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Serial dexamethasone suppression tests in depressed patients treated only with electroconvulsive therapy
Journal of Affective Elsevier
Disorders,
13 (1987) 233-240
233
JAD 00494
Serial dexamethasone suppression tests in depressed treated only with electroconvulsive therapy Leon Grunhaus, Clmcal
Thomas Zelnik, A. Ariav Albala, David Rabin, Athanasios P. Zis and John F. Greden
Studies Unit, Department
of Pqxhintv,
patients
Roger F. Haskett,
ffmuerslt? of Michigan Mediccrl Center. Ann Arbor, MI 48109, U.S.A. (Received (Accepted
1 April 1987) 10 June 1987)
Summary
Several systematic studies have evaluated serial dexamethasone suppression tests (DST) in patients with major depression who were treated with antidepressant medications. DST changes were noted to parallel clinical improvement in most recovering patients. If serial DSTs are a valid state-related correlate of depressive pathophysiology, all types of effective antidepressant treatment should result in DST ‘normalization’. However, no treatment modalities other than antidepressant medications have been studied serially with systematic assessments. To test whether serial DSTs reflect clinical progress in depressives treated solely with electroconvulsive therapy (ECT), we studied weekly DSTs and Hamilton Rating Scales for Depression (HRSD) in 22 drug-free depressed patients. We observed progressive DST ‘normalization’ in most patients and moderately high correlations between weekly DST and HRSD values throughout treatment. Most patients receiving ECT became DST suppressors. In most patients the DST appeared to reflect the severity of depressive pathophysiology, perhaps providing serial feedback to clinicians monitoring the progress of treatment with ECT.
Key fiords:
Dexamethasone
suppression
test; Major depression;
Introduction
A number of investigators have reported on the patterns of dexamethasone suppression test (DST) Address for correspondence: Leon Grunhaus, M.D., Assistant Professor of Psychiatry, Department of Psychiatry, University of Michigan Medical Center, Ann Arbor, MI 481090118, U.S.A. Supported in part by NIMH Grants MH28294 and MH39593, and by the University of Michigan Mental Health Research Institute and Department of Psychiatry.
0165.0327/87/$03.50
0 1987 Elsevier Science Publishers
Electroconvulsive
therapy
results in depressed patients during treatment with antidepressant medications (Carroll 1972; De La Fuente and Rosenbaum 1980; Greden et al. 1980, 1983; Holsboer et al. 1982, 1983; Targum 1983; Gerken et al. 1985; Bowie and Beaini 1985; Baumgartner et al. 1986; Grunhaus et al. 1987). From these studies it appears that the normalization of a previously nonsuppressive DST parallels a successful course of antidepressant treatment. Initial reports suggested that similar patterns of normalization occurred during electroconvulsive
B.V. (Biomedical
Division)
ther+
(ECT)
(D>Aen
1979
1979
1981)
Hweler
more
recent
demon>trrlted
dn
a>cwatmn
not
4lbA.1
et aI
Carroll
normahzdtmn 19%.
aid
Debanand
To
et al
further
1981
outcome
et al
Greden
ECT
the eftects
rewlt,
\\\r \tudwd
22 wrrelv
deprewd
N Ith
onI\
ueehl\
mctdlatrl> follw
cbnlcal dfter
prr\>l\r
DST\
ECT
(2)
,tJte-relatlonshp Are
absolute
TABLE
Do
If
so
b’e
cner do
tlmr
>ensl
cllnlcal
of pa&nts
treated
plana
In monitoring mlth
lJnl\erslt\
of
the
ECT hale
~mpro~rment”
po\t-dexamethasone meaningful
A DSTb
tCSL[)
and
patients
Studw~
or
the
1984
Selected patent
patlent
recel\rd
Pschatq
bledlcal
Center
AND
CLINICAL
Each dw+xtlc
13
prnod
a
cl~mcal
ot e\aluatmn lnten~as
cortlal
dmgno>tlc
cllnic~l
the Schedule phrrrua
OF
INDIi
our
In TabIs
standard
dt IeJ\t
stdff psjchatnst)
Intrnwc
b\
for
tSpltzsr
da
IDCIAL
a tramrd
4tfectl\e and
Intenw\er
Dlsorda
Endlcott
one
NR
4 b
2 5
R
NR NR
20
1
R
NR
1
R
NR
2
and
1975).
(4)
(1
NR
(1
NR
1
L
1
-I
2
6 U> 3 2
NR
Phl Phl Phi T4H
R
Phi Phi
1
Phi NR
R
4 TAH
>
Phi
II ?
R
NR
r’ 10
R
NR
4
R
Phi
5
R
Phi
tt 4 NR
-’ 1fJ
NR
>
T4H R
Phi Phi
R
ealua-
(3) a a-uctured
PATIENTS
NR
research drug-free
(2) [HO or three unstructured (Including
13
12
the
and clinical
(1) ct lo-13
r\aluatmn
tmn h\ a w-uor
(3)
ECT’
FEATLIRES
of
hetL\een
are wmmanzed
I
DEhlOGRAPHIC
Attcctl\e
Ps>chobmlog>
of
dcmographc
for rJch
hobpltal-
tar
Chrucal
Department
Mlch+yn
\\err:
Llrut
1
lm-
nonsup-
depressed Clm~csl
In the
features
and
addressed
pretreatment
the
Program 1979
pnt~entb and
In
Dlsordrr~
on DST
DSTb
dunng
treatment (1)
\\lth
cliruc,~ll~
progrre
betore
normahze
,idnunl>tered”
\alueb
nlth
ratlngb
Ing questions
lzed
DST
tCor\ell
ot ECT
treated
concurrent
Twsnt>-two
ha\e
het\Jeen
1987)
t~anune ECT
t31 al
pubhcatmn\ from
Methods
and
Papakostd,
Phi
usmg Sch~zoph\wxl
exdmlnatlon
and
xreemng fanuly dnd
lntenwts
(6)
collection \\ere
Crlterta 1980)
medical
of Informatmn
using
cornplIed
(RDC)
(Spltzer
Dlqgnostlcran~
lllne>ses
longltudm~l
ot pre\ mus
Research
hston
\ierr:
Carroll blind
Incluslon DSTh
cntetw treated
pnor
techmcnl
bource\
medlcal
Ic)s~ (greater
here dunng
Illnrs~
than
205
or drug
no
Hlth
AND
choactl\e (other In
to DST
research
tre:atment
that Hould
et al
1981).
