- Email: [email protected]
Plasma dexamethasone and the dexamethasone suppression test
Journal o/ 4//ecrrw
Drsorders
IS (1988)
9?-100
El>eXler
JAD
00554
Plasma dexamethasone
and the dexamethasone
Irutlal and follow-up tests In depressed Gordon
F Johnson
suppression patients
‘, Glenn E Hunt ’ and Ian Caterson
i Rews~on
recel\ed
(Accepled
28 Januan
9 Fehruan
test
’
1988)
1988)
Plasma dexamethasone concentrations FoUowlng oral dexamethasone adnumstratlon v.ere exammed In 78 patients with major depression pnor to and dunng treatment The test-retest stablhty of plasma dexamethasone levels wltlun patients aas satlsfacton Hlth an overall slgruflcant posltlve correlation between tests for each patient However slgruflcant \anability was noted in lndlvldual patients Change in pre-DST cortlsol and plasma dexamethasone levels were the tHo vanables m that order of importance contnbutlng to change m DST status In studies exanunmg the cluucal utlhty of senal dexamethasone suppression tests as a guide to recolen from depresslon. the effect of banabilIty m plasma desamethasone concentrations should be taken into account
Key nsords
Dexamethasone
suppression
test, Test-retest
Introduction
In patients with depression, falure to adequately suppress plasma cortlsol followmg a dexamethasone suppression test (DST) has been advocated as 3 laboratory ad m the diagnosis, and
Address for correspondence fcssor ne\
Department
N S W 2006 Prebmmarv
of Psyclua~n
G F Johnson Um\erslty
-
0165-0327/88/$03
Shd-
Auslraha
results of ISIS study were presented al the 4th
World Congress on B~oloncai Pstch~atn _ 1985
4sscx1a1e Proof S\dne\
Phtladelphta
U S 4
stablhty,
hl;?lor depression
normahsdtlon of cortlsol response during treatment. as a guide to chmcal outcome (Carroll et al . 1981, Greden et al. 1983) The mechamsms underlymg abnormal cortlsol response to dexamethasone m depressed patients are complex but major determmants of non-suppresslon are cortlsol hypersecretion dnd the a\h~lablhty of plasma deuimethasone (Poland et al 1987) Wide lntra-lndl\ldual vanablhtb in plasma dexamethasone concentrdtlons occurs followmg dexamethasone adrrurustration and there IS an mberse cunlhnear relatlonskp between plasma cortlsol and plasma dexamethasone with slgmflcant differences In plasma dexamethasone levels
50 I 1988 Elsewer Science Pubhshers B V (Blomedul
Dlklslon)
94
between suppressors and non-suppressors dt alI samplmg times (Holsboer et al 1984 Johnson et al 1984 Arana et al 1985 Carr et al. 1986) Therefore failure to suppress plasma cortlsol ma\ result from altered hypothalanuc-pltultarqadrenal (HPA) aus function associated mlth depre5slon hut It ma\ also be deternuned by lo\i plabma dexamethasone levels Moreover. dose-response studies suggest that \ahd categonsatlon of de\amethasone huppresston status can best he made u hen plasma delamethasone levels he ~lth~n a defmed range or mmdob Tlus detects patlent> Hhohe plasma dexamethasone levels are too Ion or too hqJ~ leadlng to false-posltlbe or false-negatl\e result5 respectIveI> (Johnson et al 1987) Recently. test-retest \ranablllt> of plasma dekamethahone concentrations has been reported (Johnson et al. 1986 Berger et al 1985 Baumgartner et al 1986, Holshoer et al 1986 Carson and Halbrerch. 1987) Where change In DST 3tatus ulth benal testing IS to be used to monitor cluucal recovery. changes In plasma dexamethasone levels may confound the slgruflcance of change m DST status particularly normahsatlon The follobmg report exanunes the stablhty of plasma dexamethasone concentrations hetkbeen tests m 78 patients with major depresslon and evaluates the contnbutlon of change m dekamethasone concentratlonb and change m predexamethasone plasma cortlsol levels to altered DST status Methods
Patients mlth maJor depression uere selected from consecutl\‘e adrmsslons to the Affective DISorders LJtut. Royal Prince Alfred Hospital Dlagnoses were made Independently hq two psychsatnsts usmg DSM-III cntena (Amencan Psycluatnc Association 1980) A 2-5-day basehne stahlhsatron penod was obsened pnor to the Imteal DST Patients were rated on a 21-Item Hamilton Rating Scale for Depression (Harrulton 1960) Routine laboratory tests Included h\er and thyroid function tests and the usual exclusion cntcna nere applied as detailed elseuhere (Carroll et al 1981. Johnson et al 1984) During treatment and pnor to discharge cluucal ratings and a repeat DST aere obtained In 78
patients out of 145 consecutlbe adrru~~lons \\lth m.qor depresblon Special effort> were taken to obtain a follow-up DST In patients who were non-suppressor> on the lmtlal test Flfti-se\en ot the 145 consecutl\e admIssIons Here non-supprebsors on rrutlal testing of which 37 had a repeat DST The other 41 patients that had a repeat DST Here suppresborb on the mltlal tebt T\\entb-se\en of the Inltlal patient3 sampled \\ere part of a pre\ IOUS report In\ esttgatlng plasma dekamethasone and plasma cortlsol and DST (Johnson et al 1984) Patients recelred chmclan’b choice of treatment such as electrocon\ulsr\e thrrapq (ECT) or antrdeprebsant< Adequac! of antldepressant drug treatment was morutored by routine plasma Ir~el ashay Pm edures
The DST procedure has the same on adnusslon and dl.scharge Blood for plasma cortlsol teas collected at 4 p m on day 1 and tbo 0 5mg tablet5 of deuamethasone \\ere adnutustered orally at 11 p m On da> 2 blood \\as collected for corttsol and dexamethasone assay at 8 a m and 4 p m The cntenon for non-suppression \\a5 a plasma cortisol concentrdtlon greater than 139 nmoljl (5 pg/dl) Plasma cortlsol was measured hq radlolmmunoassaq (RIA) (Chmcal Assaks Cambndge. hlA) The Intra- and Interassav coefflclents of Lanatlons uere less than 105 Dexamethabone was also measured by RIA. the standard used was 9n-fluor-lip 17 21-trlhvdrouh-16n-methyl-l 4pregnadlen-3.20-dlone (Stcralolds WIlton, NH) and the tracer \\as [6 7(n)- ‘Hjdevamethasone (New England Nuclear Boston MA) The antiserum to deramethasone was from RIA-Labor (Prof Vecsel Pharmakologrsches lnstltut der Unrversltat Heidelberg) The mtra- and Interassaq coefflclents of lanatlon \\erre less than 100; and the assay \\as sen>ltl\e to less than 0 3 nmol,#l Several btudles have reported the cross-reactlrlty betueen dexamethasone and cortlsol to be less than 25 (Hlchenb and Hogans 1974 Enghsh et al 1975 Kaaal et al 1985) and the cross-reactlon between devamethasone and its maJor metabohtes, h-hqdroxy-deuamethasone and 20-dlh>drodexamethasone to be less than 14 (English et al 1975)
