Neuropsychiatric symptoms in primary progressive aphasia: phenomenology, pathophysiology, and approach to assessment and treatment


part of

SUMMARY Primary progressive aphasia (PPA) is a neurodegenerative syndrome 
characterized by insidious and progressive loss of language. Current diagnostic criteria 
require symptoms to be largely restricted to language dysfunction for at least the first 
2  years of the syndrome. However, as the disorder progresses  –  and sometimes even 
in the early stages  –  patients with PPA may exhibit neuropsychiatric symptoms. In this 
article, we review the phenomenology and frequency of neuropsychiatric symptoms in 
PPA. Among the few studies of this topic that have been performed, there is consistent 
agreement that neuropsychiatric symptoms are not uncommon among PPA patients. In 
some cases, particularly the semantic variant of PPA, symptoms are similar to those found 
in the behavioral variant of frontotemporal dementia. We further review the approach to 
assessment of behavioral symptoms in PPA and their possible management strategies, and 
speculate regarding their potential neurobiological substrates.

1Frontotemporal Disorders Unit & Alzheimer’s Disease Research Center, Department of Neurology, Massachusetts General Hospital 
& Harvard Medical School, MA, USA 
2Department of Psychiatry, University of Manitoba, Winnipeg, MB, Canada 
3Department of Neurology, McLean Hospital & Harvard Medical School, MA, USA 
4Martinos Center for Biomedical Imaging, Massachusetts General Hospital & Harvard Medical School, MGH Frontotemporal Disorders 
Unit, 149 13th Street, Suite 2691, Charlestown, Boston, MA 02129, USA 
*Author for correspondence: Tel.: +1 617 726 5571; Fax: +1 617 726 5760; bradd@nmr.mgh.harvard.edu

 � Primary progressive aphasia is typically conceptualized as a disorder primarily affecting language, but 
clinical practice and a review of the literature indicates that neuropsychiatric symptoms are common.

 � Very little is known about the biological basis of neuropsychiatric symptoms in primary progressive 
aphasia, but a few studies suggest that neurodegeneration in particular brain regions or circuits may 
underlie some of these symptoms.

 � There is relatively little systematic research on the clinical characteristics of neuropsychiatric symptoms in 
primary progressive aphasia, and no evidence-based literature on their management.

P
ra

ct
ic

e 
P

o
in

ts

Neuropsychiatric symptoms in 
primary progressive aphasia: 
phenomenology, pathophysiology, 
and approach to assessment and 
treatment

REVIEW

Mandana Modirrousta1,2, Bruce H Price1,3 & Bradford C Dickerson*1,4

Primary progressive aphasia (PPA) is a neuro­
degenerative syndrome characterized by the 
insidiously progressive loss of language abili­
ties [1]. According to contemporary diagnos­
tic criteria, the diagnosis of PPA requires that 
aphasia must be the most salient symptom and 
the major cause of impaired daily living activi­
ties for approximately the first 2 years of the 

clinical syndrome [1–3]. PPA is usually viewed as 
one major clinical form of the frontotemporal 
lobar degeneration (FTLD) spectrum of neuro­
degenerative diseases [4]. Depending on the 
type of language problem, PPA is further sub­
categorized into a nonfluent/agrammatic variant 
(PPA­G, known previously as progressive non­
fluent aphasia [PNFA]) involving effortful and 

133ISSN 1758-202410.2217/NMT.13.6 © 2013 Future Medicine Ltd Neurodegen. Dis. Manage. (2013) 3(2), 133–146

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agrammatic speech, a semantic variant (PPA­S, 
also known as semantic dementia [SD]) involv­
ing impaired single­word comprehension and a 
logopenic variant (PPA­L, also known as logo­
penic progressive aphasia) involving impaired 
word retrieval and repetition [2].