no hstoq helo~
FOR
hod\
INDIi
drugs
IDL’AL
HRSD
no
12
rllnzbs
and
mere
rncludlng
P-\TIENTS
HRSD
Patent Sr\ent>-one
female
ST-\ND-\RDIZED
T\ro third. DST
drpre>rsl\e Of
ani
psi-
course
of
ECT
to pxtlclpatz
met
these
cntena
The
SERIAL
(Table
1) met
disorder
(hlDD)
thsse
Four
d dlagnosls
deprewd
ibetght)
Hho
ot 21 pattents
18 and 22) iterr
9 recel\cd
rrwltb
nlth
In the sample
s\mptoms
17
to DST
consent
patlent>
&xvpr
luwnnl
no
the
~~eeehlb
Deprrwon
tar the ddnum,tratlon
Informed
for major
dogenous
v,rlpht
no pregnarq
Included
cnterld
Iniahdate
lncludlng
Ons-IhId DST L1
(3)
of seers
normal
abuse
Prr- ECT *
ECT
All
Tmentv-one
(2) ueehl\
(6)
blind
dunng
(4)
for
no treatment
those necsssan
and
1982)
Scale
b> raters (5)
mrdlcntmn
than
et cil
Rating
1960)
of ECT).
deprxwl\e
ECT
lmalldatlng
HRSD \ ALLIES
HRSD
score
ulth
of \anance (Cxroll
no alcohohsm trtxtment
(1)
exclu~~rlv
to and
of the DSTs
serious
C.1.r:
completed
\cere
s\mptoms
DST
(HRSD)
dlag-
reults
an\
Hanulton
(Harmlton
et aI
(Pri\ltera
17-item
Fol-
Dagno\tlc
1975
al\\a>h
(5)
records
conemus
et al
carbJmazepine
laboratory
mrdcal
to knItdate
rc\ Iens
lo\\lng noses
comprehen~l\r
to rule out sertous
17
(815)
umpolar
6 had
mean
TlhlE
age
the
( f SD)
of bipolar total
barnpIe
for the rntlrc
POINTS
Post ECT DST
HR3D
DST
WdI\d
1 !I I
No
tdlsordrr)
,I Astor! of
dr-
(No.\
Patent
of sctuzoaffcctl\e percent
sn-
had
patlent.
nondeltwonal
No
RDC
w.pnn,< R R NR R R R R P.ml_ll R NR Dl.~\~IlllllUd R R R R \\ ithdreu NR P.ifll&il R R R P.lrlldl
outcome
\arlable\
points tr~;ltmrnr
the
dctrrnuned
upon
course
group
prior
(2) upon completion
clInIcall\ (3)
tar
tl I rmmrdlatelv ECT
Lompletmn
four
11mr
flrbt
ECT
ot one-llurd
cow,2
ot
Jnd (41 \slthln
at
LO the
tHo-thirds
l-3
of the
for each pa~rsn~
dd\>
ot
the
tollwIng
ECT
thr: 1~151
EC T trtxtmrnt
ElectrIcal
Impul>rb
In>trument but
\\\rt:
one
L~YZ (patient
tredfment4)
s‘1e3
kzure
\\lth
the
~lmultaneou~
to
succln!
(average
dohe = 1
No
the
The
17-11em
DSTh
and
brl\\een
lI1lWl 1rt11iullILl~t?lt'
1 IlI,Jllll
HRSD
both
ECT
\\ere
w~nc~dsd ‘~l\\a>h
\rlth
dntldrpresbant 10 da>> pnor
treatment The
on da\>
Indicated
b>
patlent
docrlnr
CW~CO~S~ \\ertl
u,~l patient\ The wxdl
Jnd
total
ternunsd
JXOZIJI~~ d,lta
r\aluated
tar the group
number
LLIIuc~II~
aseh>mrnt\
clinical
of To
ECT
tor both
No
11 and
Senal
DST
ECT,
treat-
trqurnc\ No
fl\s
15
au>
tar
11 tredl-
ECT
due
16 \\lthdre\t
Fmal
In
Inds-
outcome
to
con\arld-
16 are excluded
from
data
data
In an earlier
The
patient
311 ECT
of aggregate
dppexed
For
not
15 listed
honzontal
after
all analyses
\\ertl
adrrunlstered
the
dt
treatment4
patwnt
results on
Nos
for
dunng
electrocon~ul~r~r
Patlent
rscelvlng
sedatrle-
pomt
condltlonb
Mere
2
or
tram
report
one patlent
( 4lbala
(No
et al
2)
1981)
IndI\~d-
a> LoI\ hole tredtmrnts
btandardlze
ate nnalbzed
111th IWIJ~CI~ and wurnsn-
31s
to treatment)
bornatlc
dwxntlnued
blzs for paitlents problem\
paral\
gl!copvrrolatc
or at an\
each
DST
arro\\>
confuwm
>ent after
ot group
of to
In Fig
lrert:
mental
mlmITuzs
dose = C, 75
admuubtered
Thu,
treatnlents
from
msnt>
To
and
conconutant
number
ECT
pendent
~nt~rprelation
short-acting
mubcle
hg)
to ECT
ddnurustrred 2
each
for
\\ere
course: b\
total
ments Table
treatments
a
or
anesthetIc
(alerage
antlpsbchotlc
medlcatlonb
cnntounded \rerl,l\
prtrlormsd
of
and
wxetmns
hipnotlc
tllrrllys
111 all
rscorded
doss = 0 3 mg 45 nun prior
to reduce
c Irtllllll
use
lchohns
111 alI unilateral
Standard
krp
mg/
hledcralr
tournrqurt
rscordlngs
mg ‘kg) (aLwage
\\A
J Irmb
Induce
a
8 rrce:l\cd
actl\ll\
Included
prztrralment
b>
bltrmporall>
No
~13s of
El33
barblturatc
Isa>t
generaled
admlmslrrrd
the
HRSD
M~S drtlrmng and
of
DST
-Ill
DST
normAt> before
\Aues
\\t3re log-transformed
ot dlbtnbutmn btatr>tlcal
analtses
and ctquaht> \\ere
10 obwn ot variance>
pertormed
To
de-
termlnr the slgnlflcance of decreases 111DST Calue\ end HRSD scores o\er ttmr dunng ECT treatmen t one-\\ a> ANOVA \\ Ith re:peJted meahurrz \b,l~\ used palred r-tests aere used tar paramrtnc compxlrons bet\iren pre- and posttreatment DST and HRSD rebulth. rehpcctl\elv For dtchotomous \arl&le> HT used either the chl-bquxed tebt or Fl3her.s exact prob&tlltk tebt Pcx>on’> product-moment correlatlon~ Here used to J~VZM the relatron\hlp betireen DST values and HRSD score> tar each Indlvldual patlent dunng the course of ECT treatment Rewlts
STANDARDIZED
hlean post-deuamethasone plasma cortlsol \alues and HRSD scores at the four standardized serial time points dunng ECT treatment are sho\sn In Fig 1 These aggregate data mdlcate that progressive normahzatlon of the DST occurred dunng resolutlon of the depressl\e syndrome mlth treatment One-wav ANOL’A alth repeated measures conflrmed qnlflcant reductions m these score5 oker time (P < 0 001) PaIrwise compansons between pre- and post-ECT treatment Lalues confIrmed tughI> slgruflcant reductions (P < 0 001) In both DST and HRSD bcores
