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Recent advances in hormone replacement therapy
Roger NJ Simth/John WW Studd, Kings College Hospital, London
I n v i e w o f t h e benefits o f h o r m o n e replacement t h e r a p y ( H R T ) a n d t h e experience t h a t o n l y 1 0 % of w o m e n m a i n t a i n t h e r a p y , i t IS v i t a l t h a t a l l doctors are f a m i l i a r w i t h t h e pros a n d cons of H R T , so t h a t w o m e n m a y be correc t ly advised H e r e we discuss new issues a n d developments m H R T a n d c u r r e n t views o n i n d i c a t i o n s , compl i cat ions , a n d regimens of t r e a t m e n t
M r Smith- is- correntiy Research Fellow and Mr Studd I S currently Consultant Gynaecolopst m the Department of Obstetrics and Gynaecology at The Chelsea and Westmrnster Hospital, London
Correspondence to Mr John Studd, Consultant Gynaecologist, Chelsea and •Westminster Hospital, London SW10 9 N H
I > n England and Wales there are approx i mately 10 m i l l i o n climacteric or postmenopausal' women ( C e n t r a l Statistical' Office, 1991), therefore one i n five o f the t o t a l populat ion IS a potent ia l candidate for hor mone replacement therapy ( H R T ) {Ftg 1)
Therapy has medical implications m several areas, mcludmg depression, ischaemtfr heart dtsease- (fHE>->, stroke- and-thrombosis, osteoporosis, premature menopause, and breast cancer
Depression I t IS generally accepted t h a t the climacteric frequently leads to- -^^anous unpleasant symptoms, which are opt imal ly treated w i t h oestrogen replacement (Studd et al, 1977) T h e best charactenzed o f these are h o t flushes and vagmal dryness I n addit ion , a variety o f other symptoms, such as m -sommar headaches,, d-yspareuniar loss, o f l i b ido , generalized aches and pams, poor concentration, poor memory , i r r i t a b i l i t y and depression, are often associated -with the menopause and constitute the less we l l -defmed menopausal syndrome T h e emergence of data supporting: the theory that fluctuations m oestrogen levels may p r o foundly influence m o o d supports the existence of such a climacteric syndrome before the fmal cessation of penods
Fig 1 Number of climacteric and postmenopausal women in England and Wales (Central Statistical Office, 1991)
Changes m the pattern of ovanan hor mone secretion are often associated w i t h the development o f depression I n premenst^ua^ syndrome (PMS), the m o o d change is an abnormal response t o the physiological changes o f the menstrual cycle, b u t m b o t h postnatal depression and clunactenc depression m o o d change is associated w i t h a major upheavat o f ovanan f o n c t t o n These observations suggest that ovanan hormones may modulate mood , a concept m keepmg w i t h the generally greater mcidence of depressive disorders m women compared w i t h men
T h e pubhshed data all suggest that oestrogen elevates m o o d Oestrogen-therapy has been shown to accelerate recovery f r o m postnatal depression (Henderson et al, 1991), t o be an effective treatment for PMS, mcludmg premenstrual depression (Magos et al , 1986a), and t o signi£<anjly ekva-te m o o d m. clunactenc. depression (Montgomery et al, 1987) (Fig 2) Oestrogen also elevates m o o d m asymptomat ic non-depressed postmenopausal women ( D i t k o f f et al , 1991), and m h igh doses IS an effective treatment for severe depression (Klaiber et al^ 1979) By compan-son there is no evidence that either pro gestogens or progesterone elevate mood They are no t effective treatments for PMS and Magos et al (1986b) have shown that progestogens can cause many of the symptoms o f PMS, mcludmg depression
W h i l e much collaborative w o r k o n the relationship between oestrogen, progesterone and depression remains t o be done, i t is now t ime for a wider acceptance by psychiatrists that oestrogen has a role i n the treatment of depression m women
Ischaemic heart disease, stroke and thrombosis
I t IS regrettable that I H D is s t i l l widely regarded as a contraindication t o H R T , as this IS completely at odds w i t h the pubhshed data