The presence of prominent early neuro­
psychiatric or behavioral symptoms is generally 
considered exclusionary for PPA. Patients with 
a neurodegenerative syndrome in which these 
symptoms are the earliest feature may fit crite­
ria for the behavioral variant of frontotemporal 
dementia (bvFTD) [5]. In spite of this distinc­
tion, which is particularly important for clinical 
research on these disorders, some patients whose 
diagnosis fits the criteria for PPA have prominent 
early neuropsychiatric or behavioral symptoms 
(a point discussed briefly in the new diagnostic 
criteria) [2]. Many others have relatively mild 
but notable symptoms in these domains, par­
ticularly as PPA progresses to involve abilities 
beyond language.

In this article, we review the existing medi­
cal literature that has investigated the neuro­
psychiatric symptoms in patients with PPA. We 
discuss the phenomenology and clinical features 
of these symptoms and speculate regarding 
their neurobiological substrates, highlighting 
relevant studies when considering the approach 
to treatment.

Review of the literature on 
neuropsychiatric symptoms in PPA
A systematic search for papers reporting stud­
ies of neuropsychiatric symptoms in PPA was 
conducted. The following MeSH search terms 
‘primary progressive aphasia’, ‘neuro psychiatric’, 
‘psychiatric’, ‘behavioral’, ‘neuroanatomy’ and 
‘neuroimaging’ were used. Subsequently, each 
subcategory of PPA (‘semantic dementia’, ‘pro­
gressive non-fluent’ or ‘agrammatic aphasia’ and 
‘lopogenic’ PPA) was combined with the other 
search terms and were searched for separately. 
The studies were identified from the follow­
ing databases: Pubmed (Medline); Embase; 
PsychInfo; and Cochrane. The references of 
all the identified articles were reviewed and 
relevant references were added to the review 
list. Finally, we entered each of the review list 
articles into the Science Citation Index of the 
Institute for Scientif ic Information Web of 
Science, and articles citing those in the review 
list were reviewed and relevant primary research 
articles were added to the list. Research and 

review articles were restricted to the English 
language from 1949 to present were included. 
We identified multiple studies reporting on the 
spectrum of neuro psychiatric symptoms in PPA, 
eight studies reporting investigations of specific 
neuropychiatric symptoms and two case reports.

�� Studies of the spectrum of 
neuropsychiatric symptoms in PPA
The studies varied in patient selection and 
comparison groups. In some studies, patients 
with PPA were analyzed as one group, whereas 
other studies employed subtype categories. The 
majority of studies used the Neuropsychiatric 
Inventory (NPI) to measure the frequency or 
severity of neuropsychiatric symptoms. A few 
studies used the Frontal Behavioral Inventory 
(FBI) or the behavioral domain of the Clinician 
Dementia Rating Scale (CDR). Except for two 
longitudinal studies, the rest were either cross­
sectional studies or retrospective chart reviews. 
Table 1 summarizes the studies that investigated 
the spectrum of neuropsychiatric symptoms in 
PPA using the NPI, FBI or CDR.

In addition to the studies that used behav­
ioral scales to measure neuropsychiatric symp­
toms, Snowden et al. evaluated the behavior of 
30 bvFTD and 11 SD patients using a newly cre­
ated semi­structured interview conducted with 
caregivers [6]. With regard to basic emotions, all 
patients were impaired in their capacity to show 
basic emotions, but SD patients were less impaired 
than bvFTD patients in their capacity to express 
anger, sadness and disgust. They did, however, 
commonly show impairments in the expression 
of fear. In the bvFTD group, changes in primary 
emotions were largely characterized by a reduc­
tion in expression of emotion, whereas some 
SD patients exhibited exaggerated emotional 
displays, while others showed diminished emo­
tional responses. With regard to social emotions, 
both groups showed reduced demon strations of 
empathy or embarrassment, and increased self­
ishness. As for interest in social interactions, 
patients with SD and bvFTD showed an oppo­
site pattern: bvFTD patients were more likely to 
avoid social contact, whereas SD patients were 
more likely to seek social contact (in contrast 
to Bozeat et al.’s findings [7]). Eating behaviors 
were altered in both groups, but with differ­
ent patterns. bvFTD patients, especially those 
with prominent dis inhibited behavior, showed 
increased eating and were indiscriminate in the 
type of food they ingested, whereas SD patients 

Neurodegen. Dis. Manage. (2013) 3(2) future science group134

REVIEW Modirrousta, Price & Dickerson



Ta
b

le
 1

. S
u

m
m

ar
y 

o
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tu
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ie
s 

o
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sp
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in

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ar

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p

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ap
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ia

.