POINTS
pressed \s euthynuc) there wa5 a stead! decrease In the percentage of both nonsupprebsors and depressed patients dunng treatment Thus categoncal analyses hupported trend.4 from mean data
Ttwteen patients (Nos 1 2 4 5 6. 7. 9 12 13 14. 15. 20 21) had pohttredtment DST supprewon DSTs and good response Three pattents (NOS 3.8.10) had posttreatment DST huppresslon but only partral or nonresponse Three patrents had posttreatment DST nonsuppresslon. of these
Table 3 re\eals that \\hen data \\ere annl>zrd categoncxll!, (wppressors \s nonwppressors deTABLE
ASSESSMENT
3
NLlhfBERS
-ZND
DARDIZED
SERIAL
PERCENTAGES TIhlE
OF
PATIENTS
WHO
4RE
DST
NONSLtPPRESSORS
lmmedm1e
One-thud
ECT
T\ro-rlurd>
pre-ECT DST non,uppreas,\e
l
AND
DEPRESSED
ECT
Immedk~le posl-ECT
,> /I’B dl,
n
lO,f 22
l-l,?1
s
9
90 9
bb 7
38 1
13 8
22,::. loo
lb 21 76 2
13 71 61 9
6, 20
Deprrwd
**
(HRSD
* C~I-quxr
= 26 74
21
3 19
> 101
II 4
“Ch-quare=2457
d/ =
d/=3
AT
POINTS
3
P < 0 001 P
30
STAN-
0
20406080130
0
20406OLam
40
so
80
I no
TREATMENT COURSE
(Days)
239 tuo
(Nos
call\
17
~hlle
patwnts cme
22) had pxt~al
one (No
\\ert:
not
their
(Nob
11
a
ml\,lng
data
patlent
(81%)
31on had three
III
treatments
ekplalned
(No
a good
or the\
In amman
I?
outcome and
DST
compared
\\ho
had
good
outcome
among
rrjpondm
13 of 14 (934)
DST
\\ere
ot
DST \ e:\xt
good
These
16
one
(FIbher
J Stated dIfferentI>
DST
ECT
wpprch>ors
apt
data
Induce>
and
that
anal\sls
tlons
o\er \\e
anuned
(1984)
of mean time
values
may
ulthm-subject blhty.
Daw
lead
senal
values
and
rather
strong
values
and
each
of repeated To
parable
post-deuamethasone matching
HRSD
temporal HRSD
wares
assoclatlon
scores
and
plasma
uas
ex-
cortlbol
(Fig
2)
between
elident
A
DST
m
man!
patients Indlrldual HRSD
plots
betueen-subject tlon
meekI\
\anation
between
DST
terns
that
ot DST
ment
wluch
m
patwnts
m Fig
Suggestlbe methasone
had
paralleled
of
absocld-
2)
Inspect-
Indl\Idual
cl~rucal
pat-
Improve-
the aggregate
pat-
1
ot
1980
bald
1981
et
al
plasma
rhythms
cortlsol
Nos
tient>
10. 17
of
\\ere
post-dexa-
noted
htudled
subjects
in ths
\\eekl!
ot
Our
m
4ome
study
uh~h
they Influenced
et al
1982.
Carroll group 61 5
1984)
The
hg
63 8
one-tlurd.
serial
DST
et al mean
from kg
each
to deterrmne
Edelstem
changed
for
and
fmdmgs
1983
for
kg
the
and
and
sect
respectl\ely
m
Ilmlted
number
farlure
ot
ment>
most
ma\
Jgalnbt
re-
Thlb I e
the
pro-
that
ob-
onI>
to normalize
d
when
poHer
of
about
Jnd poor outcome
greatly
lIkeI>
to
and
de\amethasone
during
while
mean
DST
values
depression
to normahze
(Figs
1 2)
Thus
aggre-
depressr\e
of
obwn
It I> uell eplbode
ac’robs patients
more
buppressorb
DST
but
\\e
good
ot
chnlcJ
lng
that
doe> not folio\\ It ma>
the out-
dunng Improve-
ot the dlscrepancles be clanfled
follou
known
cllmcal
of
cdutlon
nonsuppre>hlon
might
atlon
report5
Normallzatlon
Some
studies
pilot
conflrmatlon
predict
treatment
bet\keen
In
treat-
are
patlent>
DST
ment
~lnu~s
ECT or
ECT
ECT
brologlcal
in mo5t
AUI
of
to
to
1982)
strengthen
r preclude
at
rebpond
number
data
rndrpen-
aId Identrtlca-
Albald
responders
pro\ Ide
from
that uould
not
does
tern
patients to
perwstent
and
ECT
treatments
d lack of assoclatlon
mo>t
~m~llar
not
periods
HRSD
moderateI\
conslderatlonb
O\er-lnterpretatlon
e\en
\\eekl>
btudleh
does
ECT
conflrmed
DST that
progress
tound
antlde-
are
llrrutlng
optImaI
to become
mltlal
generalI>
the
come
after
that
benefit
Hahkett
These
treatment
normal-
ot
buppreshorh
ot the DST
1982
\\eelght
gate data
fall
that
DST
patlents
change5
DST
and DST
markers’
buggest
clinical
that
to be tenuoub
obJectl\e
tlon
pa-
a cnnlounded
Lalues
Thub
C I~n~ctans could dent
DST
treatment
to normahze
conttnue
of
ot depreh-
tlms
Illustrate
analws
1983
proportlon
ot h,ubJects tall
eftectlle
statrst~cal
\I-
1981
admlnlhtratron
senal
and
1983
marher
d problem
most
Fuente
al
hImpI\
o\er
also
encountered
mean begun
to
tram
become
bened gILen
I> not
correlated
ECT
La
\ilth
hupportb
1980
et
com-
treated
It also \uggchth
DST
matching
to htrongli ce~\lng
(De et al
In a large
medlcdtlon~
Thus had
the
to
entlre
treatment
post-ECT
contmued
to
(Berger
Felnberg
weight
65 1 and
the
the extent
62 6 kg before
t\\o-thrds
of
report>
that
ther-
tmdlng
15 a state-related
FIndIngs
\core>
This
Holsboer
\temmlng
prebsant
that
\\elghts
during
normallz~tlon
In patlent>
Grrdcn
pathophk,lolog>
Ilhel>
We
1983)
determlmng
21)
pnor
the DST
I Hashett
oscdlatmg
(eg.