The data were analyed using chl-sqtwe Imear regresslon analysis of vanance nlth repeated measures and multtple regression analysis usmg a standard statlsttcal package (Not-us15 1985) The results In tables and text are eupresbed ~5 mean f SD Results Details of the 78 patients studled and thetr DST status (suppressor or non-suppressor) on adnuwon and pnor to discharge are shown m Table 1 DST status did not change m 44 patients hho uere either suppressors (group 1 II = 32) or nonon both test5 (group 4. 11= 12) suppressors Change from non-suppresston to suppresslon occurred In 25 patients (group 3) and con\ersel> from suppresston to non-suppresslon m rune patlents (group 2) There Here no slgmftcnnt dlfferences bet\\een the four DST groups and age Height. gender. duratton of hospltahsatlon or proportlon of pattents Hlth melanchoha (Table 1) Seventy of depresslon as measured by the 21-Item Harrulton Depresston Rating Scale Has not stgtuflcantI! drfferent between suppressors and non-suppressors on mltlal rutmg or pnor to discharge Furthermore. none of the subfactor scores on the Hanulton scale were slgruflcantly dtfferent be-
TABLE
tHeen the groups Smular chrucal Improvement ds reflected bv decreased Hanulton scores pnor to dtscharge uas observed In all four groups (Table 2) 41~0. there Here no slgmflcant differences In treatment allocatIon such as ECT or sntldepressant medlcatton between the groups (Table 2) Mean plasma dexamethasone concentrations mere slgruftcantI\ different beween suppressors and non-suppressors on both lrutlal and follow-up testmg On Inltlal testing the plasma dewmethdsone concentratlom In suppressors \\ere bgher compared to non-suppressors at 8 J m (11 7 + 5 5 1s 79+31 nmol/l) and 4 pm (43t27 \s 25kl 1 nmol/‘l) (I= (1 76)=1339 and 1383 P < 0 001. re5pectl\el>) Slnular differences \\ere obsened on folloa-up between suppressors and non-suppressors at 8 a m (13 1 f 5 2 ~‘5 9 3 f 6 5 nmol/l) and at 4 p m (4 S f 2 7 15 2 7 f 1 6 nmol,/l) ( F = 7 02 and 8 60. P < 0 005 respectirelb) The 4-p m plasma deuametha\one lebels on first and second testmg (DSTl and DSTZ) are shoHn for each pattent In Fig 1 Overall there WJS a posrtlve correlation between 4-p m plasma dexamethasone levels between tests for all patients (r = 0 62) Hoaeker conslderable differences betHeen tests occurred In some patients Afternoon dexamethasone concentrations waned more than
1
DET4ILS
OF P4TIENTS
WITH
MAJOR
DEPRESSION
ON
suppre\sors
Suppre,bor
on both
non-supprebwr
(group
1)
(group 2)
10
ADh~ISSIOlu
AND
PRIOR
TO DISCHARGE
(n = 78)
Non-
Non-
Total
suppressor
suppressor,
(hfean _+SD)
lo suppresbor
on both
(group 3)
(group 4)
hlales
13
4
9
7
33
Female\
19 -
5 -
16
5
45
37 L
9
25
12
7x
4ge
51
36
48
58
49 & 2
Weight (kg) Da\\ heluecn
66 5
64
59 4
63 1
64 t
32
31
36
35
34+’
Total
1SStS
DSM-Ill Mqor
1
draqnosrs depresslon
with melanchoha ~lth pswhow features onI\ ’ Numbers
”
I6
5
13
4
38
14 (6)
4
10 (3)
5 (31
33
2
0
2
shown m parentheses are Ihe wbset of pauents \slth mel~choha
3 and psvchotlc feaures
7
1
1 7 nmol m 22 patients (1 7 = standard error of the estunate for the lmear regresslon equation). and for ten of these patients the \anahlhtj mas greater than 3 4 nmol/l (Patients 20 25 28 29. 30. 32. 34 50. 66. 75. FIN 1 ) Mean plasma devamethasone levels remalned relatl\ely stable In the tno groups *hose DST status did not change although the absolute concentratmns were h&er m the suppressors on both tests compared to the non-supprebsors (two upper panels Fig 2) Thus IS In contrast to the tugher mean plasma dexamethasone levels on the second test m patrents that changed from non-suppressor to suppressor (lower nght panel Fig 2) Thus Increase was pnmanlq due to SLYpatients H hose dexamethasone levels rose from a range of 2-4 to 4-10 nmol/l (patrents 20 29 32 35. SO and 68 Fig 1) Conversely there was a fall m plahma dexamethasone on the second DST m tao of the rune patients that were suppressors on Irutlal sampling. and non-suppressors on folkw-up testing (patients 1 and 30 Fig 1) In one female patient from group 2 (patient 30). plasma dexamethasone fell from 10 5 to 1 2 nmol/l on retesting Thus patient had a kstory of I v drug abuse and be-
cause she was ldentlfled a5 an outlrcr she nds excluded from the analqsrs The slgmflcant sbfts m plasma drxamethasone that occurred m some patients could not be explamrd b> age wevght. se\ (open and filled circles In Fig 1) or presence of melanchohc feature> (patients 39-71) hloreobrr treatment per se did not explain the dramatlc shfts m dexamethasone concrntratlons between tests The net change In 4-p m plasma dexamethasone from test 1 to test 2 In the three patients treated Hlth loa-dose benzodlazepmes bias 0 2 nmol,‘l. m the 40 patients takmg antidepressants the Increase was 0 5 nmol/l for the >e\en patients takmg antldeprcssants and hthwm there NJS a net Increase of 1 5 nmol/l and for the SLX patients takmg both antidepressants and neuroleptlcs the net glun uas onlb 0 1 nmol/l The effect of ECT on plasma devamethasone levels was slnular to the group @Len antldepressants wth a net gam In deuamethasone of 0 6 nmol/ I on the second DST Pre-DST plasma cortlsol values on mltlal and folk\\-up testing are Illustrated In Fig 2 for each of the four groups Pre-DST plasma cortlsol concentrations uere lugher in non-suppressors (447 +
97
12
10
0
MALES
0
FEMALES
8
8” 8
6
4
2
(I
suppressors on Fig
1 Afternoon
lo discharge
(4 p m
(DSTZ)
) plasma
male pallenls
ulth
concentrahons
mayor deprewon
17 h folloamg
Numhers
1-38
on
1 mg dexamethasone Into four group,
both
on adnusslon (DSTl) accordmg
of 139 nmol,‘l
are patients ullh
features
DST2
non suppressors
suppressor
corhsol cnwnon
are pauenls ulth prvchotlc
191 nmol/l) compared to the suppressors (314 f 179 nmol/l F = 9 66. P < 0 005) Seventy-four per cent of the non-suppressors had afternoon (4 p m ) pre-DST cortlsol concentrations abobe 300 nmol/l on the uutlal test. whuzh IS above the 9S? confidence mtenals for normal controls There was a fall m pre-DST cortlsol on folio\\-up testing m patients who suppressed on both tests or whose
DSTl
nonsuppressor to
on borh teals using a posr-dexamelhasone
and numbers 72-78
DSTZ
Pauenrs are dlwded
and fllled Lucles Indicate female patlenls
are pattents ulth melanchoha
DSTl
to
nonsuppressor
dexamethasone
