How Mitochondrial Dysfunction Fuels
Cancer, Diabetes & Insulin Resistance
Professor Thomas Seyfried Discussion about the damaging effects
of poor nutrition on mitochondrial function, insulin resistance, and the increased
risk of cancer & diabetes. We explore how chronic inflammation,
insulin resistance, and lifestyle factors contribute to
mitochondrial dysfunction.
Diabetes
Impedes Mitochondrial
ATP Energy Production
Mitochondrial dysfunction drives
diabetes by crippling energy (ATP)
production, leading to fat buildup (lipotoxicity)
that blocks insulin signaling (insulin
resistance)
in muscle/liver, and causing beta-cell
failure
in the pancreas, preventing proper
insulin release, all while generating
excess reactive
oxygen species (ROS)
that further damage cells, a cycle
worsening glucose control in both Type 1
and Type 2 diabetes.
How it works:
Energy Metabolism
Disruption: Mitochondria fail to produce
enough ATP, starving energy-demanding cells
in the pancreas, liver, and muscles,
hindering their function.
Insulin
Resistance:
In muscle and liver, dysfunctional
mitochondria can't burn fats efficiently,
leading to fat accumulation (lipotoxicity)
that interferes with insulin's ability to
signal cells to take up glucose, causing
resistance.
Beta-Cell
Dysfunction:
Impaired mitochondria in pancreatic
beta-cells can't sense glucose or produce
enough insulin, leading to insufficient
secretion, a core problem in diabetes.
Oxidative Stress:
Faulty mitochondria generate excessive ROS
(free radicals), damaging cellular
components, worsening insulin resistance,
and pushing beta-cells towards failure.
Mitochondrial Dysfunction in Diabetes: Shedding
Light on a Widespread Oversight
February 13, 2025
Abstract
Diabetes mellitus
represents a complicated metabolic condition
marked by ongoing hyperglycemia arising from
impaired insulin secretion, inadequate insulin
action, or a combination of both. Mitochondrial
dysfunction has emerged as a significant
contributor to the aetiology of diabetes,
affecting various metabolic processes critical
for glucose homeostasis.
This review aims to
elucidate the complex link between mitochondrial
dysfunction and diabetes, covering the spectrum
of diabetes types, the role of mitochondria in
insulin resistance, highlighting
pathophysiological mechanisms, mitochondrial DNA
damage, and altered mitochondrial biogenesis and
dynamics. Additionally, it discusses the
clinical implications and complications of
mitochondrial dysfunction in diabetes and its
complications, diagnostic approaches for
assessing mitochondrial function in diabetics,
therapeutic strategies, future directions, and
research opportunities.
Mitochondrial
Dysfunction, Oxidative Stress, and Inter-Organ
Miscommunications in T2D Progression
January 25, 2024
Abstract
Type 2 diabetes (T2D) is a heterogenous disease,
and conventionally, peripheral insulin
resistance (IR) was thought to precede islet
β-cell dysfunction, promoting progression from
prediabetes to T2D. New evidence suggests that
T2D-lean individuals experience early β-cell
dysfunction without significant IR. Regardless
of the primary event (i.e., IR vs. β-cell
dysfunction) that contributes to dysglycemia,
significant early-onset oxidative damage and
mitochondrial dysfunction in multiple metabolic
tissues may be a driver of T2D onset and
progression.
Oxidative stress, defined as the generation of
reactive oxygen species (ROS), is mediated by
hyperglycemia alone or in combination with
lipids. Physiological oxidative stress promotes
inter-tissue communication, while pathological
oxidative stress promotes inter-tissue
mis-communication, and new evidence suggests
that this is mediated via extracellular vesicles
(EVs), including mitochondria containing EVs.
Under metabolic-related stress conditions,
EV-mediated cross-talk between β-cells and
skeletal muscle likely trigger mitochondrial
anomalies leading to prediabetes and T2D.
This article reviews the underlying molecular
mechanisms in ROS-related pathogenesis of
prediabetes, including mitophagy and
mitochondrial dynamics due to oxidative stress.
Further, this review will describe the potential
of various therapeutic avenues for attenuating
oxidative damage, reversing prediabetes and
preventing progression to T2D.
Mitophagy and
mitochondrial dynamics in type 2 diabetes
mellitus treatment
March 24, 2022
Abstract
The prevalence of type 2
diabetes is associated with inflammatory bowels
diseases, nonalcoholic steatohepatitis and even
a spectrum of cancer such as colon cancer and
liver cancer, resulting in a substantial
healthcare burden on our society. Autophagy is a
key regulator in metabolic homeostasis such as
lipid metabolism, energy management and the
balance of cellular mineral substances.
