Haemoglobin mass and running time trial performance after recombinant human erythropoietin administration in trained men

A Lucia; AJ Brien; B Berglund; BD Levine; C Ahlgrim; C Lundby; C Lundby; C Lundby; CC Chang; CP Alfrey; D Boning; Diresibachew H. Wondimu; DL Costill; DP Wilkerson; Elias T. Zambidis; Evangelia Daskalaki; G Banfi; G Ninot; G Russell; GP Millet; H Ehrenreich; I Mujika; JD Belcher; JJ Thomsen; JM Kirkeberg; John D. McClure; Jérôme Durussel; K Heinicke; K Miskowiak; KI Birkeland; L Rice; L Rice; M Audran; M Brines; Martin Anderson; Neal Padmanabhan; NV Olsen; P Connes; P Rasmussen; PB Laursen; R Parisotto; Rajan K. Patel; RJ Shephard; RR Engel; RS Franco; SW Ryter; TD Noakes; TD Noakes; Tushar Chatterji; W Jelkmann; W Schmidt; Yannis P. Pitsiladis

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Haemoglobin mass and running time trial performance after recombinant human erythropoietin administration in trained men

Authors: A Lucia
AJ Brien
B Berglund
BD Levine
C Ahlgrim
C Lundby
C Lundby
C Lundby
CC Chang
CP Alfrey
D Boning
Diresibachew H. Wondimu
DL Costill
DP Wilkerson
Elias T. Zambidis
Evangelia Daskalaki
G Banfi
G Ninot
G Russell
GP Millet
H Ehrenreich
I Mujika
JD Belcher
JJ Thomsen
JM Kirkeberg
John D. McClure
Jérôme Durussel
K Heinicke
K Miskowiak
KI Birkeland
L Rice
L Rice
M Audran
M Brines
Martin Anderson
Neal Padmanabhan
NV Olsen
P Connes
P Rasmussen
PB Laursen
R Parisotto
Rajan K. Patel
RJ Shephard
RR Engel
RS Franco
SW Ryter
TD Noakes
TD Noakes
Tushar Chatterji
W Jelkmann
W Schmidt
Yannis P. Pitsiladis
Publication date: 1 January 2013
Publisher: 'Public Library of Science (PLoS)'
Doi

Abstract

Recombinant human erythropoietin (rHuEpo) increases haemoglobin mass (Hbmass) and maximal oxygen uptake (v˙ O2 max). Purpose: This study defined the time course of changes in Hbmass, v˙ O2 max as well as running time trial performance following 4 weeks of rHuEpo administration to determine whether the laboratory observations would translate into actual improvements in running performance in the field. Methods: 19 trained men received rHuEpo injections of 50 IUNkg21 body mass every two days for 4 weeks. Hbmass was determined weekly using the optimized carbon monoxide rebreathing method until 4 weeks after administration. v˙ O2 max and 3,000 m time trial performance were measured pre, post administration and at the end of the study. Results: Relative to baseline, running performance significantly improved by ,6% after administration (10:3061:07 min:sec vs. 11:0861:15 min:sec, p,0.001) and remained significantly enhanced by ,3% 4 weeks after administration (10:4661:13 min:sec, p,0.001), while v˙ O2 max was also significantly increased post administration (60.765.8 mLNmin21Nkg21 vs. 56.066.2 mLNmin21Nkg21, p,0.001) and remained significantly increased 4 weeks after rHuEpo (58.065.6 mLNmin21Nkg21, p = 0.021). Hbmass was significantly increased at the end of administration compared to baseline (15.261.5 gNkg21 vs. 12.761.2 gNkg21, p,0.001). The rate of decrease in Hbmass toward baseline values post rHuEpo was similar to that of the increase during administration (20.53 gNkg21Nwk21, 95% confidence interval (CI) (20.68, 20.38) vs. 0.54 gNkg21Nwk21, CI (0.46, 0.63)) but Hbmass was still significantly elevated 4 weeks after administration compared to baseline (13.761.1 gNkg21, p<0.001). Conclusion: Running performance was improved following 4 weeks of rHuEpo and remained elevated 4 weeks after administration compared to baseline. These field performance effects coincided with rHuEpo-induced elevated v˙ O2 max and Hbmass.</p&gt