In 78 pauents
DSTZ
suppressor
both
(suppressors or non-suppressors) mdlcate
DSTl
DSTP
DSTl
10 their
(5 pg,,dl)
major depressmn
and pnor DST
EMU\
Open circles
number> 39-71
Mean Lalues for each column appear In Fig 2
DST status changed from non-suppresslon to suppresslon (upper left and lower right panels. Fig 2. respectively) Pre-DST cortlsol values were hqgher on retestmg m the patients that snItched from suppressors to non-suppressors (louer left panel) and remalned elevated throughout hospltahsatlon In the patients that were non-suppressors on both tests (upper r&t panel) Three of the SIX patients
9x
Flp
2 Afternoon
connectmg
(3 p m
groups according rerpecu\el\
cornal
Ths MC) bottom
alrchcd
non-suppresston
plabma sorucol (whd
tDSTlt
and pnor
to thelr DST SIJIU~ on adnuwon
right panels rhow pre-DST SMUI
I pre-DST
cIrcIes) on ndrm,smn
from
and pnor
and dexamethaone IO non-bupprewon
IO supprewon
(loner
quarest
to dwhrlrge
(loser
Isft
right panel) lndute
~+lth rdlsed dexamethasone lebels on follow-up from group 3 (patients 32 35. 68) had elevated pre-DST cortlsols throughout hospltahsatlon Stepwse multlple regresston analysis mdlcated that differences m pre-DST cortlsol values from test 1 to test 2 could explain 195 of the lanablhty In post-DST cortlsol values A further 6% of the vanabthty could be evplalned by changes In plasma dexamethasone levels No other variables such as age. sex, or treatment dunng hospt ahsatlon. had a slgmflcant Influence on predlctlng change In postDST cortlsol values Analysts of the residuals mdlcated no sequential effects ober time of study equahty of vanance and a normal dlstnbutlon A multtple regression analysis of all patients uho here non-suppressors on dt least one test (groups 2, 3 and 4) mdtcated that the drfferences rn preDST cortlsol levels \bere kghly correlated Hlth changes In post-DST corttsol lebels (r = 0 52) and could account for 27% of the kanabrhty As before differences m plasma dexamethasone levels mere negatively correlated v+tth change In postDST cortlsol (r = -0 34) and could explam a further 7’F of the vanabIlIty
and dcxameth~ronr
In 7X depreurd
Lortlwl
pAneI)
patents
concenrr~wn~
Patlent:. uerr
ullng rl cor~~~ol cn~enon of 139 nmol
plasma levels 111wppreaors
panels Illustrrlte the change> In pre-DST
suppressmn
t DST pou~l\e)
bnes connecung
IO discharge (DSTZ)
and
I
an both tests and non-uppres,ora
and plJ\nu In pdtwnt,
dr\ameth~wnr uhose
DST
tdotwd
dl\lded lipper
left and
on both W>I~
In parwnrb uhow SUIU>
The number ot patwnrs In rJLh group 13 g\en
Ilnex
Into four
nornulwd
DST from
In Table 1 T-burl
1 SEhf
Dwuwon
Vanablhty In plasma de\amethasone concentrations was exanuned In 78 patient> nlth major depression pnor to and during antidepressant treatment The test-retebt stablhty of plasma dexamethasone concentrations hlttun patients UJS ~lth an overall slgmflcant posItIke satisfactory correlation between plasma dexamethasone Ielels between test> for each patient However mdt\ldual analysis shoaed wide differences In dexamethasone concentrations m some patients at both 8 a m and 4 p m Ths uas ebldent both m patients whose DST status did not change between tests buch as those \rho Here suppressor5 throughout, and In those In \\horn DST status changed on follow-up testmg The extent of change In plasma dexamethasone concentrations was substantial m some patients hlth 4-p m plasma dexamethasone levels varying by a factor of more than 1 7 nmol/l m 22 patients and In ten of these the difference betbeen tests nas greater than 3 4 nniol/l
Preblous reports habe dlffered on the extent of test-retest stablIlt of plasma dexamethasone and Its chrucal slgruflcance Carroll et al (1980) reported only nunor banablhty rn plasma dexamethasone concentrations m four patients studied dunng Illness and after recovery despite change in DST status from non-suppression to suppression Honever. Berger et al (1985) reported substantial vdnatlon rn plasma dexamethasone levels at 9 a m In 12 patients Hlth at least three senal DSTs dunng hosprtahsatlon They concluded that there was a hnuted mtra-mdlbldual stablhty of dexamethasone pharrnacokmetlcs Smularly. Baumgartner et al (1986) reported wide mtra-lndl\ldual vanatlon In dexamethasone concentrations dunng senal testing m 26 patients with major depressl\e disorder A progressive fall m mean post-dexamethasone cortlsol concentrations over 5 weeks however \\as not accompamed by any slgmficant changes In mean dexamethasone concentrations It was concluded that tlus has not a slgmflcant factor m change m DST status Holsboer et al (1986) reported a slgmflcant nse In plasma dexamethasone concentration In 31 depressed patients who showed lrutral non-suppresslon of cortrsol. but Bho became suppressors dunng treatment. whrle 14 patients uho were suppressors on both tests sho\hed no slgruflcant difference In deKamethasone concentratrons In contrast. Carson and Halbrelch (1987) reported no slgmflcant change overall In plasma dexamethasone concentrations m 15 patients with major depression pnor to and durmg treatment mcludlng those whose DST status changed from non-suppresslon to suppresslon However. slgmfrcant banability was noticed In mdlvldual patients. particularly those v. ho remained suppressors throughout. suggesting an effect of treatment or change In chrucal status, on dexamethasone pharmacokmetlcs The mecharusms underlying vanablhty m dexamethasone concentrations are uncertam but may result from changes m absorption. metabohsm or ehmmatron of dexamethasone Holsboer suggested that a ION plasma dexamethasone level In nonsuppressors ts a state-dependent phenomenon resulting from accelerated metabohsm of dexamethasone wluch normabses on chrucal recovery Whle such a general trend was not observed m thrs study tbs mecharusm cannot be excluded m