Mitophagy is selective
autophagy for clearing the damaged mitochondria
and dysfunctional mitochondria. A myriad of
evidence has demonstrated a major role of
mitophagy in the regulation of type 2 diabetes
and metabolic homeostasis. It is well
established that defective mitophagy has been
linked to the development of insulin resistance.
Moreover, insulin resistance is further
progressed to various diseases such as
nephropathy, retinopathy and cardiovascular
diseases. Concordantly, restoration of mitophagy
will be a reliable and therapeutic target for
type 2 diabetes.
Recently, various
phytochemicals have been proved to prevent
dysfunctions of β-cells by mitophagy inductions
during diabetes developments. In agreement with
the above phenomenon, mitophagy inducers should
be warranted as potential and novel therapeutic
agents for treating diabetes. This review
focuses on the role of mitophagy in type 2
diabetes relevant diseases and the
pharmacological basis and therapeutic potential
of autophagy regulators in type 2 diabetes.
Mitochondrial
dysfunction in type 2 diabetes mellitus: an
organ-based analysis
February 1, 2019
Abstract
Type 2 diabetes mellitus
(T2DM) is a systemic disease characterized by
hyperglycemia, hyperlipidemia, and organismic
insulin resistance. This pathological shift in
both circulating fuel levels and energy
substrate utilization by central and peripheral
tissues contributes to mitochondrial dysfunction
across organ systems. The mitochondrion lies at
the intersection of critical cellular pathways
such as energy substrate metabolism, reactive
oxygen species (ROS) generation, and apoptosis.
It is the disequilibrium of these processes in
T2DM that results in downstream deficits in
vital functions, including hepatocyte
metabolism, cardiac output, skeletal muscle
contraction, β-cell insulin production, and
neuronal health.
Although mitochondria
are known to be susceptible to a variety of
genetic and environmental insults, the
accumulation of mitochondrial DNA (mtDNA)
mutations and mtDNA copy number depletion is
helping to explain the prevalence of
mitochondrial-related diseases such as T2DM.
Recent work has uncovered novel mitochondrial
biology implicated in disease progressions such
as mtDNA heteroplasmy, noncoding RNA (ncRNA),
epigenetic modification of the mitochondrial
genome, and epitranscriptomic regulation of the
mtDNA-encoded mitochondrial transcriptome.
The goal of this review
is to highlight mitochondrial dysfunction
observed throughout major organ systems in the
context of T2DM and to present new ideas for
future research directions based on novel
experimental and technological innovations in
mitochondrial biology. Finally, the field of
mitochondria-targeted therapeutics is discussed,
with an emphasis on novel therapeutic strategies
to restore mitochondrial homeostasis in the
setting of T2DM.
2017 Society for Free Radical
Biology and Medicine
Mitochondrial
dynamics in type 2 diabetes:
Pathophysiological implications
April 11, 2017
Abstract
Mitochondria
play a key role in maintaining cellular
metabolic homeostasis. These organelles
have a high plasticity and are involved
in dynamic processes such as
mitochondrial fusion and fission,
mitophagy and mitochondrial biogenesis.
Type 2 diabetes is characterised by
mitochondrial dysfunction, high
production of reactive oxygen species
(ROS) and low levels of ATP.
Mitochondrial fusion is modulated by
different proteins, including
mitofusin-1 (MFN1), mitofusin-2 (MFN2)
and optic atrophy (OPA-1), while fission
is controlled by mitochondrial fission 1
(FIS1), dynamin-related protein 1 (DRP1)
and mitochondrial fission factor (MFF).
PARKIN and (PTEN)-induced putative
kinase 1 (PINK1) participate in the
process of mitophagy, for which
mitochondrial fission is necessary. In
this review, we discuss the molecular
pathways of mitochondrial dynamics,
their impairment under type 2 diabetes,
and pharmaceutical approaches for
targeting mitochondrial dynamics, such
as mitochondrial division inhibitor-1
(mdivi-1), dynasore, P110 and
15-oxospiramilactone.
Furthermore, we
discuss the pathophysiological
implications of impaired mitochondrial
dynamics, especially in type 2 diabetes.
