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Effect of medroxyprogesterone on arterial blood gases, leptin and neuropeptide Y in postmenopausal females

Depts of ¹ Pulmonary Diseases, ² Physiology and ³ Clinical Chemistry, Turku University Central Hospital and University of Turku, Turku, Finland

CORRESPONDENCE: T. Saaresranta, Dept of Pulmonary Diseases, Turku University Central Hospital, Kiinamyllynkatu 4–8, FIN-20520, Turku, Finland. Fax: 358 23133328. E-mail: tarja.saaresranta@tyks.fi

Keywords: breathing, chronic obstructive pulmonary disease, hypercapnia, leptin, neuropeptide Y, progesterone

Received: September 20, 2001
Accepted July 7, 2002

This work was supported by grants from the Finnish Medical Foundation, the Finnish Anti-Tuberculosis Association Foundation, the Väinö and Laina Kivi Foundation and the Turku University Foundation.

	Abstract

TOP Abstract Subjects Methods Discussion Acknowledgements References

 
Natural progesterone, a potent respiratory stimulant, stimulates leptin production in premenopausal females. Leptin and its counterpart neuropeptide Y (NPY) have recently been linked with respiration. The effect of medroxyprogesterone acetate (MPA) on arterial blood gases, serum leptin and NPY was evaluated in this study.

Fourteen postmenopausal females with respiratory impairment, due mostly to chronic obstructive pulmonary disease, were recruited for a randomised, double-blind, placebo-controlled crossover trial. Arterial blood gases, serum leptin and NPY concentrations were measured at baseline and after 14 days of treatment with placebo and MPA, separated by a 6-week washout period.

Thirteen patients completed the trial. The mean±sd carbon dioxide tension in arterial blood (P_a,CO2) was 5.4±0.6 kPa at baseline, and decreased by 0.8±0.3 kPa during treatment with MPA. The oxygen tension in arterial blood (P_a,O2) and pH did not change. At baseline, the mean base excess was 0.6±1.9 mmol·L^–1 and the mean bicarbonate (HCO₃^–) concentration was 25.1±1.6 mmol·L^–1. With MPA, base excess decreased by 2.2±1.2 mmol·L^–1 and HCO₃^– by 1.9±1.0 mmol·L^–1 from baseline. The mean concentrations of serum leptin (19.8±9.9 µg·L^–1 at baseline, 19.7±9.8 µg·L^–1 with MPA) or NPY (94.0±18.3 pmol·L^–1 at baseline, 85.1±41.2 pmol·L^–1 with MPA) did not change. However, the reduction in P_a,CO2 correlated with the reduction of serum leptin concentration.

Medroxyprogesterone acetate effectively decreased the carbon dioxide tension in postmenopausal females with chronic respiratory impairment. The results suggest that a decrease in the carbon dioxide tension of 0.9 kPa is necessary for a reduction in serum leptin concentration.

Breathing is regulated through voluntary (cortex) and involuntary (emotional, metabolic, neural and endocrine components) control mechanisms. Furthermore, the endocrine and nervous systems have complex interactions. Although some endocrine links with breathing are well established, a comprehensive understanding of the interactions of hormones and breathing is lacking.

Leptin and neuropeptide Y (NPY) regulate food intake, but are also involved in other functions. Recent data suggests that leptin may increase ventilation 1, whereas NPY has the opposite effect 2. Leptin inhibits NPY expression 4. In premenopausal females, natural progesterone stimulates leptin release 5.

Postmenopausal females have lower leptin levels 7 and higher NPY levels 9 than premenopausal females. After the menopause, females frequently gain weight. They also have an increased prevalence of sleep-disordered breathing 10. This increase has been attributed to the decline in serum progesterone concentrations, since progesterone is a potent respiratory stimulant. Alterations in serum leptin levels have also been linked with alterations in female hormone concentrations, i.e. progesterone 11.