I n one o f the rare circumstances m
Bncish Joumil of Hospiod Mediane 1993, Vol 49, No 11 799
i i „ L _ I I h I I 1 H I ^ I L | p i I i l L L I U
2 -
» - * i 1 i 1 i-.—
Ftg. 2 Effect of oestradiQl 5Q mg, implaata o a perimeaopausaL deprea-sion (Montgomery et al, 1987} * = significantly different from placebo (P<0 01)
Fig 3 Potential impact of hormone replacement therapy (HRT) upon annual deaths from ischaemtc heart disease
wiuch the data are i n ahnost complete agreement, i t is clear t h a t H R T markedly reduces the nsk of I H D A recent metaanalysis of 31 pubhshed studies f o u n d an overall nsk rat io for I H D o f 0 56 (95% confidence mterval. 5.-0.61.). foe oestrogen users (Stampfer and C o l d i t z , 1991) Even when only the 13 most rigorous studies employmg a prospective cohor t design were mcluded, the nsk rat io f o r oestrogen users was stiU 0 58 (95 % confidence mterval 0 48-0 69). T h i s reduct i on m n s k o f I H D 14 numencally the most significant l ong - term effect of H R T , because I H D is the greatest cause o f death among postmenopausal women U s m g the 1990 m o r t a h t y statistics and populat ion data f r o m the 1981 census, a reduced relative r isk o f death f r o m I H D among oestrogen users of 0 56 w o u l d be translated i n t o a savmg o f approximately 24 000 lives per annum m England and
800
Myocartisi krfafctwfl nsk
Strokarek
Fig 4 Differential effects of the piit and hormone replacement therapy upon cardiovascular disease
Wales alone i f all postmenopausal women used H R T (Central Statistical Office, 1991, Office o f Population Censuses and Surveys, 1991) (Fig 3)
T h e one theoretical flaw m this epidemiological consensus is that for the last t w o or three decades H R T may n o t have been given t o patients w i t h a h igh nsk o f heart disease Thus i t is possible t h a t these encou-ragmg results are due t o selection bias, a l though the L i p i d Research Climcs study f o u n d the greatest reduction m cardiovascular mor tahty among high-nsfe patients w i t h elevated b lood h p i d levels (Bush et al, 1987)
U n t i l recently i t was t h o u g h t that oestrogen acted mamly t h r o u g h h p i d changes, 1 e b y mcreasmg high density l ipoprotem and r e d u c i r ^ low density- hpoprotem cholest e r o l Recent data mdicate that oestrogen also has other desirable physiological actions A n i m a l data have shown that oestrogen exerts a direct atheroma-m h i b i t m g action o n the artenal wal l mde-pendently^of b l o o d cholesterol-(Hoagfc and 2dversmit , 1986) Co l our flow D o p p l e f imagmg has demonstrated that oestrogen mcreases penpheral b l o o d flow, b o t h m the uterme artery and m the m t e m a l carotid artery (Bourne et al, 1990, Gangar et al, 1991). Oestrogen-may also-work b y modi fy -m g carbohydrate metabohsm and body fat d i s t n b u t i o n , b o t h o f which are related t o I H D nsk
A history o f thrombosis is also often regarded as an absolute contramdication t o H B T v presumably because, i t is. assumed t h a t postmenopausal H R T has the same thrombogemc potent ia l as the contracept ive p i l l T h i s is n o t the case ( f j g 4) There is n o w wor ldwide expenence o f H R T , pre-dommant ly oral conjugated eqmne oestro-gens (Premarm), which has n o t sho-wn any mcreased mcidence of thrombosis , mdeed, H R T actually reduces the r isk o f stroke (Paganmi-Hi l l et a l , 1988)
Thnm H R T
t »
Fig 5 Increase in bone density achieved with different routes of oestrogen administration (Chnstiansen and Christiansen, 1981, Lindsay et al, 1976, Stevenson et al, 1990, Studd et al, 1990) Implant = 75 mg, patch = 50 ng, oral = oestradiol 2 mg