Mitochondrial
dysfunction and insulin resistance: an
update
March 4, 2015
Abstract
Mitochondrial
dysfunction has been implicated in the
development of insulin resistance (IR);
however, a large variety of association
and intervention studies as well as
genetic manipulations in rodents have
reported contrasting results. Indeed,
even 39 years after the first
publication describing a relationship
between IR and diminished mitochondrial
function, it is still unclear whether a
direct relationship exists, and more
importantly if changes in mitochondrial
capacity are a cause or consequence of
IR.
This review will
take a journey through the past and
summarise the debate about the
occurrence of mitochondrial dysfunction
and its possible role in causing
decreased insulin action in obesity and
type 2 diabetes. Evidence is presented
from studies in various human
populations, as well as rodents with
genetic manipulations of pathways known
to affect mitochondrial function and
insulin action. Finally, we have
discussed whether mitochondria are a
potential target for the treatment of
IR.
Curr Pharm Des. 2013 Feb 20
. Mitochondrial dysfunction and
oxidative stress in insulin resistance
Abstract
Evidence is mounting of the involvement of mitochondrial
dysfunction in insulin resistance, diabetes and
associated complications. This review aims to provide an
overview of the effects of insulin resistance on
mitochondrial function in several tissues. We consider
the pathogenesis of insulin resistance from a
mitochondrial perspective and contemplate potential
beneficial effects of strategies aimed at modulating
mitochondrial function in insulin resistance, including
insulin and insulin-sensitizing drugs, antioxidants, and
selectively targeting antioxidants to mitochondria.
Mitochondrial function is fundamental to metabolic
homeostasis. In addition to converting nutrient flux
into energy molecule ATP, the mitochondria generate
intermediates for biosynthesis and reactive oxygen
species (ROS) that serves as a secondary messenger to
mediate signaling transduction and metabolism.
Alterations of mitochondrial function, dynamics and
biogenesis have been observed in various metabolic
disorders including aging, cancer, diabetes and obesity.
However, the mechanisms responsible for mitochondrial
changes and the pathways leading to metabolic disorders
remain to be defined. In the last few years, tremendous
efforts have been devoted to addressing these complex
questions and led to significant progress. In a timely
manner, the Forum on Mitochondria and Metabolic
Homeostasis intends to document the latest findings in
both original research article and review articles, with
the focus on addressing three major complex issues:
(1)
mitochondria
and mitochondrial oxidants in aging - the oxidant theory
(including mitochondrial ROS) being revisited by a
hyperfunction hypothesis and a novel role of SMRT in
mitochondria-mediated aging process being discussed;
.
(2) impaired mitochondrial capacity (e.g., fatty acid
oxidation, OXPHOS for ATP synthesis) and plasticity
(e.g., the response to endocrine and metabolic
challenges, and to calorie restriction) in diabetes and
obesity; .
(3) mitochondrial energy adaption in cancer progression
- a new view being provided for H+-ATP synthase in
regulating cell cycle and proliferation by mediating
mitochondrial OXPHOS, oxidant production, and cell death
signaling. It is anticipated that this timely Forum will
advance our understanding of mitochondrial dysfunction
in metabolic disorders.
Obesity increases the risk for type 2 diabetes through
induction of insulin resistance. Treatment of type 2
diabetes has been limited by little translational
knowledge of insulin resistance although there have been
several well-documented hypotheses for insulin
resistance. In those hypotheses, inflammation,
mitochondrial dysfunction, hyperinsulinemia and
lipotoxicity have been the major concepts and have
received a lot of attention. Oxidative stress,
endoplasmic reticulum (ER) stress, genetic background,
aging, fatty liver, hypoxia and lipodystrophy are active
subjects in the study of these concepts.
However, none
of those concepts or views has led to an effective
therapy for type 2 diabetes. The reason is that there
has been no consensus for a unifying mechanism of
insulin resistance. In this review article, literature
is critically analyzed and reinterpreted for a new
energy-based concept of insulin resistance, in which
insulin resistance is a result of energy surplus in
cells. The energy surplus signal is mediated by ATP and
sensed by adenosine monophosphate-activated protein
kinase (AMPK) signaling pathway. Decreasing ATP level by
suppression of production or stimulation of utilization
is a promising approach in the treatment of insulin
resistance. In support, many of existing insulin
sensitizing medicines inhibit ATP production in
mitochondria.