the SIX patients who showed marked increases in dexamethasone levels associated ulth change in DST status from non-suppression to suppression Test-retest differences did not appear to be dssoelated with treatment allocatlon. either ECT or antidepressants or the presence of other psychotropic drugs The slgmflcance of althm-patient Lananon in plasma dexamethasone levels depends on the extent and direction of the change m plasma levels lrutlal DST status, and concurrent changes in predexamethasone plasma cortlsol A nse m plasma dexamethasone levels m patients who are uutlal suppressors or a fall m patients Hho are uutlal non-suppressors IS hkely to be of less slgmflcance than a nse m plasma dexamethasone m mltlal non-suppressors or a fall m uutlal suppressors that may contnbute to change m DST status Thus IS Illustrated m three of the SIX patients with railsed plasma dexamethasone levels on follow-up whose change In DST status from non-suppressor to suppressor occurred despite elevated pre-DST cortlsols throughout hospltahsatlon Recent studies by Holsboer et al (1986) and Wledemann and Holsboer (1987) report that early blophase lunetlcs of dexamethasone are rndlstmgulshable among DST suppressors and nonsuppressors, raising doubt as to the Importance of actual plasma dexamethasone levels 9-17 h following adnumstratlon In deternunmg DST response Studies to examme the relatlonsbp between early blophase kmetlcs and plasma levels 9-17 h followmg and the relatlonshrp to plasma ACTH-cortlsol response are currently under day In our laboratory Whole change m plasma dexamethasone levels was a slgmflcant deternunant of change m DST status m some patients difference In pre-DST plasma cortlsol levels between tests uas the most Important deternunant of change In post-DST cortlsol lebels Thus IS consistent with other studies showing cortlsol hqpersecretlon to be a slgmflcant detemunant of non-suppresslon of plasma cortlsol followmg dexamethasone adnumstratlon (Asms et al, 1981. Poland et al. 1987) The changmg Interactions between pre-DST plasma cortlsol and plasma dexamethasone dunng treatment appear to largely determme the test-retest differences In DST status
In the majonty of patients chrucal Improvement, as measured by change m Hanulton scores on follow-up. uas accomparued by a fall m preDST
plasma cortlsol
To the extent that elevated
4-p m plasma cortlsol concentrdtlons are d rehdble Index of Increased HPA axis function (Astus et al 1981, Chnstensen et al 1985). their fall durIng treatment with a concurrent change from non-suppresslon to suppresslon m some patients 15 conslstent with reports that normahsatlon of the
Chnstensen L
t 19851 rwn
J
Dlsord
Chn BJ
and
J
hfarkb
R
Kronfol
Z
Pavctiatrv
Holsboer
hl (1960)
tlcal Manual ctuatnc Arana
Assoclatlon
of hlental
Assoclatlon
G W
G hf
Sachar
Ostron 138
Arch
3rd edn
E J
and Stall>-
Amencan
Psb-
M
(1985)
Psq&atn
Halbrelch
U
F S (1981)
42
The
and progNathan
R
Cortlsol secretIon and
response m depressIon
Am
J
Pswzhratn
D
dersmethasone F
A
Haack
D and Vecsel
P (1986) Senal De~a-
Gerken
K
half-bfe Gen
G
Hunt
methasone
M
Parke
K -M , Kneg
The effect of #e&t
dexamethasone
18
levels
J-C
and
Von Zerssen
loss and mappropnate
on
the
DST
P\vchatr
D
plasma Re,
15
351-360 V
Moms
H
and Gdhland
serum dexamethasone BJ
Schroeder,
Femberg
M
methasone rponse
Metab Felnberg
Haskett
R
James
DeVlgne
(1986)
and
of
tn the dexamethasone
Mukhopadhvav
ulth
The effect
Johnson
S
Greden
J (1980)
cortlsol
endogenous
J F
Plasma dexa-
suppressjon
depresston
J
reClan
bup-
m dcprss-
E (1986)
Shortened non-
813-815
A
kanable
and Boll
E 11986)
m deprebw~n
htophase hmetlo Kerr
tcst-re-
Ps\chatrv
K
md
Reb 17
I
Catcrson
test (DST)
G
Hunt
G
\one levels Johnson
G
Kerr
K
supprewon
(1984)
and plasnw Pbbchatr
Proceedings
IV World
Phladelpba Hunt
G
U S 4
Kerr
dekamethasone test
K
plasma
dexa-
Res
13
(1986)
The
dexametha-
Congress on Bmlo@cal
Elsekler
Amsterdam
I
and Caterson
nlndo\s
In
1
and Catcrson test and
11987)
The
and the devamethasone
depresslon
N
Greden MLI
J and Young
J F
, Kronfol
Tanka Z
J
Lobr
Albald N
A
Stemer
E (1981) A speclflL laboraton Arch
Gen
Psvcbatn
SW
213-216
S
Ich&.wa
metabolic
and Halbrelch cortlsol
U
1
Blol
and Homma
propertles
dexamethasone
m
among
Ps\cbatn
Il\er
22
Endocnnol
Metahol
M J (1985)
Poland
R E
(1987)
and dexamethasone
Effect of treatment Btol
Psbcluatn
on 22
accelerated
flulure
J
Chn
60 848-854
SPSS-Y
Rubm
Advanced
R T
Lesser
Neuroendocnne
depressmn
SI~IISIICS Guide
II
Serum
Pshchatn K
sane bnetlo admuustratmn
I
hf
Lane
LA
aspects of pnman
deuamethabone
hvpoth~amcFpltult~,n’-adrcnal
Wledemann
dl>ea>es
In rend
m and
hlc-
Cbcago
P J (1987)
Gen
Dlfferenceb
predntsolone
mind rend
of dexamethasone
Norusls
hl (1985)
cortlsol
metdboh,m
1340-1348
18 15-22 pla>ma
Kaua~
nantr of the dexamethasone
51 433-437 M
test for the &agnosls of melanchoba Carson
(198-I)
19 2X1-291
Gerken
supprewon
dexamethasone
Gras-HIII
21 735-743
and Tanka,
concentrations
EndoLnnol BJ
K
, RIC~K J
In pattents
J
concentrations
suppresslon test BIOI Psychatry
M
P
1015-1039
(1985)
Carroll,
\ecsel
and dlfferenual
levels III depressed pa:lent>
suppressmn
Carroll
and
Psvcluatrv 43
G
Desamethasone
Res
Carr
4
for
97-103
The mfluence 45-64 Bergcr
Neuro-
20 266-271
and Boll
K
test ,tudles and earl\
plasma
Psvchtatr
Arch
m depressed dcvamcthasone
Wledemann
Pan III
banables
The pro-
J Nsurol
Chem
BIOI Ps\cbatn
Arch
methasone SuppressIon Tests In psvch~atnc Illness of mtenemng
Carroll
of melJncholla
concentrations
Wledemann
Pskcbatn
1218-1221
Baumgartner,
L
Supprerslon
305-313
1193- 1204
&an-u
Grunbau\
response of cornsol and CortIcosterone F
Johmon
DC
Test for dlagnow
Gen
L and Halpem
dexamethasone
Dtagnostlc
R J and Omsteen
SuppressIon
noIts m psqcluatry Asms
Dlsorderr
Washmgton
Baldessanru
Dexamethasone
(1980)
D
Dexamethasonr
Chn
The plasma dexamethasone Psvchatnc
J
4 F (1974~ Radw1mmunodb,a\
m plasma
Haack
suppressors
Amencan
9
Eur
4 ratmg for dcprebslon
sI\es and control>
Holsboer
(1975)
treatment
Plasma dexamethasone
Holsbocr
4
and test-retebt reproduclblht\
and Hogans
pre,slon
V and Parhe
23 56-62
dexamethasone F
H ‘I
III deprcs-
40 493-500
.rurg Psbchatn
cal recovery m patients Nlth depresslon should. however, take mto account the effect of \anahlhty
cortlsol
for dexamethasone
hng (1983)
Tebts m antIdepressant
hl
Chn>tenwn
9 239-244
Gardner
cew of normallratlon Gen
P
and Thomsen
plasma
procedure
Pharmacol J F
0 L
8 271-278
Chahrabortb
Greden
Kragh-Sorenwn
Pedersen afternoon
radlolmmunoassa\
Hlchem
References
L F
C B
J 4ffec1
Enghsh
Studies exanunmg the chmcal utlhty of the dexamethasone suppresslon test to motutor chru-
m plasma dexamethasone concentrations To do ths requires simultaneous measurement of plasma dexamethasone and plasma cortlsol
Gram
Spontansous
Harmlton
DST comcldes with chrucal Improvement
P
Knrtensen
and Hart endogenous
concentratmns
cortical suppres\ton
rlctnlt\
dnd
as deternu-
test response
4rLh
44. 790-796
and Holxhoer dunng of
F
the DST the
te\t
(1987) after drug