Ttere - are. ^ezeraL -differences, between H R T and the combined oral contraceptive p d l ( C O C P ) wh i ch account for this apparent discrepancy M o s t i m p o r t a n t l y , the synthetic oestrogens m the C O C P are f our t o eight times as potent as the natural oestrogens m H R T at mducing. the hver enzyme systems that produce c l o t t m g factors (Campbell , 1982) I n addiuon , the dose o f oestrogen t h a t is usually employed m H R T is approximately one s ix th o f that commonly used m the C O C P T h e avoidance of first-pass hepatic effects by employmg a non-oral route of delivery reduces any potent ia l thrombogemc nsk even further W h i l e conventional oral H R T results m some nunor changes m laboratory measures of c l o t t m g funct ion , such as a shght reduc-tton m a n t i t h r o m b m I I I , no such changes m coagulation, fibrmolysis or platelet funct ion are seen, even w i t h a potent non-oral preparat ion, e g a 50 m g subcutaneous oestrad io l implant (Studd et al, 1978)
Thus I H D , or the presence of nsk factors for I H D , should be regarded, no t as contraindications, b u t as positive mdications f o r postmenopausal H R T A history of previous thrombosis need only constitute a contramdication m those rare cases where there is a permanent mcrease m thrombot i c nsk , e g due t o a n t i t h r o m b m I I I , p ro tem C o r p r o t e m S def faeuqr Where concern exists, non-oral oestrogens such as percutaneous patches or subcutaneous implants
1 - \f Vol 49 No 11
should be used m preference t o oral therapy
Osteoporosis I n osteoporosis, bone is normal ly m m e r -ahzed b u t reduced m quant i ty such t h a t mass per u m t volume is reduced Osteoporosis IS a major cause of pam, disabihty, suffenng and death m elderfy women One quarter of white women over the age o f 60 years have radiological evidence of vertebral crush fractures, whde the combmed m a -dence of fractures of vertebra, femoral neck and forearm m the over-65s is estimated t o b e 55-4Q%- (-Stevenson a n d Whttei iead, 1982) I n t u r n , the fmancial burden on the health service is considerable, -mth fracture o f the femur bemg the t h i r d commonest reason for occupancy o f a non-psychiatnc hospital bed m England and Wales
The- trs^edy. is that postmenopausal osteoporosis is preventable First , i t is wel l established t h a t oestrogen replacement therapy b o t h prevents the acceleranon o f bone loss which normally accompanies the menopause (Lmdsay et al , 1978) and reduces tke. sihsfiiquent n s k o f feictiice ( K e i l e t ai,. 1987) Second, oestrogen actually mcreases bone density, so that oestrogen replacement can be used t o correct l ow bone density m thosealready at mcreased nsk of fracture I n this respect oestrogen seems to exhib i t a dose-response effect For example,, ora l oestrogen m general mcreases vertebral bone density by approximately 1-2% per annum (Lmdsay et al , 1976, Christiansen and Christiansen, 1981), whereas the 75 m g oestradiol implant , which achieves oestrad i o l levels m general at least double those of oral therapy, has been shown to mcrease vertebral bone density b y 8 3% per annum (Studd et al, 1990) T h e comparable figure for the 50 ^g transdermal patch is a 3 5% mcrease over 12 months (Stevenson et a l , 1990) (Fig 5) T h e f m d m g o f a significant correfation between oestradiol level and mcrease m vertebral bone density by Studd et al (1990) confirms this dose-response relationship
Oestrogen should be regarded as the benchmark agamst which al l other potent ia l treatments, b o t h prophylactic andremedial , should be judged Calc ium supplements are prescnbed as a non-hormonal alternative t o oestrogen, b u t although calcium may be impor tant m early life t o estabksh adequate peak bone mass, there is no evidence t h a t c r f c r a m i a t e r r n h f e e i ther prevents- ortreats-osteoporosis Sinularly, while undoubtedly able t o mfluence bone mass, physical exer-
801
Recent advances m hormone replacement therapy
I M n M l l l d l B l
oiiii.»nattmit KH*MM«ltf 2 «
i f c i M i I i M t o a n •akiiuitnD]
- r 05
r r r
10 I S 20 25
Beiaiivanslcan<195%«>n6denc8inferval
30 3S
Fig 6 Disparity of data concerning oestrogen and breast cancer incidence (from Dupont and Page, 1991, references from tfie figure can be found with origmaf article)