The effective therapies such as weight
loss, exercise, and caloric restriction all reduce ATP
in insulin sensitive cells. This new concept provides a
unifying cellular and molecular mechanism of insulin
resistance in obesity, which may apply to insulin
resistance in aging and lipodystrophy
Relationships between Mitochondrial Function
and
Metabolic Flexibility in Type 2 Diabetes Mellitus
Abstract
INTRODUCTION: Mitochondrial
dysfunction, lipid accumulation, insulin resistance and
metabolic inflexibility have been implicated in the
etiology of type 2 diabetes (T2D), yet their
interrelationship remains speculative. We investigated
these interrelationships in a group of T2D and obese
normoglycemic control subjects.
METHODS: 49 non-insulin dependent male
T2D patients and 54 male control subjects were enrolled,
and a hyperinsulinemic-euglycemic clamp and indirect
calorimetry were performed. A muscle biopsy was taken
and intramyocellular lipid (IMCL) was measured. In vivo
mitochondrial function was measured by PCr recovery in
30 T2D patients and 31 control subjects.
RESULTS: Fasting NEFA levels were
significantly elevated in T2D patients compared with
controls, but IMCL was not different. Mitochondrial
function in T2D patients was compromised by 12.5%
(p<0.01). Whole body glucose disposal (WGD) was higher
at baseline and lower after insulin stimulation.
Metabolic flexibility (ΔRER) was lower in the type 2
diabetic patients (0.050±0.033 vs. 0.093±0.050, p<0.01).
Mitochondrial function was the sole predictor of basal
respiratory exchange ratio (RER) (R(2) = 0.18, p<0.05);
whereas WGD predicted both insulin-stimulated RER (R(2)
= 0.29, p<0.001) and metabolic flexibility (R(2) = 0.40,
p<0.001).
CONCLUSIONS: These results indicate
that defects in skeletal muscle in vivo mitochondrial
function in type 2 diabetic patients are only reflected
in basal substrate oxidation and highlight the
importance of glucose disposal rate as a determinant of
substrate utilization in response to insulin.
In pancreatic β cells, mitochondria play a central role
in coupling glucose metabolism to insulin exocytosis,
thereby ensuring strict control of glucose-stimulated
insulin secretion. Defects in mitochondrial function
impair this metabolic coupling, and ultimately promote
apoptosis and β cell death. Various factors have been
identified that may contribute to mitochondrial
dysfunction.
In this review we address the emerging
concept of complex links between these factors. We also
discuss the role of the mitochondrial genome and
mutations associated with diabetes, the effect of
oxidative stress and reactive oxygen species, the
sensitivity of mitochondria to lipotoxicity, and the
adaptive dynamics of mitochondrial morphology.
Better
comprehension of the molecular mechanisms contributing
to mitochondrial dysfunction will help drive the
development of effective therapeutic approaches.
Mitochondrial dysfunction in diabetes: from molecular
mechanisms
to functional significance and therapeutic
opportunities
Abstract
Given their essential function in aerobic metabolism,
mitochondria are intuitively of interest in regard to
the pathophysiology of diabetes. Qualitative,
quantitative, and functional perturbations in
mitochondria have been identified and affect the cause
and complications of diabetes.
Moreover, as a
consequence of fuel oxidation, mitochondria generate
considerable reactive oxygen species (ROS). Evidence is
accumulating that these radicals per se are important in
the pathophysiology of diabetes and its complications.
In this review, we first present basic concepts
underlying mitochondrial physiology. We then address
mitochondrial function and ROS as related to diabetes.
We consider different forms of diabetes and address both
insulin secretion and insulin sensitivity. We also
address the role of mitochondrial uncoupling and
coenzyme Q.
Finally, we address the potential for
targeting mitochondria in the therapy of diabetes.
Mitochondrial
dysfunction in type 2 diabetes and obesity
Abstract
Insulin resistance in skeletal muscle is a major
hallmark of type 2 diabetes mellitus (T2D) and obesity
that is characterized by impaired insulin-mediated
glucose transport and glycogen synthesis and by
increased intramyocellular content of lipid metabolites.
Several studies have provided evidence for mitochondrial
dysfunction in skeletal muscle of type 2 diabetic and prediabetic subjects, primarily due to a lower content
of mitochondria (mitochondrial biogenesis) and possibly
to a reduced functional capacity per mitochondrion.
This
article discusses the latest advances in the
understanding of the molecular mechanisms underlying
insulin resistance in human skeletal muscle in T2D and
obesity, with a focus on possible links between insulin
resistance and mitochondrial dysfunction.
