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Difference between revisions of "SUIT-026 O2 mt D063"

From Bioblast
(Created page with "{{MitoPedia |abbr=RET (Respiratory control) |description=400px |info='''A''' - '''SUIT-026''' |application=AmR |SUIT number=D064_1S;2Rot...")
 
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::: '''[[SUIT protocol pattern]]:'''  1S;2Rot;3D;4Ama
::: '''[[SUIT protocol pattern]]:'''  1S;2Rot;3D;4Ama


SUIT-026 AmR mt D063 has been designed to serve as a respiratory control of the [[SUIT-026 AmR mt D063]]study the [[Reverse_electron_flow_from_CII_to_CI| RET]] production of ROS in isolated mitochondria. The protocol is focused on [[LEAK]] state for the [[S-pathway]] to provide the conditions of high membrane potential, redox power in the Q-junction and no presence of reduced NADH. Under these conditions, in several samples has been described that a reverse flow of the electrons into the membrane arm and the quinone binding site of the Complex I occurs, promoting the production of ROS. The addition of [[rotenone]] provides excellent control to this mechanism because this compound blocks the point on which the electrons leak from the Complex I. The last step, the titration of ADP at saturating concentrations to reach [[OXPHOS]] allow us to harmonize this protocol with [[SUIT-006 O2 mt D022]] for quality control and a full assessment of the coupling control.
SUIT-026 O2 mt D063 has been designed to serve as a respiratory control of the [[SUIT-026 AmR mt D064]] study the [[Reverse_electron_flow_from_CII_to_CI| RET]] production of ROS in isolated mitochondria. The protocol is focused on [[LEAK]] state for the [[S-pathway]] to provide the conditions of high membrane potential, redox power in the Q-junction and no presence of reduced NADH. Under these conditions, in several samples has been described that a reverse flow of the electrons into the membrane arm and the quinone binding site of the Complex I occurs, promoting the production of ROS. The addition of [[rotenone]] provides excellent control to this mechanism because this compound blocks the point on which the electrons leak from the Complex I. The last step, the titration of ADP at saturating concentrations to reach [[OXPHOS]], allow us to harmonize this protocol with [[SUIT-006 O2 mt D022]] for quality control and a full assessment of the coupling control.




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  Communicated by  [[Iglesias-Gonzalez J]] and [[Gnaiger E]] (last update 2019-06-26)
  Communicated by  [[Iglesias-Gonzalez J]] and [[Gnaiger E]] (last update 2019-06-26)


{{Template:SUIT-026 AmR mt D062}}
{{Template:SUIT-026 O2 mt D063}}


== Strengths and limitations ==
== Strengths and limitations ==
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== Compare SUIT protocols ==
== Compare SUIT protocols ==
 
::::* [[SUIT-006 O2 mt D022]]: CCP mtprep for S-pathway.
::::* [[SUIT-026 AmR mt D064]]: Protocol to evaluate the RET production of ROS.




Revision as of 12:43, 26 June 2019


high-resolution terminology - matching measurements at high-resolution


SUIT-026 O2 mt D063

Description

SUIT-026 AmR mt D064.png

Abbreviation: RET (Respiratory control)

Reference: A - SUIT-026

SUIT number: D064_1S;2Rot;3D;4Ama

O2k-Application: AmR

MitoPedia: SUIT - Protocol for the respiratory control of SUIT-026 AmR mt D064
SUIT protocol pattern: 1S;2Rot;3D;4Ama

SUIT-026 O2 mt D063 has been designed to serve as a respiratory control of the SUIT-026 AmR mt D064 study the RET production of ROS in isolated mitochondria. The protocol is focused on LEAK state for the S-pathway to provide the conditions of high membrane potential, redox power in the Q-junction and no presence of reduced NADH. Under these conditions, in several samples has been described that a reverse flow of the electrons into the membrane arm and the quinone binding site of the Complex I occurs, promoting the production of ROS. The addition of rotenone provides excellent control to this mechanism because this compound blocks the point on which the electrons leak from the Complex I. The last step, the titration of ADP at saturating concentrations to reach OXPHOS, allow us to harmonize this protocol with SUIT-006 O2 mt D022 for quality control and a full assessment of the coupling control. 


Communicated by  Iglesias-Gonzalez J and Gnaiger E (last update 2019-06-26)
MitoPedia: SUIT

Steps and respiratory states

1S;2Rot;3D;4Ama.png


Step State Pathway Q-junction Comment - Events (E) and Marks (M)
1S SL(n) S CII 1S
2Rot SL(n) S CII 1S;2Rot
3D SP S CII 1S;2Rot;3D
3c SP S CII 1S;2Rot;3D;3c
4Ama ROX 1S;2Rot;3D;3c;4Ama
  • Rox is the residual oxygen consumption in the ROX state, due to oxidative side reactions, estimated after addition of antimycin A (inhibitor of CIII). Rox is subtracted from oxygen flux as a baseline for all respiratory states, to obtain mitochondrial respiration (mt).


Questions.jpg


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Bioblast links: SUIT protocols - >>>>>>> - Click on [Expand] or [Collapse] - >>>>>>>
MitoPedia: SUIT
Coupling control
» Coupling control state
» ET capacity
» OXPHOS capacity
» LEAK respiration
Pathway control
» Electron transfer pathway
» Fatty acid oxidation pathway control state, F
» NADH electron transfer-pathway state, N
» Succinate pathway control state, S
» NS-pathway control state, NS
» Glycerophosphate pathway control state, Gp
» Complex IV single step, CIV
» Anaplerotic pathway control state
Main fuel substrates
» Glutamate, G
» Glycerophosphate, Gp
» Malate, M
» Octanoylcarnitine, Oct
» Pyruvate, P
» Succinate, S
Glossary
» List of SUIT states
» SUIT concept

Strengths and limitations

Compare SUIT protocols


References

MitoPedia concepts: SUIT protocol, SUIT A, Find 


MitoPedia methods: Fluorometry 




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