Plasma dewmethdoral and Intra\enou\ BIOI
Ps\cbJtn
72
Drsorders
IS (1988)
9?-100
El>eXler
JAD
00554
Plasma dexamethasone
and the dexamethasone
Irutlal and follow-up tests In depressed Gordon
F Johnson
suppression patients
‘, Glenn E Hunt ’ and Ian Caterson
i Rews~on
recel\ed
(Accepled
28 Januan
9 Fehruan
test
’
1988)
1988)
Plasma dexamethasone concentrations FoUowlng oral dexamethasone adnumstratlon v.ere exammed In 78 patients with major depression pnor to and dunng treatment The test-retest stablhty of plasma dexamethasone levels wltlun patients aas satlsfacton Hlth an overall slgruflcant posltlve correlation between tests for each patient However slgruflcant \anability was noted in lndlvldual patients Change in pre-DST cortlsol and plasma dexamethasone levels were the tHo vanables m that order of importance contnbutlng to change m DST status In studies exanunmg the cluucal utlhty of senal dexamethasone suppression tests as a guide to recolen from depresslon. the effect of banabilIty m plasma desamethasone concentrations should be taken into account
Key nsords
Dexamethasone
suppression
test, Test-retest
Introduction
In patients with depression, falure to adequately suppress plasma cortlsol followmg a dexamethasone suppression test (DST) has been advocated as 3 laboratory ad m the diagnosis, and
Address for correspondence fcssor ne\
Department
N S W 2006 Prebmmarv
of Psyclua~n
G F Johnson Um\erslty
-
0165-0327/88/$03
Shd-
Auslraha
results of ISIS study were presented al the 4th
World Congress on B~oloncai Pstch~atn _ 1985
4sscx1a1e Proof S\dne\
Phtladelphta
U S 4
stablhty,
hl;?lor depression
normahsdtlon of cortlsol response during treatment. as a guide to chmcal outcome (Carroll et al . 1981, Greden et al. 1983) The mechamsms underlymg abnormal cortlsol response to dexamethasone m depressed patients are complex but major determmants of non-suppresslon are cortlsol hypersecretion dnd the a\h~lablhty of plasma deuimethasone (Poland et al 1987) Wide lntra-lndl\ldual vanablhtb in plasma dexamethasone concentrdtlons occurs followmg dexamethasone adrrurustration and there IS an mberse cunlhnear relatlonskp between plasma cortlsol and plasma dexamethasone with slgmflcant differences In plasma dexamethasone levels
50 I 1988 Elsewer Science Pubhshers B V (Blomedul
Dlklslon)
94
between suppressors and non-suppressors dt alI samplmg times (Holsboer et al 1984 Johnson et al 1984 Arana et al 1985 Carr et al. 1986) Therefore failure to suppress plasma cortlsol ma\ result from altered hypothalanuc-pltultarqadrenal (HPA) aus function associated mlth depre5slon hut It ma\ also be deternuned by lo\i plabma dexamethasone levels Moreover. dose-response studies suggest that \ahd categonsatlon of de\amethasone huppresston status can best he made u hen plasma delamethasone levels he ~lth~n a defmed range or mmdob Tlus detects patlent> Hhohe plasma dexamethasone levels are too Ion or too hqJ~ leadlng to false-posltlbe or false-negatl\e result5 respectIveI> (Johnson et al 1987) Recently. test-retest \ranablllt> of plasma dekamethahone concentrations has been reported (Johnson et al. 1986 Berger et al 1985 Baumgartner et al 1986, Holshoer et al 1986 Carson and Halbrerch. 1987) Where change In DST 3tatus ulth benal testing IS to be used to monitor cluucal recovery. changes In plasma dexamethasone levels may confound the slgruflcance of change m DST status particularly normahsatlon The follobmg report exanunes the stablhty of plasma dexamethasone concentrations hetkbeen tests m 78 patients with major depresslon and evaluates the contnbutlon of change m dekamethasone concentratlonb and change m predexamethasone plasma cortlsol levels to altered DST status Methods
Patients mlth maJor depression uere selected from consecutl\‘e adrmsslons to the Affective DISorders LJtut. Royal Prince Alfred Hospital Dlagnoses were made Independently hq two psychsatnsts usmg DSM-III cntena (Amencan Psycluatnc Association 1980) A 2-5-day basehne stahlhsatron penod was obsened pnor to the Imteal DST Patients were rated on a 21-Item Hamilton Rating Scale for Depression (Harrulton 1960) Routine laboratory tests Included h\er and thyroid function tests and the usual exclusion cntcna nere applied as detailed elseuhere (Carroll et al 1981. Johnson et al 1984) During treatment and pnor to discharge cluucal ratings and a repeat DST aere obtained In 78
patients out of 145 consecutlbe adrru~~lons \\lth m.qor depresblon Special effort> were taken to obtain a follow-up DST In patients who were non-suppressor> on the lmtlal test Flfti-se\en ot the 145 consecutl\e admIssIons Here non-supprebsors on rrutlal testing of which 37 had a repeat DST The other 41 patients that had a repeat DST Here suppresborb on the mltlal tebt T\\entb-se\en of the Inltlal patient3 sampled \\ere part of a pre\ IOUS report In\ esttgatlng plasma dekamethasone and plasma cortlsol and DST (Johnson et al 1984) Patients recelred chmclan’b choice of treatment such as electrocon\ulsr\e thrrapq (ECT) or antrdeprebsant< Adequac! of antldepressant drug treatment was morutored by routine plasma Ir~el ashay Pm edures
The DST procedure has the same on adnusslon and dl.scharge Blood for plasma cortlsol teas collected at 4 p m on day 1 and tbo 0 5mg tablet5 of deuamethasone \\ere adnutustered orally at 11 p m On da> 2 blood \\as collected for corttsol and dexamethasone assay at 8 a m and 4 p m The cntenon for non-suppression \\a5 a plasma cortisol concentrdtlon greater than 139 nmoljl (5 pg/dl) Plasma cortlsol was measured hq radlolmmunoassaq (RIA) (Chmcal Assaks Cambndge. hlA) The Intra- and Interassav coefflclents of Lanatlons uere less than 105 Dexamethabone was also measured by RIA. the standard used was 9n-fluor-lip 17 21-trlhvdrouh-16n-methyl-l 4pregnadlen-3.20-dlone (Stcralolds WIlton, NH) and the tracer \\as [6 7(n)- ‘Hjdevamethasone (New England Nuclear Boston MA) The antiserum to deramethasone was from RIA-Labor (Prof Vecsel Pharmakologrsches lnstltut der Unrversltat Heidelberg) The mtra- and Interassaq coefflclents of lanatlon \\erre less than 100; and the assay \\as sen>ltl\e to less than 0 3 nmol,#l Several btudles have reported the cross-reactlrlty betueen dexamethasone and cortlsol to be less than 25 (Hlchenb and Hogans 1974 Enghsh et al 1975 Kaaal et al 1985) and the cross-reactlon between devamethasone and its maJor metabohtes, h-hqdroxy-deuamethasone and 20-dlh>drodexamethasone to be less than 14 (English et al 1975)