(Fig
and
and
slgruflcant
patterns
normallratlon roughI>
shoHn
patients
most
values
relealed
these two ianables
1011 re\eals
tern
of
scores for each patlent
change
that electrocon\ul~l\e of DST
medrcatlon
Robenbaum
result
thus possl-
separate11
\\rlght
to tho>e obsened
lzatlon
loss of
lndlcate
a collectIon
~\t:
obsena-
address
patlent
ttteo-
emphasized
to d slgrufrcant
InformatIon
plotted
have
Jnd
patterns
antldepresbant
Targum
/t~ciuvhul purlertu of set-t& DST uttd HRSD swettretm durrt~g ECT rrearntettt Glbbonb
value,
treatment
DiscussIon
ot
po\ttredtment
= 0 15 N S
ECT
hJd
buppres-
\rlth
betiteen
bc-
dwxmtlnurd
po>ttreatment
(335)
nonapprraron
thlh anal>~~
\\ert:
pre\~ousl>)
18)
\\lth
patlent
cllnlThree
corwdrrrd
ECT
16
or nonre~pone
19) had good outcome
i\ell
b\. longer
reco\en
renu,slon a uniform be that
from from
a
pat-
J slnular
240 process occurs with the DST. Further refinements of research strategies are needed to address unanswered questions. For example, this study should be repeated with concomitant plasma dexamethasone levels to control for the possibility that repeated administration of barbiturates for ECT might change dexamethasone metabolism. If so. however, we would have expected to find progressively more nonsuppression, exactly opposite to what we observed. Finally, serial DSTs in untreated patients, i.e., those involved in placebocontrolled studies, may provide information on ‘naturalistic’ the course of hypothalamicpituitary-adrenal axis dysfunction in depression.
enous
deprewon
loss.
and
Gerken,
A., Maler.
DST
docrinology. Gibbon\, aalarieb
depressives chiatry.
16 (1981)
of
Gredcn.
Biol.
Psy-
Kurten,
I., Serial
dexametha-
in psychiatric
illness,
Psychiat.
(1979)
R. et al., Neuroendocrinological
neurophysiological are
there
Biol.
P.C.S.
in
major
markers
Psychiatry,
and
xamethasone
studies
biological
17 (1982)
Beaini,
A.Y.,
suppression
test,
the
dis-
endogenoua
Greden.
1217-1242.
J.F.,
of
Br. J. Psychiatry,
the
de-
147 (1985)
of recovery
The
pression.
In:
(Eds.),
Davies,
M..
depression,
B.J.,
M.,
38 (1981)
W., Are serial
J.F.
R.M.
Mowbray
Studies.
I5 (1980)
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2 (1980) et
al..
of melancholia,
of
therapy?,
suppression
J. Affect.
La
Fuente,
dysfunction
J.R.
and
and
blood
Am. J. Psychiatry, Debanand,
D.P.,
Novacenko,
Rosenbaum, levels
137 (1980)
Decina,
H. and
P.,
Mali&
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and non-suppressors
therapy,
Biol.
Dysken,
M.W.,
Pandey,
Am. J. Psychiatry, Edelstein.
C.K.,
Effects test. Feinberg,
Paper
H.A.,
Hopkins.
N..
S., Serial
DST’s
in initial
sup-
with electroconvulsive
Chang,
136 (1979)
1328-1329.
loss
Carroll,
P.. Fawzy, on
the
F.I.
undergoing
1987. scale
R.F.
and
Dornfeld,
L.,
suppression
B.J.. Biological
‘markers’
for endog-
and
~nde\
Psvchlatt-v.
Dexamethaaonc of melnncho
test-retert
A.. Kotun,
reprodw-
J. ,lIaskett. predicts
H.1,
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!n
for Biological
P\vch-
J. Neural.
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affecting
therapy. and
outcome
after
Psychopharmacol.
Affect.
~ccessful Bull..
Liebl,
R.
elcc-
1X
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A. and of climcal 1X (1983)
Some
27 (1967)
in
ECT,
Psychiatry
chiatric Tnrgum. Biol.
relapse:
the
Institute. The
Psychiatry.
rcptrrt of steroid\
micro-
steroid\
in body fluid\
and
J. (‘Ii”.
ultr:ih!
tndocr~nol
in the
Robins,
Ihwrden
Diwsion.
New
Nr\*
1975
I!., Research
Dlagnoatlc
Disorder\. York
State
3rd P\\
1977. of serial
management
IX (1983)
York.
of Function
Division,
York,
.II
611.-620.
New
Group
application
with
Intelsupprr-
cl
for Affective Research
Institute.
New
R.W.
17 (1982)
Research
mc+
outcome
the dexamethaaonr
J., Schedule
J. and
and
55-64
Biometrics
Endicott,
Biometrics
tcbt repcmw
routine
Gardner,
with
Psychiatry, Endicott,
for a Selected
studies
of re\t’r
case\
a prelimmarv
course
4 (1981) J.F.,
Psychiatric
S.D.,
Four
of the protein-bmdlng
patients:
Schizophrenia. R.L.,
1
973-990.
Rrs..
Biol.
State
ds-
illnea.
M.. Lee, J. et al., Nrurocndocrlne
Greden.
R.L. and
W..
radioassay.
by carbamazepine
hion test,
Repeated
911.
to
psychiatric
M.R..