CISC alone i s n o t adequate t o prevent menopausal osteoporosis F luonde mcreases bone mass, b u t has been f o u n d t o mcrease fracture madence because o f an adverse effect upon bone quahty (Lindsay and Cosman, t99£9" Ca i c i t onm is able t o prevent bone loss b u t has the major disadvantage o f admimstrat ion b y either mject ion o r nasal spray, and i t is very expensive T h e most mterestmg non-hormonal approach t o date IS the bisphosphonate, disodium e t i dronate- (Didronely T h » preparat ion has the convemence o f oral admimstrat ion , is able n o t on ly t o prevent bone loss b u t also t o mcrease bone density by approximately 2% per year, and has been shown t o reduce the mcidence o f radiologically detected vertebral fracture (Storm-et a l , 19.9&, Watts -et al , 1990)
T h e mechamsm b y wh i ch oestrogen exerts i t s beneficial effect upon bone mmeral and m a t r i x is at present u n k n o w n I t does n o t seem t o influence c a l a u m or -o-tamm D metabolism,, h u t may a.ct. m -direct ly by mcreasmg the act iv i ty o f caicit o n m A l b n g h t et al (1941) beheved that postmenopausal osteoporosis was essent ia l ly a generahzed deficiency of collagen, v n t h loss o f the collagenous bone m a t n x bemg the prmcipa l mechamsm I t is k n o w n t h a t postmenopausal oestrogen therapy results m a 3 0 % mcrease m skm thickness and a 3 4 % mcrease m s k m collagen content (Bnncat et al , 1985) I t is possible t h a t i n a similar manner oestrogen mcreases the co l lagenous m a t n x o f bone (Studd et a l , 1990) T h i s IS current ly bemg mvestigated by means of serial h is tomorphometnc studies o n bone biopsy specimens T h e possibihty t h a t oestrogen may act t h r o u g h collagen
holds ou t the possibihty that oestrogen therapy may be able t o promote healmg of bone m which trabecular d isrupt ion has already occurred, and thus be used t o treat severe osteoporosis m which bones have already fractured
Premature menopause and infertility
Cases of premature menopause are usually id iopathic b u t may also be secondary t o surgery, chemotherapy or chromosomal disorders such as Turner ' s syndrome W h i l e the adverse sequelae o f premature w i t h drawal of oestrogen such as premature osteoporosis and mcreased nsk o f I H D should be prevented w i t h appropnate H R T , the personal tragedy o f in f e r td i ty m such women has u n t d recently remamed untreatable T h e advent o f o v u m donation m the context of assisted conception has changed that depressmg out look Abdalla et al (1989) treated 29 women w i t h a mean age o f 36 years Donated oocytes were fert i l ized w i t h spermatozoa f r o m the recipient's p a r t n e r and then frozen u n t i l either i n t r a -uterme embryo transfer or zygote m t r a -faHopian transfer was undertaken Pregnancy rates o f approximately 3 0 % were achieved, and this success rate has been mamtamed w i t h 116 pregnancies m 371 couples- (AbdaH* a n d Studd, mrpubhshed data) I t must be remembered that these are n o t agemg women t r y m g t o cheat nature, b u t rather women w h o m nature has cheated
Ereast caacer T h e hfet ime mcidence o f breast cancer m the developed w o r l d is approximately 10% and any factor that may mcrease this figure IS a larmmg Epidemiological e-vidence that early menarche, late f i rst pregnancy and late menopause are assoaated widbtan mcreased n s k of breast cancer has been mterpreted as mdicatmg that ovanan hormones, part i cular ly oestrogen, mcrease the n s k of breast cancer
U n l i k e the s i tuat ion w i t h I H D and H R T ^ where the data are m agreement^ there is great dispanty among the numerous studies that have sought t o mvestigate the relationship between H R T and breast cancer mcidence (Fig 6) O f the 28 studies pubhshed smce 1972, 19 faded t o achieve statistical significance O f the significant studies, SIX showed an increased nsk of breast cancer w i t h oestrogen use and three a reduced n s k Such data are d i f f i cu l t t o interpret Meta-analysis of al l 28 studies
802 I<M1 Vnl if, 11
Recent advances m hormone replacement therapy