St
u

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y 

(y
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r)
Ty

p
e 

o
f s

tu
d

y 
P

at
ie

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ts

 (n
)

Sc
al

e
O

u
tc

o
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e 
m

ea
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re
M

aj
o

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lt

s
A

d
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it
io

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al

 n
o

te
s

R
ef

.

R
o

se
n

 
et

 a
l. 

(2
00

6)

C
ro

ss
-s

ec
ti

o
n

al
PP

A
-S

 (3
3)

, 
PP

A
-G

 (1
7)

, 
PP

A
-L

 (1
7)

, 
b

vF
TD

 (5
0)

 a
n

d
 

A
D

 (1
19

) 

N
PI

To
ta

l N
PI

 
sc

o
re

, 
FT

D
-s

p
ec

ifi
c 

N
PI

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co

re

b
vF

TD
 >

 P
PA

-S
 >

 P
PA

-L
 ≈

 P
PA

-G
 ≈

 A
D

–
[1

8]

M
ar

ra
 e

t a
l. 

(2
00

7)
C

ro
ss

-s
ec

ti
o

n
al

PP
A

-G
 (1

0)
, 

b
vF

TD
 (2

2)
 a

n
d

 
A

D
 (2

0)
 

N
PI

M
ea

n
 s

ev
er

it
y 

sc
o

re
b

vF
TD

 >
 P

PA
-G

 ≈
 A

D
N

o
 P

PA
-G

 w
it

h
 

d
el

u
si

o
n

s,
 h

al
lu

ci
n

at
io

n
s 

o
r a

b
er

ra
n

t 
m

o
to

r 
b

eh
av

io
rs

[1
9]

B
an

ks
 a

n
d

 
W

ei
n

tr
au

b
 

(2
00

8)

C
ro

ss
-s

ec
ti

o
n

al
PP

A
 (4

2)
 (n

o
t 

su
b

ty
p

ed
) a

n
d

 
b

vF
TD

 (2
8)

 

N
PI

N
PI

 s
ev

er
it

y 
sc

o
re

, 
n

u
m

b
er

 o
f 

sy
m

p
to

m
s

b
vF

TD
 >

 P
PA

N
u

m
b

er
 o

f s
ym

p
to

m
s 

in
 lo

n
g

-d
u

ra
ti

o
n

 P
PA

 (>
5 

ye
ar

s)
 ≈

 b
vF

TD
M

o
o

d
, a

g
it

at
io

n
, 

n
ig

h
tm

ar
e 

sy
m

p
to

m
s,

 
ap

at
h

y 
an

d
 a

p
p

et
it

e 
sy

m
p

to
m

s 
co

m
m

o
n

 
in

 P
PA

[2
2]

Fa
te

m
i 

et
 a

l. 
(2

01
1)

C
ro

ss
-s

ec
ti

o
n

al
PP

A
 (5

5)
 (n

o
t 

su
b

ty
p

ed
), 

C
TL

 (1
11

) 

N
PI

Fr
eq

u
en

cy
 o

f 
sy

m
p

to
m

s
PP

A
 >

 C
TL

 (a
p

at
h

y,
 d

ep
re

ss
io

n
, a

p
p

et
it

e,
 m

o
to

r s
ym

p
to

m
s,

 a
n

xi
et

y 
an

d
 ir

ri
ta

b
ili

ty
) 

PP
A

 ≈
 C

TL
 (s

le
ep

-r
el

at
ed

/n
ig

h
t-

ti
m

e 
sy

m
p

to
m

s)