Progestins are frequently used as a part of postmenopausal hormone replacement therapy. A synthetic progesterone derivative, medroxyprogesterone acetate (MPA), effectively stimulates breathing in postmenopausal females 12 and produces some improvement in sleep-disordered breathing in such individuals 13. The exact mechanisms through which progestins stimulate breathing are not known. MPA is considered to be a central respiratory stimulant 15 but there is also evidence for peripheral action 16. MPA induces complex endocrine alterations, which seem to be associated with breathing 17. The effect of plain progestin therapy on leptin or NPY levels is not known. The effects of short-term treatment MPA on arterial blood gases, serum leptin and NPY levels in postmenopausal females with respiratory impairment were investigated in this study.

	Subjects

TOP Abstract Subjects Methods Discussion Acknowledgements References

 
Fourteen postmenopausal females with constant or episodic hypercapnic or hypoxaemic respiratory impairment were recruited for the trial. Their respiratory impairment was due to chronic obstructive pulmonary disease (COPD) (n=11), end-stage asthma or late sequelae of pulmonary tuberculosis. Their mean age±sd was 68.1±7.9 yrs and their mean body mass index (BMI) 26.6±6.1 kg·m^–2. The postmenopausal state was confirmed by measurement of serum follicle stimulating hormone (FSH) concentration over 30 IU·L^–1.

The subjects were strictly requested not to use any medication affecting the central nervous system, alternative therapy or any hormone replacement therapy except the study drugs. Subjects using long-term oxygen therapy, with cancer, psychiatric, neurological, thromboembolic or hepatic diseases, renal failure, unstable hypertension, severe rheumatoid arthritis, insulin-dependent diabetes or severe hyperlipidaemia (total serum cholesterol >9.5 mmol·L^–1 or serum triglycerides >2.5 mmol·L^–1) were excluded. One subject who smoked less than five cigarettes per day was advised not to smoke during the 9 h preceding each study visit. All other subjects were current nonsmokers.

	Methods

TOP Abstract Subjects Methods Discussion Acknowledgements References

 
The study followed a double-blind randomised placebo-controlled crossover design and included three visits (fig. 1). There was a 6-week washout period between the 2-week placebo and MPA treatment periods. The choice of a 6-week washout period was based on a previous study, where, in a slightly younger postmenopausal female population, 6 weeks were needed for all the measured variables to return to baseline after cessation of MPA 12. The same visit protocol was followed at baseline, after a 2-week placebo and a 2-week MPA (60 mg·day^–1) period (Lutopolar®; Orion Pharma, Espoo, Finland). The placebo tablets were identical in appearance to the MPA tablets and were provided by the same manufacturer. The visit protocol included measurements of weight, arterial blood gases, serum concentrations of leptin, NPY and alanine aminotransferase, blood haemoglobin and flow volume spirometry (VMAX 22D; Sensor Medics, Boulder, CO, USA). The subjects had at least a 15-min rest period in the sitting position before the blood samples were obtained after overnight fasting. Subjects kept a diary of their symptoms and possible adverse events for the 14 days prior to each visit.

View larger version (28K): [in this window] [in a new window]   Fig. 1.— Flow diagram of the study. MPA: medroxyprogesterone acetate.

All patients gave written informed consent. The study protocol was approved by the Joint Commission on Ethics of Turku University and Turku University Central Hospital, and by the National Agency for Medicines.

Statistical analyses
The results were analysed using statistical methods developed for a crossover design of two treatments and two periods 18. First any carryover effect was identified using analysis of variance of repeated measurements according to Jones and Kenward 18, performed with the MIXED procedure. The testing for a carryover effect evaluated whether there was any residual effect of MPA on measured variables after a 6-week washout. The period effect tested whether the order of placebo and active drug had any effect on the results. A p<0.1 was considered significant for a carryover effect, whereas a p<0.05 was considered significant for period and treatment effects. Distribution and variance for each parameter were tested. The study sample was also analysed as a single placebo controlled study, and paired comparisons of differences ((placebo–baseline) versus (MPA–baseline)) were made. Depending on the distributions of differences ((placebo–baseline) and (MPA–baseline)), either a paired t-test (in parametric cases) or Wilcoxon Signed-Rank test (in nonparametric cases) were used. The correlations for serum leptin and NPY levels with BMI and arterial blood gases were tested at each of the three time points (at baseline, with placebo and with MPA) using Spearman's or Pearson's correlation coefficients, as applicable. The p-values were corrected according to the Bonferroni principle. Correlations between changes in serum leptin and NPY levels and other parameters were tested using Spearman's or Pearson's correlation coefficients, as applicable.