* A difficult qu&ticm. IS whether HRT may be given to women who have already had breast cancer There are no specthcally relevant data to give an answer, but m light of the above it seems appropriate to judge each case on its merits and to prescribe HRT where a strong indication exists '
yieLis. a. relative n s k o£ 1 QJ f o r oestrogen users, b u t the 9 5 % confidence mterval o f 0 96 -1 2 mdicates that this difference is n o t staustically significant ( D u p o n t and Page, 1991) A simdar study covermg only 16 studies found a relative risk of 1 3 (95% confidence mterval 1 2 - 1 6) b u t must be criticized because of its selective nature (Steinberg et al , 1991) Perhaps the most obvious conclusion i s t h a t there is no evidence of a major i n c r e a s e m the mcidence of breast cancer m oestrogen users
T h e above data are all concerned w i t h the mcidence of breast cancer W h i l e there are few data concemmg m o r t a h t y f r o m breast cancer m oestrogen users, those that exist are o f great mterest Even m a study i n which the mcidence o f breast cancer m oestrogen users was mcreased, H u n t et al (1987, 1990) and Bergkvist et a l (1989) reported a reduced m o r t a h t y f r o m the disease There are several possible explananons for this apparent discrepancy First , breast cancer occurring in oestrogen users may have a better prognosis, this idea is supp o r t e d by the high p r o p o r t i o n o f stage I tumours occurrmg among oestrogen users ( H u n t et al, 1987, 1990) and the sigmficantly improved 5-year survival f ound by Bergkvist et al (1989)
T h e imphcat ion that oestrogen improves prognosis- is n o t necessardy- m conf l ict -wi th k n o w n data regardmg tamoxifen, as t a m o x i fen has b o t h oestrogen antagomst and agonist properties I n postmenopausal women i t may induce endometrial prohfera-t i o n and vagmal bleedmg, and m some cases hyperplas i i a n d even eaFemoma l a a d d i t i o n , I t has oestrogen-like favourable effects upon h p i d fractions (Love et al, 1991) and, hke oestrogen, reduces the risk of myocardial infarct ion (McDonald and Stewart, 1991)
Asecondexplanaiion. is .thatthemcreased level of breast screening by means of palpat i o n and mammography t h a t oestrogen users are subjected t o may result m the overdiagnosis of histologically ambiguous lesions (Studd, 1989), or the detection of tumours of very low grade malignancy which otherwise wou ld never have become chnicaUy apparent or w o u l d no t have done so for many years I n support o f the lat ter concept is the presence of chnically imsus-pected m-s i tu and invasive breast carcmoma at medicolegal autopsy (Nielsen et al, 1?87) and the f m d m g by K i e m i et al (1992) t h a t , e v e n after adjustment f o r s i z e , tumours detected by screenmg were of lower h is to logical and cytological mahgnancy
T h e r e is. a. suggestion from, epidemio^ logical and cell culture studies that progesterone may mcrease the nsk of breast cancer These data are confused, b u t the chmcal imphcanons are senous However , the conclusions remam unconvmcmg and further w o r k is required t o clarify the issue
I t i s possible t h a t , i n spite of the selection and survival bias of these studies, H R T may be associated w i t h a shght mcrease m i n c i dence of breast cancer, b u t t h a t this is balanced by a correspondmg reduction m m o r t a h t y Whi l e the explanation of th is paradox remams unknown , the result is t h a t the effect o f H R T upon breast cancer is probably neutral
A di f f i cult question is whether H R T may be given t o women who have already had breast cancer There are no specifically relevant data t o give an answer, b u t m hght o f the above i t seems appropnate t o judge each case on its merits and t o prescribe H R T where a strong mdication exists Use of oestrogen replacement does n o t preclude the concomitant use of tamoxi fen