D
el

u
si

o
n

s,
 e

u
p

h
o

ri
a 

an
d

 
h

al
lu

ci
n

at
io

n
s 

w
er

e 
ra

re
 

o
r a

b
se

n
t 

in
 P

PA

[2
0]

Li
u

 e
t a

l. 
(2

00
4)

C
ro

ss
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ec
ti

o
n

al
SD

 (2
7)

, b
vF

TD
 

(2
4)

 a
n

d
 A

D
 o

r 
m

ild
 c

o
g

n
it

iv
e 

im
p

ai
rm

en
t 

(2
2)

 

N
PI

Fr
eq

u
en

cy
 o

f 
sy

m
p

to
m

s
El

at
io

n
/e

u
p

h
o

ri
a,

 d
is

in
h

ib
it

io
n

, a
b

er
ra

n
t 

m
o

to
r b

eh
av

io
rs

: 
b

vF
TD

 ≈
 S

D
 >

 A
D

Sl
ee

p
 d

is
o

rd
er

s:
 S

D
 >

 b
vF

TD
 a

n
d

 A
D

A
p

at
h

y:
 b

vF
TD

 >
 S

D

–
[8

]

R
o

h
re

r a
n

d
 

W
ar

re
n

 
(2

01
0)

C
ro

ss
-s

ec
ti

o
n

al
PP

A
-S

 (9
), 

PP
A

-G
 

(1
4)

, P
PA

-L
 

(7
) a

n
d

 P
PA

 
as

so
ci

at
ed

 w
it

h
 

m
u

ta
ti

o
n

s 
in

 
th

e 
G

RN
-P

PA
 (3

) 

N
PI

Fr
eq

u
en

cy
 o

f 
sy

m
p

to
m

s
Fr

eq
u

en
cy

 >
50

%
 in

 a
ll 

PP
A

 s
u

b
ty

p
es

: a
g

it
at

io
n

/a
g

g
re

ss
io

n
, 

d
ep

re
ss

io
n

, a
n

xi
et

y,
 a

p
at

h
y,

 d
is

in
h

ib
it

io
n

, i
rr

it
ab

ili
ty

/l
ab

ili
ty

 a
n

d
 

ab
n

o
rm

al
 a

p
p

et
it

e/
ea

ti
n

g
 d

is
o

rd
er

s
Fr

eq
u

en
cy

 >
50

%
 in

 P
PA

-S
: d

ep
re

ss
io

n
, a

n
xi

et
y,

 ir
ri

ta
b

ili
ty

, 
d

is
in

h
ib

it
io

n
 a

n
d

 a
b

n
o

rm
al

 a
p

p
et

it
e/

ea
ti

n
g

 s
ym

p
to

m
s

Fr
eq

u
en

cy
 >

50
%

 in
 P

PA
-G

: a
g

it
at

io
n

, d
ep

re
ss

io
n

 a
n

d
 a

p
at

h
y

Fr
eq

u
en

cy
 >

50
%

 in
 P

PA
-L

: a
g

it
at

io
n

, a
n

xi
et

y,
 ir

ri
ta

b
ili

ty
 a

n
d

 a
p

at
h

y

N
o

 r
el

at
io

n
sh

ip
 b

et
w

ee
n

 
to

ta
l s

co
re

 a
n

d
 e

it
h

er
 

d
u

ra
ti

o
n

 o
f d

is
ea

se
 o

r 
M

M
SE

 s
co

re

[9
]

X
io

n
g

 e
t a

l. 
(2

01
1)

R
et

ro
sp

ec
ti

ve
 

ch
ar

t 
re

vi
ew

PP
A

 w
it

h
 A

D
 

sp
ec

tr
u

m
 

p
at

h
o

lo
g

y 
(1

3)
 

an
d

 P
PA

 w
it

h
 

FT
LD

 s
p

ec
tr

u
m

 
p

at
h

o
lo

g
y 

(2
0)

 

N
PI

Fr
eq

u
en

cy
 o

f 
sy

m
p

to
m

s
Ea

ti
n

g
 d

is
o

rd
er

s,
 d

is
in

h
ib

it
io

n
, a

p
at

h
y 

h
ad

 h
ig

h
es

t 
sp

ec
ifi

ci
ty

 fo
r 

FT
LD

 s
p

ec
tr

u
m

 p
at

h
o

lo
g

y
Th

e 
ab

se
n

ce
 o

f 
d

ep
re

ss
io

n
 n

o
t 

u
se

fu
l 

in
 p

re
d

ic
ti

n
g

 F
TL

D
 

p
at

h
o

lo
g

y

[2
3]

K
n

o
p

m
an

 
et

 a
l. 