Psycho-
depre.\sive
suppresslo”
of various
Y., Fink,
Criteria
Maier.
protein-binding
wres
Spltzer,
studies
application
Metabol.,
t:.,
during
dexamethasone
indicator
Papakostas,
Spltzer.
Hofschuster, tests
Psychiatry, B.E.P.,
research.
4 (19X2) 93-101.
F., Steiger,
their
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57-62.
and
suppression
Disord..
an
Relevance therapy
IX (1982)
to abnormal
Biol.
A.A.,
electroconvulsive
Bull..
F..
sion
Albala.
in
llolsboer.
lenge
338-341.
136
40 (19X3) 493 -500.
23 (1960)
Factors
pharmacol.
cd”.,
dexamethasone
140 (1983)
postECT.
(lYX4)
75- 78.
York
S.S. et al., Serial
Biol al.,
at the Society
May,
R.F..
and
463-472.
Ihi.
suppres\wn
treatment
nonsuppression
M., A ratmg Psychiatry.
Prlvitera.
Sackeim,
DST
presented
Meeting,
ference
in a patient
Am. J. Psychiatry, M. and
antidepressanta.
levels
Roy-Byrne,
of weight
of tricyclic 1260-1261.
22 (1987)
G.N.,
cortisol
Neuroendocrine
treated
Psychiatry,
dexamethasone
A.H.,
D. et
King.
P.. Pande,
J.F.,
micro-measurement
59-66.
41
a laborator\
R..
L.. Flegel.
Arch.
useful
,md
Iongitudlnal
et al., NormdllLatlon
test:
in antidepressant Psychiatry.
burg.
R.F.
depression,
Gen.
and
10 (1986)
of
Am. J. Pwchiatrv.
endogenous
Arch.
Murphy,
tests
Disord..
Haskett,
of normalization
competitive
dexamethasone
in electroconvulsive De
tests
177-194.
15-22.
oC beer
Psychiatry.
suppression
Gardner.
A specific Gen.
price display
Gen.
the process
tiolsboer,
C.C.
01
449-458.
J.F.,
MDD.
a\
et al.,
Disord.,
Greden,
test for the diagnosis
Psychiatry,
and
Research
Greden, J. Affect.
Feinberg,
laboratory
Some
in de-
IL, 1972, pp. 23-201.
Feinberg,
endogenous Carroll,
axis
B.J. Carroll
Illness:
Springfield,
B.J.,
Coryell,
B.M.
Depressive
Thomas, Carroll,
hypothalamic-pituitary-adrenal
momtorlng P\ychoneuroew
B.J.. The dexamethasone
A.A.,
from
xamethasone B.J..
The and
aid in catatonia.
Albala,
strategies
Normalization
J.M..
Arch.
~)f the dexamethasone
Haskett,
30-35. Carroll,
data.
troconvulsive
depressive
for
tlYX4)
1199.
Hnskett, P., Lund.
uc:lghl
41
F.. Weekly
in depression.
analyw
J.F. and Carroll.
Hamilton,
Res..
Davis.
priests:
and Greden,
25-43.
subtype?, Bowie,
treatment,
Holsboer,
response
test as a diagnostic
(;runhaua.
unipolar
of illnew
Psychiatry.
1183-1184.
atry
K.J. and
tests
M., Doerr,
and
B.J., Changes
among
551-560.
suppression
orders:
tests
electroconvulsive
A., Graff,
18 (1986) Berger,
J. and Carroll,
suppression
receiving
Baumgartner, sane
J.F.. Tarika,
dexamethasone
W. and
and
psychiatric
ha:
A.A., Greden,
Gen.
10 (19X5) 261-271.
R.D.
suppression
in serial
of age, severity
Arch.
suppression
bility. Albala,
effect
1080-1085.
Grcden,
References
~
polarity.
3 19.
neuroendocrlnc~ of
depre\\l\c
Caldi\(~rdci
Disorders,
13 (1987) 233-240
233
JAD 00494
Serial dexamethasone suppression tests in depressed treated only with electroconvulsive therapy Leon Grunhaus, Clmcal
Thomas Zelnik, A. Ariav Albala, David Rabin, Athanasios P. Zis and John F. Greden
Studies Unit, Department
of Pqxhintv,
patients
Roger F. Haskett,
ffmuerslt? of Michigan Mediccrl Center. Ann Arbor, MI 48109, U.S.A. (Received (Accepted
1 April 1987) 10 June 1987)
Summary
Several systematic studies have evaluated serial dexamethasone suppression tests (DST) in patients with major depression who were treated with antidepressant medications. DST changes were noted to parallel clinical improvement in most recovering patients. If serial DSTs are a valid state-related correlate of depressive pathophysiology, all types of effective antidepressant treatment should result in DST ‘normalization’. However, no treatment modalities other than antidepressant medications have been studied serially with systematic assessments. To test whether serial DSTs reflect clinical progress in depressives treated solely with electroconvulsive therapy (ECT), we studied weekly DSTs and Hamilton Rating Scales for Depression (HRSD) in 22 drug-free depressed patients. We observed progressive DST ‘normalization’ in most patients and moderately high correlations between weekly DST and HRSD values throughout treatment. Most patients receiving ECT became DST suppressors. In most patients the DST appeared to reflect the severity of depressive pathophysiology, perhaps providing serial feedback to clinicians monitoring the progress of treatment with ECT.
Key fiords:
Dexamethasone
suppression
test; Major depression;
Introduction
A number of investigators have reported on the patterns of dexamethasone suppression test (DST) Address for correspondence: Leon Grunhaus, M.D., Assistant Professor of Psychiatry, Department of Psychiatry, University of Michigan Medical Center, Ann Arbor, MI 481090118, U.S.A. Supported in part by NIMH Grants MH28294 and MH39593, and by the University of Michigan Mental Health Research Institute and Department of Psychiatry.