H R T regimens Progestogens I t has been established practice t o give cyclical progestogen w i t h postmenopausal H R T smce i t was demonstrated that a course o f tO—15 days each m o n t h co tdd prevent the development o f endometnal hyperplasia (Sturdee et a l , 1978) and atypical hyperplasia (Paterson et al, 1980) T h i s pohcy has proved effective m removmg the excess nsk of endometnal carcmoma assoc iated W i t h - unopposed oestrogen- therapy (Persson et al , 1989) Unfor tunate ly i t has produced unwanted side effects, i e cychcal bleeding and progestogemc psychological and physical symptoms
W i t h d r a w a l bleedmg is currently the greatest p m b k m w i t h esrabiished cegunens. of H R T T h e bleeding may be heavy, p r o longed and/or pa infu l , and is probably the major reason f o r lack of comphance There are several approaches t o this problem A lower dose o f progestogen may be given continuously every day w i t h the aim o f rendering the endometnum atrophic — so-called contmuous combmed therapy I n the l ong term this type o f regimen is very effective, -with 95 % o f women amenorrhoeic at 12 months I n the short t e r m , however, approximately one t h i r d o f women w d l discontmue therapy w i t h i n the f i rst 6 months , mostly because of unacceptable irregular bleedmg (Magos et a l , 1985) A suitable startmg regimen is conjugated
I
Fig 7 Short-term vanability m oestradiol levels v»fith oral, patch and implant therapy
eqmne oestrogen 0 625 m g daily together w i t h n o r e t h i s t e r o n e l 05 m g Onceamenor-rhoea has been achieved, the dose o f oestrogen may be mcreased t o 1 25 m g and the dose o f norethisterone reduced T h e progestogen is convemently prescribed as the progestogen-only contracepuve N o n -day, containmg 0 35 m g norethisterone per tablet A s l ong as the dose o f progestogen is l o w and the t o t a l m o n t h l y dose is no greater than w i t h cychcal therapy, there appear t o be no adverse metabohc sequelae (Chnstiansen and Rus, 1990) A n y bleedmg after prolonged amenorrhoea requires endo-m e t r ^ biopsy because o f the possibihty o f adverse endometnal pathology (Leather et al ,1991)
A n o t h e r o p t i o n is the new synthetic denvauve of norethynodrel , nbolone , wh i ch possesses weak oestrogemc, androgenic a n d pTog^Stogefirc properties I t has been f o u n d t o prevent postmenopausal bone loss and t o reheve menopausal symptoms (Crona et al , 1988) T h e claim is t h a t i t I S n o t u tero t roph ic , therefore progesterone I S imnecessary and there w i l l be no bleedmg Al though- t r u e f o r mos t woms^, approx i mately 15% do expenence irregular bleedi n g A possible argument against i ts l ong -t e r m use I S tha t i t may n o t af ford the same pro tec t i on agamst I H D as oestrogen because i t on ly possesses weak oestrogemc effects.and.may reduce hjgh.densiEy hpoprot e m cholesterol (Bendek-Jaszmaim, 1987, De Aloys io et a l , 1987) I t s use shoidd probably therefore be reserved f o r m e d i u m -t e r m rehef o f clunactenc symptoms where the avoidance o f bleeding is paramount '
There may y e t be a. place m. carefully selected women f o r the use of unopposed cychcal oestrogens, as approximately one
quarter o f patients o n such therapy do n o t bleed I t may be specifically smtable for the o lder postmenopausal woman w i t h - osteoporosis who refuses t o accept any vagmal bleedmg, b u t she must be counselled caref u l l y about the small b u t real n s k of endom e t n a l pathology and be prepared t o undergo an endometnal biopsy approxi mately every -Z years. (Leather a n d Studd, 1990)
Endometna l ablation may have a place m the management o f the woman m w h o m the on ly progestogemc problem i s bleeding I t wiU render roughly one t h i r d o f women amenorrhoeic and w i l l reduce the amount o f bleeding m almost all ( M ^ o s e i a l , 1991) I t does n o t obviate the need fo r progestogen as there is hkely t o be residual endometnum even m those women becoming amenorrhoeic, and m a disqmetmg number o f w o m e n troublesome dysmenorrhoea may ensue (Slade et al , 1991) There is probably a m u c h greater place for hysterectomy m the postmenopausal woman tak ing H R T than IS current ly realized I n expenenced hands the procedure is safe, i t guarantees amenorrhoea and completely avoids the need for progestogen
