A key contributor to insulin-mediated glucose uptake is insulin-induced vasodilation of skeletal muscle arterioles, which is impared with obesity and Type 2 diabetes (T2D). Abnormalities in the vascular reactivity to insulin can limit perfusion, and delivery of glucose and insulin to muscle tissue. In human patients with T2D, exercise improves insulin sensitivity and glucose uptake T2D. Furthermore, we have previously shown that daily exercise prevents impairments in insulin-induced vasodilation in OLETF rats. However, the efficacy of exercise interventions which utilize different muscle recruitment patterns (i.e. aerobic vs. sprint training) to ameliorate or reverse impairments in microvascular insulin reactivity has not been elucidated. The current ADA standard of care for T2D is treatment with metformin in combination with a diet and exercise program. Therefore, we studied the effects of endurance exercise and interval sprint training with and without metformin on the vasoreactivity to insulin in skeletal muscle arterioles from red and white muscles

Crissey, Jacqueline M.

Jenkins, Nathan T.

Laughlin, M. Harold

Padilla, Jaume

Thyfault, John P.

English

University of Missouri: MOspace

Body	  Composi+on	  and	  HbA1c	  (Fig.	  1):	  • 	  Body	  weight	  was	  reduced	  in	  all	  treatment	  groups,	  and	  %body	  fat	  was	  decreased	  in	  all	  exercise	  rats.	  • 	  Metformin	  &	  interval	  sprint	  training	  reduced	  body	  weight	  and	  %body	  fat	  more	  than	  interval	  sprint	  training	  alone.	  • 	  HbA1c	  was	  reduced	  in	  all	  treatment	  groups.	  Insulin-­‐Induced	  Vasodila+on,	  &	  ET-­‐1	  Blockade	  (Fig.	  2	  &	  3):	  • 	  Endurance	  exercise	  selectively	  improved	  insulin-­‐induced	  vasodilation	  in	  arterioles	  perfusing	  the	  high	  oxidative,	  red	  portion	  of	  the	  gastrocnemius	  muscle.	  	  • 	  ET-­‐1	  blockade	  normalized	  differences	  between	  groups,	  suggesting	  that	  improvements	  in	  the	  dilatory	  effects	  of	  insulin	  with	  exercise	  are	  ET-­‐1	  dependent.	  • 	  Effects	  of	  interval	  sprint	  training	  on	  insulin-­‐induced	  vasodilation	  in	  the	  white	  portion	  of	  the	  gastrocnemius,	  only	  occurred	  with	  ET-­‐1	  blockade,	  suggesting	  that	  ET-­‐1	  vasoconstriction	  prevented	  insulin-­‐induced	  vasodilation	  in	  arterioles	  perfusing	  low	  oxidative	  muscle.	  	  • 	  Effects	  of	  exercise	  on	  insulin-­‐induced	  vasodilation	  were	  mainly	  abolished	  in	  rats	  treated	  with	  Metformin.	  Ach-­‐Induced	  Vasodila+on	  (Fig.	  4):	  • 	  Endurance	  exercise	  and	  interval	  sprint	  training	  improved	  ACh-­‐induced	  vasodilation	  in	  arterioles	  perfusing	  the	  high	  oxidative	  red	  portion	  of	  the	  gastrocnemius	  muscle;	  whereas	  improvements	  in	  the	  low	  oxidative	  white	  portion	  of	  the	  muscle	  was	  only	  found	  with	  endurance	  exercise.	  1.	  ABSTRACT	  4.	  RESULTS	  6.	  CONCLUSIONS	  2.	  INTRODUCTION	  ACKNOWLEDGEMENTS	  Supported	  by	  the	  MU	  Life	  Sciences	  Fellowship,	  T32-­‐AR48523,	  11POST5080002,	  NIH	  RO1HL036088,	  and	  VA	  CDA-­‐2	  IK2BX001299-­‐01.	  	  The	  authors	  thank	  Dr	  R.	  Scott	  Rector	  for	  the	  HbA1c	  data,	  and	  Pam	  Thorne	  for	  all	  of	  her	  technical	  assistance.	  	   Endurance or Sprint Interval Exercise, & Metformin Treatment Differently Modify Insulin-Induced Vasodilation in Skeletal Muscle Arterioles of Obese Insulin Resistant Rats Jacqueline M. Crissey1, Jaume Padilla1, Nathan T. Jenkins1,  Jeffrey S. Martin1, John P. Thyfault 1,2,3,4, and Maurice H. Laughlin1 Departments of 1Biomedical Sciences, 2Internal Medicine, 3Nutrition and Exercise Physiology, and 4Harry S Truman VA Memorial Hospital, University of Missouri, Columbia, MO REFERENCES	  1.	  