Todd P. Silverstein · 2024 · The Journal of Physical Chemistry B · ACS Publications · added 2026-04-20
In a recent series of papers, James W. Lee reported that mitochondrial oxidative phosphorylation violates the second law of thermodynamics and that it is allowed to do so because it is a "Type-B" proc Show more
In a recent series of papers, James W. Lee reported that mitochondrial oxidative phosphorylation violates the second law of thermodynamics and that it is allowed to do so because it is a "Type-B" process that features lateral and longitudinal membrane asymmetry. We show here that these contentions are based on problematic interpretations of the literature. More reliable values of ΔGredox and ΔGATP synthesis show that the second law is not violated. More recent reports on the structures of the redox-driven proton pumps (Complexes I, III, and IV) suggest that longitudinal membrane asymmetry does not exist. Finally, Lee's predictions for the concentration of protons localized at the P-side surface of the bioenergetic membrane are likely to be much too high due to several errors; thus, his predicted high values of ΔpHsurface that violate the second law are likely to be wrong. There is currently no strong experimental or theoretical evidence to support the contention that oxidative phosphorylation violates the second law of thermodynamics. Show less
Oxaliplatin is successfully used on advanced colorectal cancer to eradicate micro-metastasis,
whereas its benefits in the early stages of colorectal cancer remains controversial since approximately
30 Show more
Oxaliplatin is successfully used on advanced colorectal cancer to eradicate micro-metastasis,
whereas its benefits in the early stages of colorectal cancer remains controversial since approximately
30% of patients experience unexpected relapses. Herein, we evaluate the efficacy of oxidative
phosphorylation as a predictive biomarker of oxaliplatin response in colorectal cancer. We found that
non-responding patients exhibit low oxidative phosphorylation activity, suggesting a poor prognosis.
To reach this conclusion, we analyzed patient samples of individuals treated with oxaliplatin from
the GSE83129 dataset, and a set of datasets validated using ROCplotter, selecting them based on
their response to the drug. By analyzing multiple oxaliplatin-resistant and -sensitive cell lines,
we identified oxidative phosphorylation KEGG pathways as a valuable predictive biomarker of
oxaliplatin response with a high area under the curve (AUC = 0.843). Additionally, some oxidative
phosphorylation-related biomarkers were validated in primary- and metastatic-derived tumorspheres,
confirming the results obtained in silico. The low expression of these biomarkers is clinically relevant,
indicating poor prognosis with decreased overall and relapse-free survival. This study proposes
using oxidative phosphorylation-related protein expression levels as a predictor of responses to
oxaliplatin-based treatments to prevent relapse and enable a more personalized therapy approach.
Our results underscore the value of oxidative phosphorylation as a reliable marker for predicting the
response to oxaliplatin treatment in colorectal cancer. Show less
Metabolic plasticity enables cancer cells to switch between glycolysis and oxidative phosphorylation to adapt to changing conditions during cancer progression, whereas metabolic dependencies limit pla Show more
Metabolic plasticity enables cancer cells to switch between glycolysis and oxidative phosphorylation to adapt to changing conditions during cancer progression, whereas metabolic dependencies limit plasticity. To understand a role for the architectural environment in these processes we examined metabolic dependencies of cancer cells cultured in flat (2D) and organotypic (3D) environments. Here we show that cancer cells in flat cultures exist in a high energy state (oxidative phosphorylation), are glycolytic, and depend on glucose and glutamine for growth. In contrast, cells in organotypic culture exhibit lower energy and glycolysis, with extensive metabolic plasticity to maintain growth during glucose or amino acid deprivation. Expression of KRASG12V in organotypic cells drives glucose dependence, however cells retain metabolic plasticity to glutamine deprivation. Finally, our data reveal that mechanical properties control metabolic plasticity, which correlates with canonical Wnt signaling. In summary, our work highlights that the architectural and mechanical properties influence cells to permit or restrict metabolic plasticity. Show less
Cytochrome c (cyt c) is a small soluble heme protein characterized by a relatively flexible structure, particularly in the ferric form, such that it is able to sample a broad conformational space. Dep Show more
Cytochrome c (cyt c) is a small soluble heme protein characterized by a relatively flexible structure, particularly in the ferric form, such that it is able to sample a broad conformational space. Depending on the specific conditions, interactions, and cellular localization, different conformations may be stabilized, which differ in structure, redox properties, binding affinities, and enzymatic activity. The primary function is electron shuttling in oxidative phosphorylation, and is exerted by the so-called native cyt c in the intermembrane mitochondrial space of healthy cells. Under pro-apoptotic conditions, however, cyt c gains cardiolipin peroxidase activity, translocates into the cytosol to engage in the intrinsic apoptotic pathway, and enters the nucleus where it impedes nucleosome assembly. Other reported functions include cytosolic redox sensing and involvement in the mitochondrial oxidative folding machinery. Moreover, post-translational modifications such as nitration, phosphorylation, and sulfoxidation of specific amino acids induce alternative conformations with differential properties, at least in vitro. Similar structural and functional alterations are elicited by biologically significant electric fields and by naturally occurring mutations of human cyt c that, along with mutations at the level of the maturation system, are associated with specific diseases. Here, we summarize current knowledge and recent advances in understanding the different structural, dynamic, and thermodynamic factors that regulate the primary electron transfer function, as well as alternative functions and conformations of cyt c. Finally, we present recent technological applications of this moonlighting protein. Show less