(2
00

8)

Lo
n

g
it

u
d

in
al

 
(1

 y
ea

r)
PP

A
-S

 (2
6)

, 
PP

A
-G

 (2
5)

, 
PP

A
-L

 (9
) a

n
d

 
b

vF
TD

 (4
7)

 

N
PI

 a
n

d
 F

B
I

Fr
eq

u
en

cy
 o

f 
sy

m
p

to
m

s
b

vF
TD

 a
n

d
 P

PA
-S

 >
 P

PA
-G

 >
 P

PA
-L

A
ft

er
 1

2 
m

o
n

th
s,

 o
n

 t
h

e 
N

PI
 a

n
d

 F
B

I, 
th

e 
PP

A
-S

 p
at

ie
n

ts
 s

h
o

w
ed

 
g

re
at

er
 w

o
rs

en
in

g
 t

h
an

 t
h

e 
o

th
er

 t
h

re
e 

su
b

ty
p

es

H
al

lu
ci

n
at

io
n

s 
an

d
 

d
el

u
si

o
n

s 
w

er
e 

in
fr

eq
u

en
t,

 b
u

t 
al

l o
th

er
 

sy
m

p
to

m
s 

re
p

o
rt

ed
 

in
 P

PA

[4
1]

A
D

: A
lz

h
ei

m
er

’s 
d

is
ea

se
; b

vF
TD

: B
eh

av
io

ra
l v

ar
ia

n
t o

f f
ro

n
to

te
m

p
o

ra
l d

em
en

tia
; C

BI
: C

am
b

rid
g

e 
Be

h
av

io
ra

l I
nv

en
to

ry
; C

D
R:

 C
lin

ic
ia

n
 D

em
en

tia
 R

at
in

g
 S

ca
le

; C
TL

: C
o

n
tr

o
l; 

D
LB

: L
ew

y 
b

o
d

y 
d

em
en

tia
; F

BI
: F

ro
n

ta
l B

eh
av

io
ra

l 
In

ve
n

to
ry

; F
TD

: F
ro

n
to

te
m

p
o

ra
l d

em
en

tia
; F

TL
D

: F
ro

n
to

te
m

p
o

ra
l l

o
b

ar
 d

eg
en

er
at

io
n;

 M
M

SE
: M

in
i M

en
ta

l S
ta

te
 E

xa
m

in
at

io
n;

 N
PI

: N
eu

ro
p

sy
ch

ia
tr

y 
In

ve
n

to
ry

; P
PA

: P
rim

ar
y 

p
ro

g
re

ss
iv

e 
ap

h
as

ia
; P

PA
-G

: P
rim

ar
y 

p
ro

g
re

ss
iv

e 
ap

h
as

ia
 

n
o

n
flu

en
t/

ag
ra

m
m

at
ic

 v
ar

ia
n

t; 
 P

PA
-L

: P
rim

ar
y 

p
ro

g
re

ss
iv

e 
ap

h
as

ia
 lo

g
o

p
en

ic
 v

ar
ia

n
t; 

PP
A

-S
: P

rim
ar

y 
p

ro
g

re
ss

iv
e 

ap
h

as
ia

 s
em

an
ti

c 
va

ria
n

t; 
SD

: S
em

an
ti

c 
d

em
en

tia
; V

aD
: V

as
cu

la
r d

em
en

tia
.

