Hallmarks of Aging: Difference between revisions

Hallmarks of Aging (view source)

Revision as of 17:12, 2 January 2024

89 bytes added , 2 January

→‎Overview

VisualWikitext

Strimo

Bureaucrats, Administrators

2,851

edits

@@ Line 61: / Line 61: @@
 === The 14 Hallmarks of Aging (2022) ===
-While these nine hallmarks have significantly advanced our understanding of aging and its relation to age-related diseases, recent critiques and evolving scientific evidence have prompted the scientific community to reconsider and expand this framework.{{pmid|34271186}}
+While these nine hallmarks have significantly advanced our understanding of aging and its relation to age-related diseases, recent critiques and evolving scientific evidence have prompted the scientific community to reconsider and expand this framework.{{pmid|34271186}} To address this, a symposium titled “New Hallmarks of Ageing” was held in Copenhagen on March 2022, where leading experts gathered to discuss potential additions and recontextualizations of these aging hallmarks. The symposium highlighted the critical need for an expanded, inclusive paradigm that encompasses newly identified processes contributing to aging. The discussions suggested the integration of five additional hallmarks such as compromised autophagy, dysregulation in RNA splicing, inflammation, loss of cytoskeleton integrity, and disturbance of the microbiome. These potential new hallmarks, along with the original nine, underscore a more comprehensive understanding of the aging process, acknowledging its multifaceted nature and its profound implications for human health and longevity.{{pmid|36040386}}
-To address this, a symposium titled “New Hallmarks of Ageing” was held in Copenhagen on March 2022, where leading experts gathered to discuss potential additions and recontextualizations of these aging hallmarks. The symposium highlighted the critical need for an expanded, inclusive paradigm that encompasses newly identified processes contributing to aging. The discussions suggested the integration of five additional hallmarks such as compromised autophagy, dysregulation in RNA splicing, inflammation, loss of cytoskeleton integrity, and disturbance of the microbiome. These potential new hallmarks, along with the original nine, underscore a more comprehensive understanding of the aging process, acknowledging its multifaceted nature and its profound implications for human health and longevity.{{pmid|36040386}}
 {| class="wikitable"
 !Level
-!
+! colspan="2" |Hallmark
-! Hallmark
 ! Description
+!Proposed
+Year
 !Category
 |-
@@ Line 77: / Line 76: @@
 | style="background-color:hsla(180, 100%, 85%);" |'''Genomic instability'''
 | style="background-color:hsla(180, 100%, 85%);" |Accumulation of DNA damage over time leading to cellular dysfunction.
+|2013
 | rowspan="5" |'''Primary Hallmarks'''
 (causes damage)
@@ Line 83: / Line 83: @@
 | style="background-color:hsla(180, 100%, 85%);" |'''Telomere attrition'''
 | style="background-color:hsla(180, 100%, 85%);" |Reduction in the length of telomeres leading to cellular aging.
+|2013
 |-
 | style="text-align:center; background-color:hsla(180, 100%, 85%);" |[[File:Epigenome-transparent-upscale.png|frameless|85x85px]]
 | style="background-color:hsla(180, 100%, 85%);" |'''Epigenetic alterations'''
 | style="background-color:hsla(180, 100%, 85%);" |Changes in DNA methylation and histone modification affecting gene expression.
+|2013
 |-
 | style="text-align:center; background-color:hsla(180, 100%, 85%);" |[[File:Spinach (RNA).jpg|frameless|75x75px]]
@@ Line 92: / Line 94: @@
 '''(Dysregulation in RNA splicing)'''
 | style="background-color:hsla(180, 100%, 85%);" |Impaired RNA construction from DNA, leading to cellular dysfunction.
+|
 |-
 | style="text-align:center; background-color:hsla(210, 100%, 85%);" |[[File:Stress signaling.png|frameless|95x95px]]
 | style="background-color:hsla(210, 100%, 85%);" |'''Loss of proteostasis'''
 | style="background-color:hsla(210, 100%, 85%);" |Disruption in protein folding and stability leading to cell damage.
+|2013
 |-
 | style="text-align:center; background-color:hsla(210, 100%, 85%);" |[[File:Macro-micro-autophagy.gif|frameless|101x101px]]
 | style="background-color:hsla(210, 100%, 85%);" |'''Compromised autophagy'''
 | style="background-color:hsla(210, 100%, 85%);" | Impaired cellular maintenance through the consumption of own components.
+|
 | rowspan="4" |'''Antagonistic Hallmarks'''
 (responses to damage)
@@ Line 107: / Line 112: @@
 | style="background-color:hsla(0, 100%, 85%);" |'''Deregulated nutrient sensing'''
 | style="background-color:hsla(0, 100%, 85%);" | Alterations in nutrient sensing pathways affecting metabolism and aging.
+|2013
 |-
 | style="text-align:center; background-color:hsla(0, 100%, 85%);" |[[File:Mitochondrion mini.svg|frameless|92x92px]]
 | style="background-color:hsla(0, 100%, 85%);" |'''Mitochondrial dysfunction'''
 | style="background-color:hsla(0, 100%, 85%);" | Decrease in mitochondrial efficiency and increase in oxidative stress.
+|2013
 |-
 | style="text-align:center; background-color:hsla(30, 100%, 85%);" |[[File:DALL·E 2023-10-15 05.28.43 - Photo of senescent cells magnified under a microscope, showing their characteristic enlarged and flattened morphology. The cells are stained with a bl.png|frameless|75x75px]]
 | style="background-color:hsla(30, 100%, 85%);" |[[Senescent Cells|'''Cellular senescence''']]
 | style="background-color:hsla(30, 100%, 85%);" |Accumulation of non-dividing, dysfunctional cells secreting harmful factors.
+|2013
 |-
 | style="text-align:center; background-color:hsla(30, 100%, 85%);" |[[File:Stem cell differentiation.svg|frameless|106x106px]]
 | style="background-color:hsla(30, 100%, 85%);" |'''Stem cell exhaustion'''
 | style="background-color:hsla(30, 100%, 85%);" |Decline in the regenerative capacity of stem cells affecting tissue repair.
+|2013
 | rowspan="5" |'''Integrative Hallmarks'''
 (culprits of the phenotype)
@@ Line 125: / Line 134: @@
 | style="background-color:hsla(30, 100%, 85%);" |'''Altered intercellular communication'''
 | style="background-color:hsla(30, 100%, 85%);" |Changes in cellular communication leading to inflammation and tissue dysfunction.
+|
 |-
 | style="text-align:center; background-color:hsla(30, 100%, 85%);" |[[File:202004 Gut microbiota.svg|frameless|75x75px]]
@@ Line 130: / Line 140: @@
 '''(Dysbiosis)'''
 | style="background-color:hsla(30, 100%, 85%);" |Changes in gut microbiome affecting health and aging.
+|
 |-
 | style="text-align:center; background-color:hsla(30, 100%, 85%);" |[[File:Histopathology of acute and chronic inflammation of the gastro-esophageal junction, annotated.jpg|frameless|75x75px]]
@@ Line 135: / Line 146: @@
 '''(Inflammaging)'''
 | style="background-color:hsla(30, 100%, 85%);" |Systemic inflammation contributing to aging and related diseases.
+|
 |-
 | style="text-align:center; background-color:hsla(30, 100%, 85%);" |[[File:Cell structure (13080952404).jpg|frameless|99x99px]]
 | style="background-color:hsla(30, 100%, 85%);" |'''Altered mechanical properties'''
 | style="background-color:hsla(30, 100%, 85%);" |Changes in cellular and extracellular structure affecting tissue function.
+|2013
 |}