The data were analyed using chl-sqtwe Imear regresslon analysis of vanance nlth repeated measures and multtple regression analysis usmg a standard statlsttcal package (Not-us15 1985) The results In tables and text are eupresbed ~5 mean f SD Results Details of the 78 patients studled and thetr DST status (suppressor or non-suppressor) on adnuwon and pnor to discharge are shown m Table 1 DST status did not change m 44 patients hho uere either suppressors (group 1 II = 32) or nonon both test5 (group 4. 11= 12) suppressors Change from non-suppresston to suppresslon occurred In 25 patients (group 3) and con\ersel> from suppresston to non-suppresslon m rune patlents (group 2) There Here no slgmftcnnt dlfferences bet\\een the four DST groups and age Height. gender. duratton of hospltahsatlon or proportlon of pattents Hlth melanchoha (Table 1) Seventy of depresslon as measured by the 21-Item Harrulton Depresston Rating Scale Has not stgtuflcantI! drfferent between suppressors and non-suppressors on mltlal rutmg or pnor to discharge Furthermore. none of the subfactor scores on the Hanulton scale were slgruflcantly dtfferent be-
TABLE
tHeen the groups Smular chrucal Improvement ds reflected bv decreased Hanulton scores pnor to dtscharge uas observed In all four groups (Table 2) 41~0. there Here no slgmflcant differences In treatment allocatIon such as ECT or sntldepressant medlcatton between the groups (Table 2) Mean plasma dexamethasone concentrations mere slgruftcantI\ different beween suppressors and non-suppressors on both lrutlal and follow-up testmg On Inltlal testing the plasma dewmethdsone concentratlom In suppressors \\ere bgher compared to non-suppressors at 8 J m (11 7 + 5 5 1s 79+31 nmol/l) and 4 pm (43t27 \s 25kl 1 nmol/‘l) (I= (1 76)=1339 and 1383 P < 0 001. re5pectl\el>) Slnular differences \\ere obsened on folloa-up between suppressors and non-suppressors at 8 a m (13 1 f 5 2 ~‘5 9 3 f 6 5 nmol/l) and at 4 p m (4 S f 2 7 15 2 7 f 1 6 nmol,/l) ( F = 7 02 and 8 60. P < 0 005 respectirelb) The 4-p m plasma deuametha\one lebels on first and second testmg (DSTl and DSTZ) are shoHn for each pattent In Fig 1 Overall there WJS a posrtlve correlation between 4-p m plasma dexamethasone levels between tests for all patients (r = 0 62) Hoaeker conslderable differences betHeen tests occurred In some patients Afternoon dexamethasone concentrations waned more than
1
DET4ILS
OF P4TIENTS
WITH
MAJOR
DEPRESSION
ON
suppre\sors
Suppre,bor
on both
non-supprebwr
(group
1)
(group 2)
10
ADh~ISSIOlu
AND
PRIOR
TO DISCHARGE
(n = 78)
Non-
Non-
Total
suppressor
suppressor,
(hfean _+SD)
lo suppresbor
on both
(group 3)
(group 4)
hlales
13
4
9
7
33
Female\
19 -
5 -
16
5
45
37 L
9
25
12
7x
4ge
51
36
48
58
49 & 2
Weight (kg) Da\\ heluecn
66 5
64
59 4
63 1
64 t
32
31
36
35
34+’
Total
1SStS
DSM-Ill Mqor
1
draqnosrs depresslon
with melanchoha ~lth pswhow features onI\ ’ Numbers
”
I6
5
13
4
38
14 (6)
4
10 (3)
5 (31
33
2
0
2
shown m parentheses are Ihe wbset of pauents \slth mel~choha
3 and psvchotlc feaures
7
1
1 7 nmol m 22 patients (1 7 = standard error of the estunate for the lmear regresslon equation). and for ten of these patients the \anahlhtj mas greater than 3 4 nmol/l (Patients 20 25 28 29. 30. 32. 34 50. 66. 75. FIN 1 ) Mean plasma devamethasone levels remalned relatl\ely stable In the tno groups *hose DST status did not change although the absolute concentratmns were h&er m the suppressors on both tests compared to the non-supprebsors (two upper panels Fig 2) Thus IS In contrast to the tugher mean plasma dexamethasone levels on the second test m patrents that changed from non-suppressor to suppressor (lower nght panel Fig 2) Thus Increase was pnmanlq due to SLYpatients H hose dexamethasone levels rose from a range of 2-4 to 4-10 nmol/l (patrents 20 29 32 35. SO and 68 Fig 1) Conversely there was a fall m plahma dexamethasone on the second DST m tao of the rune patients that were suppressors on Irutlal sampling. and non-suppressors on folkw-up testing (patients 1 and 30 Fig 1) In one female patient from group 2 (patient 30). plasma dexamethasone fell from 10 5 to 1 2 nmol/l on retesting Thus patient had a kstory of I v drug abuse and be-
cause she was ldentlfled a5 an outlrcr she nds excluded from the analqsrs The slgmflcant sbfts m plasma drxamethasone that occurred m some patients could not be explamrd b> age wevght. se\ (open and filled circles In Fig 1) or presence of melanchohc feature> (patients 39-71) hloreobrr treatment per se did not explain the dramatlc shfts m dexamethasone concrntratlons between tests The net change In 4-p m plasma dexamethasone from test 1 to test 2 In the three patients treated Hlth loa-dose benzodlazepmes bias 0 2 nmol,‘l. m the 40 patients takmg antidepressants the Increase was 0 5 nmol/l for the >e\en patients takmg antldeprcssants and hthwm there NJS a net Increase of 1 5 nmol/l and for the SLX patients takmg both antidepressants and neuroleptlcs the net glun uas onlb 0 1 nmol/l The effect of ECT on plasma devamethasone levels was slnular to the group @Len antldepressants wth a net gam In deuamethasone of 0 6 nmol/ I on the second DST Pre-DST plasma cortlsol values on mltlal and folk\\-up testing are Illustrated In Fig 2 for each of the four groups Pre-DST plasma cortlsol concentrations uere lugher in non-suppressors (447 +
97
12
10
0
MALES
0
FEMALES
8
8” 8
6
4
2
(I
suppressors on Fig
1 Afternoon
lo discharge
(4 p m
(DSTZ)
) plasma
male pallenls
ulth
concentrahons
mayor deprewon
17 h folloamg
Numhers
1-38
on
1 mg dexamethasone Into four group,
both
on adnusslon (DSTl) accordmg
of 139 nmol,‘l
are patients ullh
features
DST2
non suppressors
suppressor
corhsol cnwnon
are pauenls ulth prvchotlc
191 nmol/l) compared to the suppressors (314 f 179 nmol/l F = 9 66. P < 0 005) Seventy-four per cent of the non-suppressors had afternoon (4 p m ) pre-DST cortlsol concentrations abobe 300 nmol/l on the uutlal test. whuzh IS above the 9S? confidence mtenals for normal controls There was a fall m pre-DST cortlsol on folio\\-up testing m patients who suppressed on both tests or whose
DSTl
nonsuppressor to
on borh teals using a posr-dexamelhasone
and numbers 72-78
DSTZ
Pauenrs are dlwded
and fllled Lucles Indicate female patlenls
are pattents ulth melanchoha
DSTl
to
nonsuppressor
dexamethasone
In 78 pauents
DSTZ
suppressor
both