Unpleasant PMS-hke symptoms such as breast tenderness, nausea, headaches, i m t -abdity and water re tent ion may occur pre-menstruaUy m up t o 20% o f oestrogen users t a k m g cychcal progestogen (Studd and Magos, 1988) T h a t these symptoms are caused by progestogen and no t oestrogen was proved by Magos et al (1986b) ImnaHy a different progestogen such as norethisterone, dydrogesterone o r medroxyprogesterone acetate should be used I f symptoms persist I t may be acceptable t o reduce the number o f days f o r which progestogen is taken, b u t even a 7-day course is assoaated w i t h a 3% mcidence o f endometnal hyperplasia, and some irregular bleedmg Despite such manoeuvres, there w i l l be someworaenm'whctopifogeStogfenic-symptoms persist W i t h such seventy that either t reatment is discontmued or a hysterectomy IS the preferred o p t i o n W h e n usmg oestrad i o l implants and cychcal progestogen t o treat PMS, Watson et al (1990) f o u n d t h a t , m t h e l ong t e r m , tO-%- o f women- had- a-hysterectomy because o f adverse progestogemc symptoms
N o n - o r a l oestrogen dehvery One o f the main benefits o f non-oral oestrogen dekvery i s t h a t any p o t e n t i a l t h r o m h o -t i c tendency is minmuzed by the avoidance o f first-pass hepatic metabolism There are
804
••Jie. L U E I i l l i 1 I I J ; L * . I) i n IlM I ' II UiU 1(_ t £ | | j l i l l U l ! - l l l HJ l l I ' l i l . i H'l
Fig 8 Different routes of oestrogen delivery Mean hormone levels achieved (Englund and Johansson, 1977,1978, Thom et al, 1981, Studd et al, 1990, Stanczyck, 1991) F = follicular, L = luteal, M = menopausal, 0 = ovarian
other advantages m t h a t oral oestradiol administrat ion results m a ' ro l ler coaster' 24-hour prof i le of oestradiol concentration H i g h levels o f oestrogen ^ p e a r m the systemic c irculat ion w i t h m a few hours o f mgestion^foEowed hy a. steady dedme such, t h a t levels have fallen t o near baselme before the next dose is due I n addiUon, there is a complete reversal o f the physiological 2 1 oestradiol oestrone rat io so that the latter predommates I n comparison, b o t h transdermal patches and subcutaneous oestradiol implants mamtam the 2 1 rat io o f oestradiol oestrone and produce far more stable hormone profiles (Smith and Studd , 1992) (Fzg 7)
T h e f trst transdermal oestradiol dehvery system, Estraderm T T S incorporates oest rad io l m an alcohol reservoir contamed w i t h m an adhesive patch (Padwick et a l , 1985, Whitehead et al , 1985) W h i l e generally very w e l l tolerated, there are some cluneal problems Y o u n g women, par t i cu lar ly , may f m d the contmual wearmg o f an adhesive patch an embarrassment, a n d there may also be adhesion problems, espeaaUy m h o t weather PeAaps the most c ommon complamt is skm reactions M m o r topica l reactions were f ound m 2 0 % o f study weeks by Place et al (1985), whde Bel lantom et al (Wt) found some tmtation at the patch site m 20 o f 28 women These data almost certainly overestunate the size o f the p r o b
lem, b u t nonetheless skm i r r i t a t i o n is a significant problem fo r a m m o n t y of women and m a few may necessitate withdrawal of treatment M o s t such skm reactions are t h o u g h t t o be an i rr i tat ive response t o the alcohol m the drug, reservoir N e w transdermal patches wh i ch ut ihze different technology m order t o mimmize such skm problems are now undergomg clmical tnals , and should be available m the near future
The admmistrat ion o f cychcal norethisterone transdermally m a combmed oestrogen/progestogen patch has recently been reported (Whitehead et a l , 1990) Whether this w i l l have any advantage over oral progestogen remams t o be seen