Results
Thirteen patients completed the study protocol. One patient discontinued due to an exacerbation of COPD. No carryover effect on the measured parameters was observed. A period effect was seen in the carbon dioxide tension in arterial blood (P_a,CO2), the values being higher during the second period. The mean weight remained unchanged throughout the study. At baseline the mean forced expiratory volume in one second (FEV₁) was 1.0±0.5 L (44±19% of predicted) and the mean forced vital capacity (FVC) was 1.7±0.6 L (61±23% pred). Both FEV₁ and FVC remained unchanged throughout the study. Blood haemoglobin (baseline mean 137.8±9.7 g·L^–1) or serum alanine aminotransferase (baseline mean 17.7±6.0 U·L^–1) were within reference ranges and did not change during the trial. No adverse drug effects were observed or reported.

The mean P_a,CO2 was 5.4±0.6 kPa at baseline and decreased on average by 0.8±0.3 kPa with MPA (p<0.001). The mean oxygen tension in arterial blood (P_a,CO2) was 1.3±1.6 and did not change significantly during the study period. At baseline, the mean pH was 7.41±0.03, the change with MPA (0.01±0.03) was not significant. At baseline, the mean base excess (BE) was 0.6±1.9 mmol·L^–1 and the mean HCO₃^– was 25.1±1.6 mmol·L^–1. With MPA, BE decreased by 2.2±1.2 mmol·L^–1 (p<0.0001) and HCO₃^– by 1.9±1.0 mmol·L^–1 from baseline (p<0.0001).

The mean concentrations of serum leptin (fig. 2) or NPY (fig. 3) did not change. At baseline, mean serum leptin concentration was 19.8±9.9 µg·L^–1. On MPA, leptin was 19.7±9.8 µg·L^–1. At baseline, mean serum NPY concentration was 94.0±18.3 pmol·L^–1. On MPA, NPY was 85.1±41.2 pmol·L^–1.

View larger version (21K): [in this window] [in a new window]   Fig. 2.— Serum concentrations of leptin at baseline, with a) placebo and b) after 2-weeks of treatment with medroxyprogesterone acetate (MPA). • baseline values; values with placebo; values with MPA.

View larger version (19K): [in this window] [in a new window]   Fig. 3.— Serum concentrations of neuropeptide Y (NPY) at baseline with a) placebo and b) after 2 weeks of treatment with medroxyprogesterone acetate (MPA). • baseline values; values with placebo; values with MPA.

View larger version (17K): [in this window] [in a new window]   Fig. 4.— Changes in fasting serum leptin concentration versus changes in the carbon dioxide pressure in arterial blood (Pa,CO2) in postmenopausal females with moderate-to-severe chronic respiratory impairment showing a positive correlation (r=0.60, p=0.031).

	Discussion

TOP Abstract Subjects Methods Discussion Acknowledgements References

In obese mutant mice with leptin deficiency, leptin infusion increased ventilation 1. The effect of leptin on ventilation was independent of weight, CO₂ production and food intake, suggesting a direct effect of leptin on the central control of respiration. It was hypothesised that MPA, while improving ventilation, would increase serum leptin levels and decrease NPY, partly having its effect on breathing via altering the levels of these two hormones. However, the patients in this study showed that the serum leptin levels did not increase during MPA therapy although ventilation did. This is in contrast with the previous observations of increased leptin levels during states with simultaneously increased serum progesterone concentrations and increased ventilation, e.g. during the luteal phase of the menstrual cycle 5 or during pregnancy 21. Higher leptin levels have been reported in premenopausal females compared with postmenopausal 7 although this finding has not been confirmed by all studies in this field 22. Some authors have observed a positive correlation between leptin and progesterone levels 5, whereas others have not 21.