0165.0327/87/$03.50
0 1987 Elsevier Science Publishers
Electroconvulsive
therapy
results in depressed patients during treatment with antidepressant medications (Carroll 1972; De La Fuente and Rosenbaum 1980; Greden et al. 1980, 1983; Holsboer et al. 1982, 1983; Targum 1983; Gerken et al. 1985; Bowie and Beaini 1985; Baumgartner et al. 1986; Grunhaus et al. 1987). From these studies it appears that the normalization of a previously nonsuppressive DST parallels a successful course of antidepressant treatment. Initial reports suggested that similar patterns of normalization occurred during electroconvulsive
B.V. (Biomedical
Division)
ther+
(ECT)
(D>Aen
1979
1979
1981)
Hweler
more
recent
demon>trrlted
dn
a>cwatmn
not
4lbA.1
et aI
Carroll
normahzdtmn 19%.
aid
Debanand
To
et al
further
1981
outcome
et al
Greden
ECT
the eftects
rewlt,
\\\r \tudwd
22 wrrelv
deprewd
N Ith
onI\
ueehl\
mctdlatrl> follw
cbnlcal dfter
prr\>l\r
DST\
ECT
(2)
,tJte-relatlonshp Are
absolute
TABLE
Do
If
so
b’e
cner do
tlmr
>ensl
cllnlcal
of pa&nts
treated
plana
In monitoring mlth
lJnl\erslt\
of
the
ECT hale
~mpro~rment”
po\t-dexamethasone meaningful
A DSTb
tCSL[)
and
patients
Studw~
or
the
1984
Selected patent
patlent
recel\rd
Pschatq
bledlcal
Center
AND
CLINICAL
Each dw+xtlc
13
prnod
a
cl~mcal
ot e\aluatmn lnten~as
cortlal
dmgno>tlc
cllnic~l
the Schedule phrrrua
OF
INDIi
our
In TabIs
standard
dt IeJ\t
stdff psjchatnst)
Intrnwc
b\
for
tSpltzsr
da
IDCIAL
a tramrd
4tfectl\e and
Intenw\er
Dlsorda
Endlcott
one
NR
4 b
2 5
R
NR NR
20
1
R
NR
1
R
NR
2
and
1975).
(4)
(1
NR
(1
NR
1
L
1
-I
2
6 U> 3 2
NR
Phl Phl Phi T4H
R
Phi Phi
1
Phi NR
R
4 TAH
>
Phi
II ?
R
NR
r’ 10
R
NR
4
R
Phi
5
R
Phi
tt 4 NR
-’ 1fJ
NR
>
T4H R
Phi Phi
R
ealua-
(3) a a-uctured
PATIENTS
NR
research drug-free
(2) [HO or three unstructured (Including
13
12
the
and clinical
(1) ct lo-13
r\aluatmn
tmn h\ a w-uor
(3)
ECT’
FEATLIRES
of
hetL\een
are wmmanzed
I
DEhlOGRAPHIC
Attcctl\e
Ps>chobmlog>
of
dcmographc
for rJch
hobpltal-
tar
Chrucal
Department
Mlch+yn
\\err:
Llrut
1
lm-
nonsup-
depressed Clm~csl
In the
features
and
addressed
pretreatment
the
Program 1979
pnt~entb and
In
Dlsordrr~
on DST
DSTb
dunng
treatment (1)
\\lth
cliruc,~ll~
progrre
betore
normahze
,idnunl>tered”
\alueb
nlth
ratlngb
Ing questions
lzed
DST
tCor\ell
ot ECT
treated
concurrent
Twsnt>-two
ha\e
het\Jeen
1987)
t~anune ECT
t31 al
pubhcatmn\ from
Methods
and
Papakostd,
Phi
usmg Sch~zoph\wxl
exdmlnatlon
and
xreemng fanuly dnd
lntenwts
(6)
collection \\ere
Crlterta 1980)
medical
of Informatmn
using
cornplIed
(RDC)
(Spltzer
Dlqgnostlcran~
lllne>ses
longltudm~l
ot pre\ mus
Research
hston
\ierr:
Carroll blind
Incluslon DSTh
cntetw treated
pnor
techmcnl
bource\
medlcal
Ic)s~ (greater
here dunng
Illnrs~
than
205
or drug
no
Hlth
AND
choactl\e (other In
to DST
research
tre:atment
that Hould
et al
1981).
no hstoq helo~
FOR
hod\
INDIi
drugs
IDL’AL
HRSD
no
12
rllnzbs
and
mere
rncludlng
P-\TIENTS
HRSD
Patent Sr\ent>-one
female
ST-\ND-\RDIZED
T\ro third. DST
drpre>rsl\e Of
ani
psi-
course
of
ECT
to pxtlclpatz
met
these
cntena
The
SERIAL
(Table
1) met
disorder
(hlDD)
thsse
Four
d dlagnosls
deprewd
ibetght)
Hho
ot 21 pattents
18 and 22) iterr
9 recel\cd
rrwltb
nlth
In the sample
s\mptoms
17
to DST
consent
patlent>
&xvpr
luwnnl
no
the
~~eeehlb
Deprrwon
tar the ddnum,tratlon
Informed
for major
dogenous
v,rlpht
no pregnarq
Included
cnterld
Iniahdate
lncludlng
Ons-IhId DST L1
(3)
of seers
normal
abuse
Prr- ECT *
ECT
All
Tmentv-one
(2) ueehl\
(6)
blind
dunng
(4)
for
no treatment
those necsssan
and
1982)
Scale
b> raters (5)
mrdlcntmn
than
et cil
Rating
1960)
of ECT).
deprxwl\e
ECT
lmalldatlng
HRSD \ ALLIES
HRSD
score
ulth
of \anance (Cxroll
no alcohohsm trtxtment
(1)
exclu~~rlv
to and
of the DSTs
serious
C.1.r:
completed
\cere
s\mptoms
DST
(HRSD)
dlag-
reults
an\
Hanulton
(Harmlton
et aI
(Pri\ltera
17-item
Fol-
Dagno\tlc
1975
al\\a>h
(5)
records
conemus
et al
carbJmazepine
laboratory
mrdcal
to knItdate
rc\ Iens
lo\\lng noses
comprehen~l\r
to rule out sertous
17
(815)
umpolar
6 had
mean
TlhlE
age
the
( f SD)
of bipolar total
barnpIe
for the rntlrc
POINTS
Post ECT DST
HR3D
DST
WdI\d
1 !I I
No
tdlsordrr)
,I Astor! of
dr-
(No.\
Patent
of sctuzoaffcctl\e percent
sn-
had
patlent.
nondeltwonal
No
RDC
w.pnn,< R R NR R R R R P.ml_ll R NR Dl.~\~IlllllUd R R R R \\ ithdreu NR P.ifll&il R R R P.lrlldl
outcome
\arlable\
points tr~;ltmrnr
the
dctrrnuned
upon
course
group
prior
(2) upon completion
clInIcall\ (3)
tar
tl I rmmrdlatelv ECT
Lompletmn
four
11mr
flrbt
ECT
ot one-llurd
cow,2
ot
Jnd (41 \slthln
at
LO the
tHo-thirds
l-3
of the
for each pa~rsn~
dd\>
ot
the
tollwIng
ECT
thr: 1~151
EC T trtxtmrnt
ElectrIcal
Impul>rb
In>trument but
\\\rt:
one
L~YZ (patient
tredfment4)
s‘1e3
kzure
\\lth
the
~lmultaneou~
to
succln!
