The MICOS Complex Regulates Mitochondrial Structure and Oxidative Stress During Age-Dependent Structural Deficits in the Kidney

  1. Zer Vue
  2. Praveena Prasad
  3. Han Le
  4. Kit Neikirk
  5. Chanel Harris
  6. Edgar Garza-Lopez
  7. Eric Wang
  8. Alexandria Murphy
  9. Brenita Jenkins
  10. Larry Vang
  11. Estevão Scudese
  12. Bryanna Shao
  13. Ashlesha Kadam
  14. Jianqiang Shao
  15. Andrea G. Marshall
  16. Amber Crabtree
  17. Benjamin Kirk
  18. Alice Koh
  19. Genesis Wilson
  20. Ashton Oliver
  21. Taylor Rodman
  22. Kinuthia Kabugi
  23. Ho-Jin Koh
  24. Quinton Smith
  25. Elma Zaganjor
  26. Celestine N. Wanjalla
  27. Chandravanu Dash
  28. Chantell Evans
  29. Mark A. Phillips
  30. David Hubert
  31. Olujimi Ajijola
  32. Aaron Whiteside
  33. Young Do Koo
  34. André Kinder
  35. Mert Demirci
  36. Claude F. Albritton
  37. Nelson Wandira
  38. Sydney Jamison
  39. Taseer Ahmed
  40. Mohammad Saleem
  41. Dhanendra Tomar
  42. Clintoria R. Williams
  43. Mariya T. Sweetwyne
  44. Sandra A. Murray
  45. Anthonya Cooper
  46. Annet Kirabo
  47. Pooja Jadiya
  48. Anita Quintana
  49. Prasanna Katti
  50. Dao□Fu Dai
  51. Melanie R. McReynolds
  52. Antentor Hinton
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Abstract

The kidney filters nutrient waste and bodily fluids from the bloodstream, in addition to secondary functions of metabolism and hormone secretion, requiring an astonishing amount of energy to maintain its functions. In kidney cells, mitochondria produce adenosine triphosphate (ATP) and help maintain kidney function. Due to aging, the efficiency of kidney functions begins to decrease. Dysfunction in mitochondria and cristae, the inner folds of mitochondria, is a hallmark of aging. Therefore, age-related kidney function decline could be due to changes in mitochondrial ultrastructure, increased reactive oxygen species (ROS), and subsequent alterations in metabolism and lipid composition. We sought to understand if there is altered mitochondrial ultrastructure, as marked by 3D morphological changes, across time in tubular kidney cells. Serial block facing-scanning electron microscope (SBF-SEM) and manual segmentation using the Amira software were used to visualize murine kidney samples during the aging process at 3 months (young) and 2 years (old). We found that 2-year mitochondria are more fragmented, compared to the 3-month, with many uniquely shaped mitochondria observed across aging, concomitant with shifts in ROS, metabolomics, and lipid homeostasis. Furthermore, we show that the mitochondrial contact site and cristae organizing system (MICOS) complex is impaired in the kidney due to aging. Disruption of the MICOS complex shows altered mitochondrial calcium uptake and calcium retention capacity, as well as generation of oxidative stress. We found significant, detrimental structural changes to aged kidney tubule mitochondria suggesting a potential mechanism underlying why kidney diseases occur more readily with age. We hypothesize that disruption in the MICOS complex further exacerbates mitochondrial dysfunction, creating a vicious cycle of mitochondrial degradation and oxidative stress, thus impacting kidney health.

Translational Statement

Due to aging, the efficiency of kidney functions begins to decrease and the risk of kidney diseases may increase, but specific regulators of mitochondrial age-related changes are poorly explained. This study demonstrates the MICOS complex may be a target for mitigating age-related changes in mitochondria. The MICOS complex can be associated with oxidative stress and calcium dysregulation, which also arise in many kidney pathologies.

Graphical Abstract

Kidney aging causes a decline in the MICOS complex, concomitant with metabolic, lipidomic, and mitochondrial structural alterations.

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  1. Version published to 10.1101/2024.06.09.598108v2 on bioRxiv
  2. Version published to 10.1101/2024.06.09.598108v1 on bioRxiv