(suppressors or non-suppressors) mdlcate
DSTl
DSTP
DSTl
10 their
(5 pg,,dl)
major depressmn
and pnor DST
EMU\
Open circles
number> 39-71
Mean Lalues for each column appear In Fig 2
DST status changed from non-suppresslon to suppresslon (upper left and lower right panels. Fig 2. respectively) Pre-DST cortlsol values were hqgher on retestmg m the patients that snItched from suppressors to non-suppressors (louer left panel) and remalned elevated throughout hospltahsatlon In the patients that were non-suppressors on both tests (upper r&t panel) Three of the SIX patients
9x
Flp
2 Afternoon
connectmg
(3 p m
groups according rerpecu\el\
cornal
Ths MC) bottom
alrchcd
non-suppresston
plabma sorucol (whd
tDSTlt
and pnor
to thelr DST SIJIU~ on adnuwon
right panels rhow pre-DST SMUI
I pre-DST
cIrcIes) on ndrm,smn
from
and pnor
and dexamethaone IO non-bupprewon
IO supprewon
(loner
quarest
to dwhrlrge
(loser
Isft
right panel) lndute
~+lth rdlsed dexamethasone lebels on follow-up from group 3 (patients 32 35. 68) had elevated pre-DST cortlsols throughout hospltahsatlon Stepwse multlple regresston analysis mdlcated that differences m pre-DST cortlsol values from test 1 to test 2 could explain 195 of the lanablhty In post-DST cortlsol values A further 6% of the vanabthty could be evplalned by changes In plasma dexamethasone levels No other variables such as age. sex, or treatment dunng hospt ahsatlon. had a slgmflcant Influence on predlctlng change In postDST cortlsol values Analysts of the residuals mdlcated no sequential effects ober time of study equahty of vanance and a normal dlstnbutlon A multtple regression analysis of all patients uho here non-suppressors on dt least one test (groups 2, 3 and 4) mdtcated that the drfferences rn preDST cortlsol levels \bere kghly correlated Hlth changes In post-DST corttsol lebels (r = 0 52) and could account for 27% of the kanabrhty As before differences m plasma dexamethasone levels mere negatively correlated v+tth change In postDST cortlsol (r = -0 34) and could explam a further 7’F of the vanabIlIty
and dcxameth~ronr
In 7X depreurd
Lortlwl
pAneI)
patents
concenrr~wn~
Patlent:. uerr
ullng rl cor~~~ol cn~enon of 139 nmol
plasma levels 111wppreaors
panels Illustrrlte the change> In pre-DST
suppressmn
t DST pou~l\e)
bnes connecung
IO discharge (DSTZ)
and
I
an both tests and non-uppres,ora
and plJ\nu In pdtwnt,
dr\ameth~wnr uhose
DST
tdotwd
dl\lded lipper
left and
on both W>I~
In parwnrb uhow SUIU>
The number ot patwnrs In rJLh group 13 g\en
Ilnex
Into four
nornulwd
DST from
In Table 1 T-burl
1 SEhf
Dwuwon
Vanablhty In plasma de\amethasone concentrations was exanuned In 78 patient> nlth major depression pnor to and during antidepressant treatment The test-retebt stablhty of plasma dexamethasone concentrations hlttun patients UJS ~lth an overall slgmflcant posItIke satisfactory correlation between plasma dexamethasone Ielels between test> for each patient However mdt\ldual analysis shoaed wide differences In dexamethasone concentrations m some patients at both 8 a m and 4 p m Ths uas ebldent both m patients whose DST status did not change between tests buch as those \rho Here suppressor5 throughout, and In those In \\horn DST status changed on follow-up testmg The extent of change In plasma dexamethasone concentrations was substantial m some patients hlth 4-p m plasma dexamethasone levels varying by a factor of more than 1 7 nmol/l m 22 patients and In ten of these the difference betbeen tests nas greater than 3 4 nniol/l
Preblous reports habe dlffered on the extent of test-retest stablIlt of plasma dexamethasone and Its chrucal slgruflcance Carroll et al (1980) reported only nunor banablhty rn plasma dexamethasone concentrations m four patients studied dunng Illness and after recovery despite change in DST status from non-suppression to suppression Honever. Berger et al (1985) reported substantial vdnatlon rn plasma dexamethasone levels at 9 a m In 12 patients Hlth at least three senal DSTs dunng hosprtahsatlon They concluded that there was a hnuted mtra-mdlbldual stablhty of dexamethasone pharrnacokmetlcs Smularly. Baumgartner et al (1986) reported wide mtra-lndl\ldual vanatlon In dexamethasone concentrations dunng senal testing m 26 patients with major depressl\e disorder A progressive fall m mean post-dexamethasone cortlsol concentrations over 5 weeks however \\as not accompamed by any slgmficant changes In mean dexamethasone concentrations It was concluded that tlus has not a slgmflcant factor m change m DST status Holsboer et al (1986) reported a slgmflcant nse In plasma dexamethasone concentration In 31 depressed patients who showed lrutral non-suppresslon of cortrsol. but Bho became suppressors dunng treatment. whrle 14 patients uho were suppressors on both tests sho\hed no slgruflcant difference In deKamethasone concentratrons In contrast. Carson and Halbrelch (1987) reported no slgmflcant change overall In plasma dexamethasone concentrations m 15 patients with major depression pnor to and durmg treatment mcludlng those whose DST status changed from non-suppresslon to suppresslon However. slgmfrcant banability was noticed In mdlvldual patients. particularly those v. ho remained suppressors throughout. suggesting an effect of treatment or change In chrucal status, on dexamethasone pharmacokmetlcs The mecharusms underlying vanablhty m dexamethasone concentrations are uncertam but may result from changes m absorption. metabohsm or ehmmatron of dexamethasone Holsboer suggested that a ION plasma dexamethasone level In nonsuppressors ts a state-dependent phenomenon resulting from accelerated metabohsm of dexamethasone wluch normabses on chrucal recovery Whle such a general trend was not observed m thrs study tbs mecharusm cannot be excluded m