(average
dohe = 1
No
the
The
17-11em
DSTh
and
brl\\een
lI1lWl 1rt11iullILl~t?lt'
1 IlI,Jllll
HRSD
both
ECT
\\ere
w~nc~dsd ‘~l\\a>h
\rlth
dntldrpresbant 10 da>> pnor
treatment The
on da\>
Indicated
b>
patlent
docrlnr
CW~CO~S~ \\ertl
u,~l patient\ The wxdl
Jnd
total
ternunsd
JXOZIJI~~ d,lta
r\aluated
tar the group
number
LLIIuc~II~
aseh>mrnt\
clinical
of To
ECT
tor both
No
11 and
Senal
DST
ECT,
treat-
trqurnc\ No
fl\s
15
au>
tar
11 tredl-
ECT
due
16 \\lthdre\t
Fmal
In
Inds-
outcome
to
con\arld-
16 are excluded
from
data
data
In an earlier
The
patient
311 ECT
of aggregate
dppexed
For
not
15 listed
honzontal
after
all analyses
\\ertl
adrrunlstered
the
dt
treatment4
patwnt
results on
Nos
for
dunng
electrocon~ul~r~r
Patlent
rscelvlng
sedatrle-
pomt
condltlonb
Mere
2
or
tram
report
one patlent
( 4lbala
(No
et al
2)
1981)
IndI\~d-
a> LoI\ hole tredtmrnts
btandardlze
ate nnalbzed
111th IWIJ~CI~ and wurnsn-
31s
to treatment)
bornatlc
dwxntlnued
blzs for paitlents problem\
paral\
gl!copvrrolatc
or at an\
each
DST
arro\\>
confuwm
>ent after
ot group
of to
In Fig
lrert:
mental
mlmITuzs
dose = C, 75
admuubtered
Thu,
treatnlents
from
msnt>
To
and
conconutant
number
ECT
pendent
~nt~rprelation
short-acting
mubcle
hg)
to ECT
ddnurustrred 2
each
for
\\ere
course: b\
total
ments Table
treatments
a
or
anesthetIc
(alerage
antlpsbchotlc
medlcatlonb
cnntounded \rerl,l\
prtrlormsd
of
and
wxetmns
hipnotlc
tllrrllys
111 all
rscorded
doss = 0 3 mg 45 nun prior
to reduce
c Irtllllll
use
lchohns
111 alI unilateral
Standard
krp
mg/
hledcralr
tournrqurt
rscordlngs
mg ‘kg) (aLwage
\\A
J Irmb
Induce
a
8 rrce:l\cd
actl\ll\
Included
prztrralment
b>
bltrmporall>
No
~13s of
El33
barblturatc
Isa>t
generaled
admlmslrrrd
the
HRSD
M~S drtlrmng and
of
DST
-Ill
DST
normAt> before
\Aues
\\t3re log-transformed
ot dlbtnbutmn btatr>tlcal
analtses
and ctquaht> \\ere
10 obwn ot variance>
pertormed
To
de-
termlnr the slgnlflcance of decreases 111DST Calue\ end HRSD scores o\er ttmr dunng ECT treatmen t one-\\ a> ANOVA \\ Ith re:peJted meahurrz \b,l~\ used palred r-tests aere used tar paramrtnc compxlrons bet\iren pre- and posttreatment DST and HRSD rebulth. rehpcctl\elv For dtchotomous \arl&le> HT used either the chl-bquxed tebt or Fl3her.s exact prob&tlltk tebt Pcx>on’> product-moment correlatlon~ Here used to J~VZM the relatron\hlp betireen DST values and HRSD score> tar each Indlvldual patlent dunng the course of ECT treatment Rewlts
STANDARDIZED
hlean post-deuamethasone plasma cortlsol \alues and HRSD scores at the four standardized serial time points dunng ECT treatment are sho\sn In Fig 1 These aggregate data mdlcate that progressive normahzatlon of the DST occurred dunng resolutlon of the depressl\e syndrome mlth treatment One-wav ANOL’A alth repeated measures conflrmed qnlflcant reductions m these score5 oker time (P < 0 001) PaIrwise compansons between pre- and post-ECT treatment Lalues confIrmed tughI> slgruflcant reductions (P < 0 001) In both DST and HRSD bcores
POINTS
pressed \s euthynuc) there wa5 a stead! decrease In the percentage of both nonsupprebsors and depressed patients dunng treatment Thus categoncal analyses hupported trend.4 from mean data
Ttwteen patients (Nos 1 2 4 5 6. 7. 9 12 13 14. 15. 20 21) had pohttredtment DST supprewon DSTs and good response Three pattents (NOS 3.8.10) had posttreatment DST huppresslon but only partral or nonresponse Three patrents had posttreatment DST nonsuppresslon. of these
Table 3 re\eals that \\hen data \\ere annl>zrd categoncxll!, (wppressors \s nonwppressors deTABLE
ASSESSMENT
3
NLlhfBERS
-ZND
DARDIZED
SERIAL
PERCENTAGES TIhlE
OF
PATIENTS
WHO
4RE
DST
NONSLtPPRESSORS
lmmedm1e
One-thud
ECT
T\ro-rlurd>
pre-ECT DST non,uppreas,\e
l
AND
DEPRESSED
ECT
Immedk~le posl-ECT
,> /I’B dl,
n
lO,f 22
l-l,?1
s
9
90 9
bb 7
38 1
13 8
22,::. loo
lb 21 76 2
13 71 61 9
6, 20
Deprrwd
**
(HRSD
* C~I-quxr
= 26 74
21
3 19
> 101
II 4
“Ch-quare=2457
d/ =
d/=3
AT
POINTS
3
P < 0 001 P
30
STAN-
0
20406080130
0
20406OLam
40
so
80
I no
TREATMENT COURSE
(Days)
239 tuo
(Nos
call\
17
~hlle
patwnts cme
22) had pxt~al
one (No
\\ert:
not
their
(Nob
11
a
ml\,lng
data
patlent
(81%)
31on had three
III
treatments
ekplalned
(No
a good
or the\
In amman
I?
outcome and
DST
compared
\\ho
had
good
outcome
among
rrjpondm
13 of 14 (934)
DST
\\ere
ot
DST \ e:\xt
good
These
16
one
(FIbher
J Stated dIfferentI>
DST
ECT
wpprch>ors
apt
data
Induce>
and
that
anal\sls
tlons
o\er \\e
anuned
(1984)
of mean time
values
may
ulthm-subject blhty.