Neuropsychiatric symptoms in primary progressive aphasia REVIEW

future science group www.futuremedicine.com 135



Ta
b

le
 1

. S
u

m
m

ar
y 

o
f s

tu
d

ie
s 

o
f t

h
e 

sp
ec

tr
u

m
 o

f n
eu

ro
p

sy
ch

ia
tr

ic
 s

ym
p

to
m

s 
in

 p
ri

m
ar

y 
p

ro
g

re
ss

iv
e 

ap
h

as
ia

 (c
o

n
t.

).

St
u

d
y 

(y
ea

r)
Ty

p
e 

o
f s

tu
d

y 
P

at
ie

n
ts

 (n
)

Sc
al

e
O

u
tc

o
m

e 
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tia
.

Neurodegen. Dis. Manage. (2013) 3(2) future science group136

REVIEW Modirrousta, Price & Dickerson



had food fads and were more selective in their 
food consumption. Complex repetitive behav­
iors, including hoarding, verbal stereotypies and 
obsessive–compulsive symptoms, were prevalent 
in SD, similar to the findings of Bozeat et al. [7].

Two studies have investigated the neuro­
anatomic correlates of neuropsychiatric symp­
toms in PPA. In the f irst, NPI scores were 
compared between 27 SD patients, 24 bvFTD 
patients and 22 patients with either Alzheimer’s 
disease (AD) or mild cognitive impairment [8]. 
Principal component analysis in all patients 
showed that the presence of disinhibition was 
associated with decreased volume in the right 
anterior temporal, right ventromedial prefron­
tal cortex and right amygdala. Depression was 
associated with decreased volume in the right 
amygdala and right anterior temporal cortex and 
eating disorders were associated with decreased 
volume in the right frontal cortex and right 
ventromedial prefrontal cortex.

Rohrer and Warren recently investigated the 
neuroanatomic correlates of neuropsychiatric 
symptoms in PPA subtypes using the NPI and 
voxel­based morphometry [9]. Anxiety, apathy, 
irritability/lability and abnormal appetite/eat­
ing disorders correlated with reduced gray matter 
density in the right lateral orbitofrontal cortex, 
while disinhibition correlated with reduced gray 
matter density in the left lateral orbitofrontal 
cortex. Other correlations were found between 
apathy and atrophy in the right dorsolateral pre­
frontal cortex, irritability/lability and atrophy in 
the right anterior cingulate cortex, and disinhi­
bition and atrophy in the left anterior superior 
temporal gyrus and entorhinal cortex.

�� Studies of a single neuropsychiatric 
symptom in PPA
A number of investigations have been performed 
on a single neuropsychiatric symptom in PPA. 
With the idea that a relatively isolated language 
difficulty in a person who is otherwise healthy 
could make them vulnerable to depression and 
social withdrawal, Medina and Weintraub exam­
ined Geriatric Depression Scale (GDS) scores and 
found that a group of 61 PPA patients had higher 
GDS scores than the controls, although on aver­
age not in the ‘depressed’ range [10]. Interestingly, 
the depressed group was much more likely (43%) 
than the nondepressed group (15%) to have had 
a premorbid history of depression.

In two studies, Banks and Weintraub inves­
tigated the lack of insight in patients with PPA, 

bvFTD and AD [11,12]. They asked both the 
patients and caregivers to rate the FBI and the 
reponses were compared. PPA patients tended 
to underestimate their own behavioral changes 
relative to caregiver estimates, although not as 
prominently as bvFTD or AD patients.

In another study of insight, Eslinger et al. 
asked patients with bvFTD, PNFA, SD and AD 
to estimate their performance on tasks and also 
compared their own ratings on symptom scales 
to caregivers’ ratings [13]. They found that fronto­
temporal dementia (FTD) patients significantly 
underestimated their apathy, meaning that they 
viewed themselves as much more motivated 
than their caregivers did. This was also true 
within the PPA subgroups. Empathic concern 
was overestimated in both PNFA and SD, as was 
self­monitoring in the SD subtype.