Kirwan	  JP,	  et	  al.	  Am	  J	  Physiol-­Endoc	  M,	  2009.	  2.	  Mikus	  CR,	  et	  al.	  J	  Appl	  Physiol	  ,	  2010.	  3.	  American	  Diabetes	  Association.	  Diabetes	  Care,	  2011.	  5.	  SUMMARY	  3.	  METHODS	  Insulin-­‐induced	   vasodilation	   is	   obligatory	   for	   glucose	   disposal,	   and	   is	  impaired	   with	   insulin	   resistance.	   We	   examined	   the	   effects	   of	   endurance	  (EXT)	   and	   interval	   sprint	   (IST)	   exercise	   training	   with	   and	   without	  metformin	   (MET)	   treatment	   on	   acetylcholine	   (ACh)	   and	   insulin-­‐induced	  vasodilation	   in	  skeletal	  muscle	  arterioles	  of	  high	  and	   low	  oxidative	  muscle	  from	  obese,	  insulin	  resistant	  OLETF	  rats.	  Rats	  remained	  sedentary	  (SED),	  or	  were	   treated	   with	   EXT,	   IST,	   MET,	   EXT+MET,	   or	   IST+MET	   from	   20-­‐32wks	  (n=11-­‐13).	   At	   sacribice,	   2nd	   order	   arterioles	   from	   red	   (G2AR)	   and	   white	  (G2AW)	   gastrocnemius	   muscle	   were	   isolated	   for	   in	   vitro	   assessment	   of	  vasomotor	   responses	   to	   ACh	   (10-­‐9-­‐10-­‐4	   M),	   insulin	   (1-­‐1000	   µIU/mL),	   and	  insulin	  (1-­‐1000	  µIU/mL)	  +	  tezosentan	  (ET-­‐1	  antagonist;	  3	  μM).	  EXT	  and	  IST	  enhanced	  ACh	  responses	   in	  both	  G2AR	  and	  G2AW	  to	  a	  greater	  extent	   than	  MET	   alone	   (all	   p<0.05).	   In	   the	   G2AR,	   EXT	   improved	   insulin-­‐induced	  vasodilation	   compared	   to	   IST,	   while	   MET	   was	   greater	   than	   IST	   alone	   (all	  p<0.05).	   ET-­‐1	   blockade	   improved	   insulin-­‐induced	   vasodilation	   in	   IST	  compared	   to	  EXT,	   and	  MET	   in	   the	  G2AW,	  whereas	   IST+MET	  exhibited	   less	  vasodilation	  compared	  to	  IST	  (all	  p<0.05).	  In	  conclusion,	  the	  effects	  of	  EXT	  and	   IST	   on	   insulin-­‐induced	   vasodilation	   in	   2A	   arterioles	   of	   low	   and	   high	  oxidative	   muscle	   bibers	   are	   similar;	   but	   the	   mechanisms	   appear	   to	   be	  different.	   EXT	   selectively	   improved	   insulin-­‐induced	   vasodilation	   in	   G2AR,	  and	  was	  not	   affected	  by	  ET-­‐1	  blockade,	   suggesting	   it	   is	  mediated	  by	  nitric	  oxide.	   Conversely,	   no	   insulin-­‐induced	   vasodilation	   was	   observed	   in	   the	  G2AW	  following	  IST,	  yet	  a	  marked	  vasodilation	  occurred	  with	  insulin	  +	  ET-­‐1	  blockade.	  Overall	   these	  data	  suggest	   that	   the	   type	  of	  exercise	   training,	  and	  treatment	  with	  MET,	   have	   differential	   effects	   on	   ACh-­‐	   and	   insulin-­‐induced	  vasodilation	   in	   skeletal	   muscle	   arterioles	   perfusing	   high	   vs.	   low	   oxidative	  muscle	  bibers	  in	  the	  obese,	  insulin	  resistant	  OLETF	  rat.	  	  37O C Video Caliper Circulating Water Bath Inverted  Microscope Vessel Fluid Reservoir Monitor Otsuka	  Long	  Evans	  Tokushima	  FaXy	  (OLETF)	  rats:	  • Mutant	  CCK	  Receptor	  	  	  • Hyperphagic/obese	  	  • Insulin	  resistant	  by	  12-­‐13	  wks	  • Type	  2	  Diabetes	  by	  30-­‐40	  wks	  We	  assessed	  in-­vitro	  vasomotor	  	  responses	  to	  ACh,	  Insulin,	  Insulin	  +	  Tezosentan	  (ET-­‐1	  blockade),	  &	  SNP.	  	  Statistics:	  We	  used	  a	  repeated	  measures	  ANOVA,	  with	  post	  hoc	  tests	  for	  simple	  effects	  of	  group	  for	  the	  dose	  responses	  curves	  with	  a	  correction	  for	  multiple	  comparisons	  (P=0.0167);	  and	  one	  way	  ANOVAs,	  with	  Tukey	  post-­‐hoc	  tests,	  for	  body	  composition	  and	  HbA1c.	  	  	   