Recent studies in obstructive sleep apnoea syndrome (OSAS) and obesity hypoventilation syndrome support the present study. Obese hypercapnic patients have higher fasting serum leptin levels than obese eucapnic patients, and serum leptin more reliably predicts the presence of hypercapnia than the percentage of body fat 25. Serum leptin levels decrease with nasal continuous positive airway pressure (CPAP) treatment 26 without changes in body weight 27. Because nasal CPAP treatment improves ventilation and decreases CO₂ levels 14, an association between decreased leptin levels and decreased CO₂ levels in these studies may be assumed, although neither arterial, transcutaneous nor end-tidal CO₂ levels were not measured.

The present study population was heterogeneous in terms of hypercapnia and BMI. Four of the patients had a BMI>30 kg·m^–2 and four had a P_a,CO26.0 kPa, one patient had both. This heterogeneity may have influenced the results. Patients in previous studies of the association between serum leptin levels and breathing have been obese with OSAS or obesity hyperventilation syndrome, and hyperleptinaemia has been linked with possible obesity-related leptin resistance 25–27. Most of the patients in this study were lean, and their weight remained stable during the study. Therefore, the positive correlation between changes in serum leptin levels and P_a,CO2 levels was not related to obesity nor to weight changes. Leptin levels, in the patients in this study, were not high probably because they were neither obese nor hypercapnic 25. Both leptin 1 and MPA are powerful respiratory stimulants. When the upper airway is unloaded and the CO₂ levels are decreased, with the help of nasal CPAP or with a respiratory stimulant such as MPA (as in the present study), lower leptin levels are no longer needed to support ventilation.

The existence of states with increased serum leptin and progesterone supports the association between leptin and endogenously high progesterone concentrations. However, a synthetic progestin MPA was used in this study, the effect of which on leptin may differ from that of endogenous progesterone. In ovariectomised females on progesterone plus oestradiol replacement therapy, progesterone increased leptin secretion regardless of oestradiol concentration 6. In postmenopausal females, combined hormone replacement therapy with continuous conjugated oestrogens (0.625 mg·day^–1) for 11 months and MPA (5 mg·day^–1 for 13 days every third month) had no effect on serum leptin levels 28. Addition of progesterone (100 mg per vagina b.i.d.) to transdermal oestrogen therapy had no effect on serum leptin concentrations 29. To the best of the authors' knowledge there have been no previous reports on the effect of plain progestin therapy on leptin levels.

This study also found that serum NPY concentrations did not change during MPA therapy. NPY levels increase during pregnancy 30 and during the menopause 9. These findings suggest that NPY is unrelated to serum progesterone concentrations, although correlations between progesterone and NPY levels were not evaluated. In animal studies, the respiratory rate decreased after central administration of NPY 2. The role of NPY in human control of breathing is not established, but some data suggest that it might play a role. A post mortem study in 19 patients showed that those with very high NPY levels in the infundibular nucleus had suffered from respiratory failure for at least 10 days before death, whereas patients with low levels of NPY had died either within 2 days of the onset of cardiorespiratory disorders or of unrelated causes 31. The effect of progestin therapy on NPY concentrations has not been elucidated previously. Although the results from this study showed no significant effect of MPA on serum NPY levels, there is a high risk of a type II error due to the small sample size and high variability in the levels of serum NPY. Therefore, the possibility that MPA would have an effect on serum NPY levels cannot be excluded.

Short-term progestin therapy effectively improved ventilation and decreased the carbon dioxide tension in arterial blood in postmenopausal females with chronic respiratory impairment. Although medroxyprogesterone acetate did not alter serum leptin or neuropeptide Y levels, the decrease in the carbon dioxide tension in arterial blood was associated with a decrease in serum leptin levels. Unfortunately, the present study was underpowered to observe changes in serum neuropeptide Y. The present observations support an association of leptin with the control of breathing in human subjects. Whether the changes in leptin concentration observed in the present study, are secondary to the changes in the carbon dioxide tension in arterial blood or contribute actively to respiratory stimulation during hypercapnia remains to be elucidated.

	Acknowledgements

TOP Abstract Subjects Methods Discussion Acknowledgements References

 
The authors would like to thank E. Wallius, for statistical assistance and Orion Pharma, Espoo, Finland for the supply of medication.

	References

TOP Abstract Subjects Methods Discussion Acknowledgements References

 

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