the SIX patients who showed marked increases in dexamethasone levels associated ulth change in DST status from non-suppression to suppression Test-retest differences did not appear to be dssoelated with treatment allocatlon. either ECT or antidepressants or the presence of other psychotropic drugs The slgmflcance of althm-patient Lananon in plasma dexamethasone levels depends on the extent and direction of the change m plasma levels lrutlal DST status, and concurrent changes in predexamethasone plasma cortlsol A nse m plasma dexamethasone levels m patients who are uutlal suppressors or a fall m patients Hho are uutlal non-suppressors IS hkely to be of less slgmflcance than a nse m plasma dexamethasone m mltlal non-suppressors or a fall m uutlal suppressors that may contnbute to change m DST status Thus IS Illustrated m three of the SIX patients with railsed plasma dexamethasone levels on follow-up whose change In DST status from non-suppressor to suppressor occurred despite elevated pre-DST cortlsols throughout hospltahsatlon Recent studies by Holsboer et al (1986) and Wledemann and Holsboer (1987) report that early blophase lunetlcs of dexamethasone are rndlstmgulshable among DST suppressors and nonsuppressors, raising doubt as to the Importance of actual plasma dexamethasone levels 9-17 h following adnumstratlon In deternunmg DST response Studies to examme the relatlonsbp between early blophase kmetlcs and plasma levels 9-17 h followmg and the relatlonshrp to plasma ACTH-cortlsol response are currently under day In our laboratory Whole change m plasma dexamethasone levels was a slgmflcant deternunant of change m DST status m some patients difference In pre-DST plasma cortlsol levels between tests uas the most Important deternunant of change In post-DST cortlsol lebels Thus IS consistent with other studies showing cortlsol hqpersecretlon to be a slgmflcant detemunant of non-suppresslon of plasma cortlsol followmg dexamethasone adnumstratlon (Asms et al, 1981. Poland et al. 1987) The changmg Interactions between pre-DST plasma cortlsol and plasma dexamethasone dunng treatment appear to largely determme the test-retest differences In DST status
In the majonty of patients chrucal Improvement, as measured by change m Hanulton scores on follow-up. uas accomparued by a fall m preDST
plasma cortlsol
To the extent that elevated
4-p m plasma cortlsol concentrdtlons are d rehdble Index of Increased HPA axis function (Astus et al 1981, Chnstensen et al 1985). their fall durIng treatment with a concurrent change from non-suppresslon to suppresslon m some patients 15 conslstent with reports that normahsatlon of the
Chnstensen L
t 19851 rwn
J
Dlsord
Chn BJ
and
J
hfarkb
R
Kronfol
Z
Pavctiatrv
Holsboer
hl (1960)
tlcal Manual ctuatnc Arana
Assoclatlon
of hlental
Assoclatlon
G W
G hf
Sachar
Ostron 138
Arch
3rd edn
E J
and Stall>-
Amencan
Psb-
M
(1985)
Psq&atn
Halbrelch
U
F S (1981)
42
The
and progNathan
R
Cortlsol secretIon and
response m depressIon
Am
J
Pswzhratn
D
dersmethasone F
A
Haack
D and Vecsel
P (1986) Senal De~a-
Gerken
K
half-bfe Gen
G
Hunt
methasone
M
Parke
K -M , Kneg
The effect of #e&t
dexamethasone
18
levels
J-C
and
Von Zerssen
loss and mappropnate
on
the
DST
P\vchatr
D
plasma Re,
15
351-360 V
Moms
H
and Gdhland
serum dexamethasone BJ
Schroeder,
Femberg
M
methasone rponse
Metab Felnberg
Haskett
R
James
DeVlgne
(1986)
and
of
tn the dexamethasone
Mukhopadhvav
ulth
The effect
Johnson
S
Greden
J (1980)
cortlsol
endogenous
J F
Plasma dexa-
suppressjon
depresston
J
reClan
bup-
m dcprss-
E (1986)
Shortened non-
813-815
A
kanable
and Boll
E 11986)
m deprebw~n
htophase hmetlo Kerr
tcst-re-
Ps\chatrv
K
md
Reb 17
I
Catcrson
test (DST)
G
Hunt
G
\one levels Johnson
G
Kerr
K
supprewon
(1984)
and plasnw Pbbchatr
Proceedings
IV World
Phladelpba Hunt
G
U S 4
Kerr
dekamethasone test
K
plasma
dexa-
Res
13
(1986)
The
dexametha-
Congress on Bmlo@cal
Elsekler
Amsterdam
I
and Caterson
nlndo\s
In
1
and Catcrson test and
11987)
The
and the devamethasone
depresslon
N
Greden MLI
J and Young
J F
, Kronfol
Tanka Z
J
Lobr
Albald N
A
Stemer
E (1981) A speclflL laboraton Arch
Gen
Psvcbatn
SW
213-216
S
Ich&.wa
metabolic
and Halbrelch cortlsol
U
1
Blol
and Homma
propertles
dexamethasone
m
among
Ps\cbatn
Il\er
22
Endocnnol
Metahol
M J (1985)
Poland
R E
(1987)
and dexamethasone
Effect of treatment Btol
Psbcluatn
on 22
accelerated
flulure
J
Chn
60 848-854
SPSS-Y
Rubm
Advanced
R T
Lesser
Neuroendocnne
depressmn
SI~IISIICS Guide
II
Serum
Pshchatn K
sane bnetlo admuustratmn
I
hf
Lane
LA
aspects of pnman
deuamethabone
hvpoth~amcFpltult~,n’-adrcnal
Wledemann
dl>ea>es
In rend
m and
hlc-
Cbcago
P J (1987)
Gen
Dlfferenceb
predntsolone
mind rend
of dexamethasone
Norusls
hl (1985)
cortlsol
metdboh,m
1340-1348
18 15-22 pla>ma
Kaua~
nantr of the dexamethasone
51 433-437 M
test for the &agnosls of melanchoba Carson
(198-I)
19 2X1-291
Gerken
supprewon
dexamethasone
Gras-HIII
21 735-743
and Tanka,
concentrations
EndoLnnol BJ
K
, RIC~K J
In pattents
J
concentrations
suppresslon test BIOI Psychatry
M
P
1015-1039
(1985)
Carroll,
\ecsel
and dlfferenual
levels III depressed pa:lent>
suppressmn
Carroll
and
Psvcluatrv 43
G
Desamethasone
Res
Carr
4
for
97-103
The mfluence 45-64 Bergcr
Neuro-
20 266-271
and Boll
K
test ,tudles and earl\
plasma
Psvchtatr
Arch
m depressed dcvamcthasone
Wledemann
Pan III
banables
The pro-
J Nsurol
Chem
BIOI Ps\cbatn
Arch
methasone SuppressIon Tests In psvch~atnc Illness of mtenemng
Carroll
of melJncholla
concentrations
Wledemann
Pskcbatn
1218-1221
Baumgartner,
L
Supprerslon
305-313
1193- 1204
&an-u
Grunbau\
response of cornsol and CortIcosterone F
Johmon
DC
Test for dlagnow
Gen
L and Halpem
dexamethasone
Dtagnostlc
R J and Omsteen
SuppressIon
noIts m psqcluatry Asms
Dlsorderr
Washmgton
Baldessanru
Dexamethasone
(1980)
D
Dexamethasonr
Chn
The plasma dexamethasone Psvchatnc
J
4 F (1974~ Radw1mmunodb,a\
m plasma
Haack
suppressors
Amencan
9
Eur
4 ratmg for dcprebslon
sI\es and control>
Holsboer
(1975)
treatment
Plasma dexamethasone
Holsbocr
4
and test-retebt reproduclblht\
and Hogans
pre,slon
V and Parhe
23 56-62
dexamethasone F
H ‘I
III deprcs-
40 493-500
.rurg Psbchatn
cal recovery m patients Nlth depresslon should. however, take mto account the effect of \anahlhty
cortlsol
for dexamethasone
hng (1983)
Tebts m antIdepressant
hl
Chn>tenwn
9 239-244
Gardner
cew of normallratlon Gen
P
and Thomsen
plasma
procedure
Pharmacol J F
0 L
8 271-278
Chahrabortb
Greden
Kragh-Sorenwn
Pedersen afternoon
radlolmmunoassa\
Hlchem
References
L F
C B
J 4ffec1
Enghsh
Studies exanunmg the chmcal utlhty of the dexamethasone suppresslon test to motutor chru-
m plasma dexamethasone concentrations To do ths requires simultaneous measurement of plasma dexamethasone and plasma cortlsol
Gram
Spontansous
Harmlton
DST comcldes with chrucal Improvement
P
Knrtensen
and Hart endogenous
concentratmns
cortical suppres\ton
rlctnlt\
dnd
as deternu-
test response
4rLh
44. 790-796
and Holxhoer dunng of
F
the DST the
te\t
(1987) after drug
Plasma dewmethdoral and Intra\enou\ BIOI
Ps\cbJtn
72