A	   key	   contributor	   to	   insulin-­‐mediated	   glucose	  uptake	   is	   insulin-­‐induced	   vasodilation	   of	   skeletal	  muscle	  arterioles,	  which	  is	  impaired	  with	  obesity	  and	  Type	  2	  diabetes	  (T2D).	   	  Abnormalities	  in	  the	  vascular	  reactivity	   to	   insulin	   can	   limit	   perfusion,	   and	  delivery	  of	   glucose	   and	   insulin	   to	   muscle	   tissue.	   In	   human	  patients	   with	   T2D,	   exercise	   improves	   insulin	  sensitivity	  and	  glucose	  uptake	  T2D	  (1).	  Furthermore,	  we	  have	  previously	  shown	  that	  daily	  exercise	  prevents	  impairments	  in	  insulin-­‐induced	  vasodilation	  in	  OLETF	  rats	   (2).	   	   However,	   the	   efbicacy	   of	   exercise	  interventions	   which	   utilize	   different	   muscle	  recruitment	   patterns	   (i.e.	   aerobic	   vs.	   sprint	   training)	  to	   ameliorate	   or	   reverse	   impairments	   in	  microvascular	  insulin	  reactivity	  has	  not	  be	  elucidated.	  	  OBJECTIVE:	  The	  current	  ADA	  standard	  of	  care	  for	  T2D	  is	   treatment	   with	   metformin	   in	   combination	   with	   a	  diet	  and	  exercise	  program	  (3).	  Therefore,	  we	  studied	  the	   effects	   of	   endurance	   exercise	   and	   interval	   sprint	  training,	   with	   and	   without	   metformin	   on	   the	  vasoreactivity	   to	   insulin	   in	   skeletal	  muscle	   arterioles	  from	  red	  and	  white	  muscles.	  	  Six	  groups	  of	  OLETF	  rats:	  	  1.  EXT-­	  (n=11)-­	  From	  20-­‐30wks:	  treadmill	  	  running	  	  	  	  30	  m/min,	  (15	  %	  grade),	  60	  min,	  5	  d/wk.	  	  2.  IST-­	  (n=12)-­	  From	  20-­‐30wks:	  treadmill	  run	  2.5	  min	  	  	  	  60m/min	  (15	  %	  grade),	  4.5	  min	  rest–	  x6	  bouts,	  5	  d/wk.	  3.  SED-­	  (n=13)-­	  30wks	  sedentary	  (type	  2D).	  4.  SED+MET-­	  (n=12)-­Metformin	  treatment	  20-­‐30	  wks.	  5. EXT+MET-­	  (n=12)-­Combined	  treatment	  20-­‐30	  wks.	  6.  IST+MET-­	  (n=12)-­	  Combined	  treatment	  20-­‐30	  wks.	  Figure	  3.	  Insulin-­‐induced	  Vasodila+on	  +	  ET-­‐1	  Blockade:	  δ	  EXT	  different	  than	  IST;	  n=11-­‐13/group.	  	  	  	  	  Figure	  1.Body	  Composi+on,	  and	  %HbA1c:	  	  *Signibicantly	  	  different	  than	  SED,	  and	  δ	  different	  than	  IST.	  	  NOTE:	  HbA1c	  n=2-­3/group,	  Body	  composition	  n=11-­‐13/group	  	  	  	  CONTACT:	  jmcrissey@mail.missouri.edu	  Figure	  2.	  Insulin-­‐induced	  Vasodila+on:	  δ	  EXT	  different	  than	  IST;	  n=11-­‐13/group.	  	  	  	  Figure	  4.	  ACh	  Induced	  Vasodila+on:	  *	  EXT	  different	  than	  SED,	  Φ	  IST	  different	  than	  SED,	  and	  δ	  EXT	  different	  than	  IST;	  n=11-­‐13/group.	  	  	  Insulin-­‐induced	  vasodilation	  in	  2nd	  order	  arterioles	  perfusing	  the	  high	  oxidative,	  red	  portion	  of	  the	  gastrocnemius	  muscle	  appear	  to	  be	  most	  responsive	  to	  exercise.	  However,	  these	  effects	  are	  largely	  dependent	  on	  the	  mode	  of	  exercise	  and	  absent	  when	  animals	  are	  concomitantly	  treated	  with	  Metformin.	  

Endurance or sprint interval exercise, & metformin treatment differently modify insulin-induced vasodilation in skeletal muscle arterioles of obese insulin resistant rats

https://mospace.umsystem.edu/xmlui/bitstream/10355/16030/1/InducedVasodilationSkeletalMuscle.pdf

Endurance or sprint interval exercise, & metformin treatment differently modify insulin-induced vasodilation in skeletal muscle arterioles of obese insulin resistant rats

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