One study investigated the prevalence of mis­
identification syndrome among people with 
different types of dementia [14]. AD and Lewy 
body dementia groups had the highest preva­
lence of this syndrome (~15%). Approximately 
8% of patients with SD (n = 24) also endorsed 
some kind of misidentification symptoms (either 
by themselves or reported by their caregivers). 
These symptoms were not present in other PPA 
subtypes (n = 101) or bvFTD (n = 119).

Sollberger et al. longitudinally studied inter­
personal traits in a group of patients with AD, 
bvFTD and SD by having patients’ caregivers 
fill out the Interpersonal Adjective Scales (IAS) 
[15]. They found that SD was associated with 
prominent changes in personality trait charac­
teristics. Dominance and warmth scores became 
abnormally low at the moderate­to­severe disease 
stage, although both showed an early drop from 
premorbid levels. The extraversion score already 
showed a significant drop to an abnormally low 
level at the very mild disease stage.

�� Studies of neuropsychiatric syndromes in 
single cases
One case report described a 75-year-old female 
without any remarkable medical or psychiatric 
history who developed a full blown panic dis­
order with agoraphobia at 71 years of age [16]. A 
year after the panic disorder, the patient exhibited 
a decline in linguistic fluency, word-finding dif­
ficulties, effortful speech and hesitant utterances 
with frequent pauses, phonemic paraphasias and 
transpositional errors. Approximately 2 years 
after the onset of aphasia, she was reported to have 
developed cognitive decline substantial enough 

Neuropsychiatric symptoms in primary progressive aphasia REVIEW

future science group www.futuremedicine.com 137



to be consistent with dementia. Neuroimaging 
highlighted left temporal and inferior fron­
tal abnormalities. Although the neuro imaging 
abnormalities in this case are consistent with 
those of PPA­S, the clinical description of lan­
guage characteristics is inconsistent with this 
diagnosis, thus leaving the subtype unclear.

The second case was a 57-year-old woman who 
had received a diagnosis of PPA by her neuro logist 
6 years earlier [17]. Initially, she developed gradual 
but progressive difficulties in word finding and 
object naming with intact comprehension. As 
PPA advanced, her speech output and under­
standing of language became compromised. 
However, she continued to maintain her social 
activities. Computed tomography was reportedly 
unremarkable. Her medical history was signifi­
cant for hypertension. There was no personal or 
family history of psychiatric illness. Later during 
the course of PPA, she started to disengage her­
self from family and social activities, eat poorly 
and neglect her appearance. Her family inter­
preted these symptoms as a result of worsening 
language problems. She then developed restless­
ness and episodes of crying. She was admitted to 
the hospital after she attempted suicide by run­
ning into traffic. She was treated with venlafax­
ine, and was engaged in art, group exercise and 
pet therapy. She showed improvements in self­
care, appetite and nonverbal interactions after 

receiving treatment; thus, her mood appeared 
to improve. In our opinion, this case description 
is consistent with the PPA­S and illustrates the 
types of neuro psychiatric symptoms described 
quantitatively in the studies above.

General synthesis of literature on specific 
neuropsychiatric symptoms
The review of the existing literature indicates 
that, even when measured using a general 
screening instrument, such as the NPI, neuro-
psychiatric symptoms are not infrequent in 
patients with PPA. As this instrument has been 
used so frequently, we performed a synthesis of 
the literature reviewed above, focusing on each 
individual neuropsychiatric symptom construct 
using the NPI as a framework. In addition, at 
the end of this section we highlight a few other 
symptom constructs relevant to PPA that are 
not captured by the NPI. Table 2 demonstrates 
the frequency range of each neuropsychiatric 
symptom reported in PPA.

�� Delusions & hallucinations
Psychotic symptoms in PPA are either rare or 
absent [18–20]. The study by Rohrer and Warren 
reported a higher rate of psychotic symptoms in 
PPA­L and PPA­S (14 and 11%, respectively), 
which could be related to longer duration or 
more severe illness [9].

Table 2. Frequency ranges of neuropsychiatric symptoms in primary progressive aphasia.

Symptom All PPAs (%) PPA-S (%) PPA-G (%) PPA-L (%) Ref.

