegans, the Myc-family transcription factors (TFs) MXL-2 (Mlx) and MML-1 (MondoA/ChREBP), which function as obligate heterodimers, and PHA-4 (orthologous to FOXA) are both necessary for the full physiological benefits of DR. However, the adaptive transcriptional response to DR and the role of MML-1::MXL-2 and PHA-4 remains elusive. We identified the transcriptional signature of C. elegans DR, using the eat-2 genetic model, and demonstrate broad changes in metabolic gene expression in eat-2 DR animals, which requires both mxl-2 and pha-4. While the requirement for these factors in DR gene expression overlaps, we found many of the DR genes exhibit an opposing change in relative gene expression in eat-2;mxl-2 animals compared to wild-type, which was not observed in eat-2 animals with pha-4 loss. Surprisingly, we discovered more than 2000 genes synthetically dysregulated in eat-2;mxl-2, out of which the promoters of down-regulated genes were substantially enriched for PQM-1 and ELT-1/3 GATA TF binding motifs. We further show functional deficiencies of the mxl-2 loss in DR outside of lifespan, as eat-2;mxl-2 animals exhibit substantially smaller brood sizes and lay a proportion of dead eggs, indicating that MML-1::MXL-2 has a role in maintaining the balance between resource allocation to the soma and to reproduction under conditions of chronic food scarcity. While eat-2 animals do not show a significantly different metabolic rate compared to wild-type, we also find that loss of mxl-2 in DR does not affect the rate of oxygen consumption in young animals. The gene expression signature of eat-2 mutant animals is consistent with optimization of energy utilization and resource allocation, rather than induction of canonical gene expression changes associated with acute metabolic stress, such as induction of autophagy after TORC1 inhibition. Consistently, eat-2 animals are not substantially resistant to stress, providing further support to the idea that chronic DR may benefit healthspan and lifespan through efficient use of limited resources rather than broad upregulation of stress responses, and also indicates that MML-1::MXL-2 and PHA-4 may have distinct roles in promotion of benefits in response to different pro-longevity stimuli.
饮食限制(DR),即减少长时间内的总食物消耗的过程,已被证明可以延长跨进化多样化物种的寿命,并延缓人类与年龄相关疾病的发作。在秀丽隐杆线虫中,Myc 家族转录因子(TF)MXL-2(Mlx)和 MML-1(MondoA/ChREBP),作为必需的异二聚体,以及 PHA-4(与 FOXA 同源),都是 DR 全部生理益处所必需的。然而,对 DR 的适应性转录反应以及 MML-1::MXL-2 和 PHA-4 的作用仍然难以捉摸。我们使用 eat-2 遗传模型鉴定了秀丽隐杆线虫 DR 的转录特征,并证明了 eat-2 DR 动物中代谢基因表达的广泛变化,这需要 mxl-2 和 pha-4。虽然这些因素在 DR 基因表达中存在重叠,但我们发现许多 DR 基因在 eat-2;mxl-2 动物中的相对基因表达变化与野生型相反,而在 eat-2 动物中 pha-4 缺失时则没有观察到这种变化。令人惊讶的是,我们发现超过 2000 个基因在 eat-2;mxl-2 中综合失调,其中下调基因的启动子显著富集了 PQM-1 和 ELT-1/3 GATA TF 结合基序。我们还进一步显示了 DR 中 mxl-2 缺失的功能缺陷超出了寿命范围,因为 eat-2;mxl-2 动物的繁殖力明显较小,产卵比例也有死卵,这表明 MML-1::MXL-2 在维持资源分配给躯体和繁殖之间的平衡方面发挥了作用在慢性食物匮乏的情况下。虽然与野生型相比,eat-2 动物的代谢率没有明显差异,但我们还发现,DR 中 mxl-2 的缺失不会影响年轻动物的耗氧量。eat-2 突变体动物的基因表达特征与能量利用和资源分配的优化一致,而不是诱导与急性代谢应激相关的典型基因表达变化,例如 TORC1 抑制后自噬的诱导。 eat-2 动物也没有明显抵抗应激,这进一步支持了慢性 DR 通过有效利用有限资源而不是广泛上调应激反应来有益于健康寿命和寿命的观点,也表明 MML-1::MXL-2 和 PHA-4 可能在促进对不同长寿刺激的益处方面发挥不同的作用。