Subcutaneous ©estradiol implants, while havmg the convenience o f 6-monthly admmistrat ion and the improved comphance resulting therefrom, have the added advantage o f bemg able t o elevate oestradiol levels higher i n t o the normal premenopausal range than any other currently available route o f oestrogen admimstrat ion, such that the mean oestradioTTevelof767 p m o F htre achieved w i t h long-term use is roughly midway between physiological midluteal phase and preovulatory levels (Gamet t et al, 1990) (Fig 8) Such oestradiol levels are an advantage m women w i t h l o w bone density because they achieve a greater increase m bone density over 12 months than do the levels achieved w i t h either oral or patch
806
Recent advances m hormone replacement therapy
therapy T h e po tent ia l disadvantage is. t h a t some women may develop supraphysiolo-gical oestradiol levels G a m e t t et al (1990) f o u n d this so-called tachyphylaxis m only 3% o f long- term implant users M o s t o f these women had been receivmg repeat irnplants at b o t h a higher dose and a shorter mterval than recommended, and had a h igh mcidence of psychiatnc disorders I t seems that such women require frequent h igh doses of oestradiol t o keep symptoms at bay, this may wel l be a manifestation of a dose-response effect between oestrogen and m o o d I n practice, a l though startmg doses may be 75 or 100 m g , eventual maintenance doses should m general be 25 or 50 m g every 5-6 months I f used correctly m this manner b y a chnician alert t o the potent ia l problem, tachyphylaxis should n o t occur "Where supraphysiotogical levels already exist, the correct management i s t o contmue therapy b u t at reduced dosage u n t i l levels faU t o w i t h i n the physiological range Complete wi thdrawal o f oestrogen wou ld be b o t h unnecessanly harsh and potential ly
erous
KEY POINTS
One^trievery^livaof ̂ pioputetion inEngfa^ ctimacterte or postmenopausal womm
• Oestrogen therapy fnci^ses bone density m a dose-dependent manner
• O^trogen therapy reduces the risk of Ischaemic heart d&ease iiy over 40%
• ConfraindicMtons to the oraf eontraceptiye piil such as heart disease, hypertension and thrombosis do not apply to hormone replacemeni therapy (HRT); Indeed, these are indications for HRT
• The overaii effect ot HRT upon breast cancer Is probatiiy neutral
• Oestrogen can be effective treatment for ctimacteric depression and cyclical depression of premenstniat syndronw when approaching ttie menopause.
• Ovum donation is an effective bvatment for fiie InfertUIty of premature menopause
• Non-oral oestrogen administraflon residts in more physiofogfcaf ieveis and is potentially safer
• AX prmntihe uw (ff tajnttiraou* ©>mW»<rregla»iw oimt or liysterectomy are the best means of avoiding withdrawai t)ieeding.
Conclusion. T h e past decade has produced data demon-stratmg that H R T has even greater benefits t h a n previously thought by those who f i rs t recognized the chmactenc syndrome as just h o t flushes, sweats and vagmal dryness I t i s n o w apparent that the role o f H R T m osteoporosis is no t merely preventive b u t also remedial Evidence is emergmg t h a t oestrogen may have a major place m the treatment of depression, and i ts potent ia l t o reduce the mcidence of I H D by the order o f 4 0 % IS probably o f greater importance t o the prevention o f heart disease m women t h a n any other discovery
Undoubted ly the resumption o f menst r u a t i o n and the cychcal symptoms of m o n t h l y progestogen are strong factors, reducmg uptake and compliance, b u t use o f contmuous combmed regimens can avo id this I n view o f the potent ia l bene&ts o f H R T , hysterectomy should be more readdy offered Overall the data do n o t mdicate t h a t the nsks f r o m breast cancer are mcreased by H R T
I t IS tune that gynaecology ceased t o be the on ly branch o f the medical profession aware of the importance o f H R T I t is tune for cardiologists, psychiatrists, neurologists and general physicians t o accept that oestrogen replacement has an impor tant role m preVeWtJfve 'medtcme w i th in - theSf own- practice Every menopausal woman should be offered the potenttal beneffts o f H R T , b u t particularly those w i t h heart disease, depression and osteoporosis These are the very patients who are often demed H R T fo r illogical, reasons
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