Daw
lead
senal
values
and
rather
strong
values
and
each
of repeated To
parable
post-deuamethasone matching
HRSD
temporal HRSD
wares
assoclatlon
scores
and
plasma
uas
ex-
cortlbol
(Fig
2)
between
elident
A
DST
m
man!
patients Indlrldual HRSD
plots
betueen-subject tlon
meekI\
\anation
between
DST
terns
that
ot DST
ment
wluch
m
patwnts
m Fig
Suggestlbe methasone
had
paralleled
of
absocld-
2)
Inspect-
Indl\Idual
cl~rucal
pat-
Improve-
the aggregate
pat-
1
ot
1980
bald
1981
et
al
plasma
rhythms
cortlsol
Nos
tient>
10. 17
of
\\ere
post-dexa-
noted
htudled
subjects
in ths
\\eekl!
ot
Our
m
4ome
study
uh~h
they Influenced
et al
1982.
Carroll group 61 5
1984)
The
hg
63 8
one-tlurd.
serial
DST
et al mean
from kg
each
to deterrmne
Edelstem
changed
for
and
fmdmgs
1983
for
kg
the
and
and
sect
respectl\ely
m
Ilmlted
number
farlure
ot
ment>
most
ma\
Jgalnbt
re-
Thlb I e
the
pro-
that
ob-
onI>
to normalize
d
when
poHer
of
about
Jnd poor outcome
greatly
lIkeI>
to
and
de\amethasone
during
while
mean
DST
values
depression
to normahze
(Figs
1 2)
Thus
aggre-
depressr\e
of
obwn
It I> uell eplbode
ac’robs patients
more
buppressorb
DST
but
\\e
good
ot
chnlcJ
lng
that
doe> not folio\\ It ma>
the out-
dunng Improve-
ot the dlscrepancles be clanfled
follou
known
cllmcal
of
cdutlon
nonsuppre>hlon
might
atlon
report5
Normallzatlon
Some
studies
pilot
conflrmatlon
predict
treatment
bet\keen
In
treat-
are
patlent>
DST
ment
~lnu~s
ECT or
ECT
ECT
brologlcal
in mo5t
AUI
of
to
to
1982)
strengthen
r preclude
at
rebpond
number
data
rndrpen-
aId Identrtlca-
Albald
responders
pro\ Ide
from
that uould
not
does
tern
patients to
perwstent
and
ECT
treatments
d lack of assoclatlon
mo>t
~m~llar
not
periods
HRSD
moderateI\
conslderatlonb
O\er-lnterpretatlon
e\en
\\eekl>
btudleh
does
ECT
conflrmed
DST that
progress
tound
antlde-
are
llrrutlng
optImaI
to become
mltlal
generalI>
the
come
after
that
benefit
Hahkett
These
treatment
normal-
ot
buppreshorh
ot the DST
1982
\\eelght
gate data
fall
that
DST
patlents
change5
DST
and DST
markers’
buggest
clinical
that
to be tenuoub
obJectl\e
tlon
pa-
a cnnlounded
Lalues
Thub
C I~n~ctans could dent
DST
treatment
to normahze
conttnue
of
ot depreh-
tlms
Illustrate
analws
1983
proportlon
ot h,ubJects tall
eftectlle
statrst~cal
\I-
1981
admlnlhtratron
senal
and
1983
marher
d problem
most
Fuente
al
hImpI\
o\er
also
encountered
mean begun
to
tram
become
bened gILen
I> not
correlated
ECT
La
\ilth
hupportb
1980
et
com-
treated
It also \uggchth
DST
matching
to htrongli ce~\lng
(De et al
In a large
medlcdtlon~
Thus had
the
to
entlre
treatment
post-ECT
contmued
to
(Berger
Felnberg
weight
65 1 and
the
the extent
62 6 kg before
t\\o-thrds
of
report>
that
ther-
tmdlng
15 a state-related
FIndIngs
\core>
This
Holsboer
\temmlng
prebsant
that
\\elghts
during
normallz~tlon
In patlent>
Grrdcn
pathophk,lolog>
Ilhel>
We
1983)
determlmng
21)
pnor
the DST
I Hashett
oscdlatmg
(eg.
(Fig
and
and
slgruflcant
patterns
normallratlon roughI>
shoHn
patients
most
values
relealed
these two ianables
1011 re\eals
tern
of
scores for each patlent
change
that electrocon\ul~l\e of DST
medrcatlon
Robenbaum
result
thus possl-
separate11
\\rlght
to tho>e obsened
lzatlon
loss of
lndlcate
a collectIon
~\t:
obsena-
address
patlent
ttteo-
emphasized
to d slgrufrcant
InformatIon
plotted
have
Jnd
patterns
antldepresbant
Targum
/t~ciuvhul purlertu of set-t& DST uttd HRSD swettretm durrt~g ECT rrearntettt Glbbonb
value,
treatment
DiscussIon
ot
po\ttredtment
= 0 15 N S
ECT
hJd
buppres-
\rlth
betiteen
bc-
dwxmtlnurd
po>ttreatment
(335)
nonapprraron
thlh anal>~~
\\ert:
pre\~ousl>)
18)
\\lth
patlent
cllnlThree
corwdrrrd
ECT
16
or nonre~pone
19) had good outcome
i\ell
b\. longer
reco\en
renu,slon a uniform be that
from from
a
pat-
J slnular
240 process occurs with the DST. Further refinements of research strategies are needed to address unanswered questions. For example, this study should be repeated with concomitant plasma dexamethasone levels to control for the possibility that repeated administration of barbiturates for ECT might change dexamethasone metabolism. If so. however, we would have expected to find progressively more nonsuppression, exactly opposite to what we observed. Finally, serial DSTs in untreated patients, i.e., those involved in placebocontrolled studies, may provide information on ‘naturalistic’ the course of hypothalamicpituitary-adrenal axis dysfunction in depression.
enous
deprewon
loss.
and
Gerken,
A., Maler.
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