Delusions 2–9 5–19 0–7 14 [7–9,19,20,22]

Hallucinations 0–6 0–11 0 14 [7–9,19,20,22]

Agitation/aggression 20–50 30–64 50 57 [6,7,9,20,22]

Depression/dysphoria 38–56 44–78 57 29 [7–9,20,22]

Anxiety 15–50 41–56 36 71 [8,9,20,22]

Elation/euphoria 8–19 22–37 14 14 [8,9,20,22]

Apathy/indifference 32–56 33–65 64 57 [7–9,20,22]

Disinhibition 12–38 36–74 14 43 [6,8,9,20,22]

Irritability 18–56 33–82 29 71 [6–9,20,22]

Aberrant motor behavior 4–24 22–52 0–21 29 [7–9,19,20,22]

Night-time behaviors 22–30 44–52 21 14 [8,9,20,22]

Appetite/eating behaviors 26–50 35–67 43 43 [7–9,20,22]

Mental rigidity – 80 – – [7]

Stereotypies/rituals/compulsions – 35–91 – – [6,7]

Distractibility – 90 – – [7]

Decrease in self-care – 64–65 – – [6,7]

Poor judgment – 65 – – [7]

Social withdrawal – 18–60 – – [6,7]

Lack of empathy/selfishness – 75–91 – – [6,7]
PPA: Primary progressive aphasia; PPA-G: Primary progressive aphasia nonfluent/agrammatic variant;  PPA-L: Primary progressive 
aphasia logopenic variant; PPA-S: Primary progressive aphasia semantic variant.

Neurodegen. Dis. Manage. (2013) 3(2) future science group138

REVIEW Modirrousta, Price & Dickerson



�� Agitation/aggression
Agitation/aggression is more frequent in PPA 
patients than in controls (11 vs 1%) and increases 
over time [21]. It is present in all types of PPA 
[9,18]; however, it is less severe than in bvFTD [19]. 
In one study, agitation/aggression was reported 
in up to 50% of patients with PPA [9].

�� Depression/dysphoria
Depression/dysphoria are consistently reported 
and appear to be the most prevalent psychiatric 
symptoms across all types of PPA [9,20,22]. In fact, 
one of the case reports described a PPA patient 
who gradually became depressed and attempted 
suicide, but she eventually responded to treat­
ment [17]. We have observed a similar case in our 
practice. Nevertheless, only a subset of patients 
with these symptoms meet formal diagnostic 
criteria for clinical depression [10].

�� Anxiety
Anxiety is reported as frequently as depression in 
PPA [9,22]. It is observed in up to 70% of PPA-L 
patients [9]. Anxiety can be an isolated symptom 
or a cluster of symptoms severe enough to form 
an anxiety disorder. In one case report, a patient 
with no previous anxiety disorder developed a 
classic panic disorder with agoraphobia, fulfill­
ing DSM criteria, 1 year before the symptoms 
of PPA slowly emerged [16].

�� Elation/euphoria
Mood elation/euphoria is not as common as 
depression in PPA, although it is similarly preva­
lent in bvFTD and in PPA [22], its frequency in 
the studies ranged between 5 and 20% [9,20,22].

�� Apathy/indifference
Apathy is one of the most common symptoms in 
PPA patients [9,22] and compared with controls, 
the frequency of apathy is significantly higher in 
PPA [20] and increases over time [21]. In patho­
logically confirmed PPA cases, apathy was one of 
the clinical features that suggested FTLD rather 
than AD pathology [23].

�� Disinhibition
Disinhibition is less frequent and less severe 
in PPA than in bvFTD [19,22]; however, its fre­
quency increases over time [22]. In one study, up 
to 70% of PPA-S patients exhibited disinhibi­
tion [9]. In PPA, disinhibition is one of the dis­
tinguishing features that points toward FTLD 
pathology rather than AD pathology [23].

�� Irritability
Banks and Weintraub reported a similar propor­
tion of mood symptoms including irritability 
in PPA and in bvFTD [22]. Irritability is more 
frequent in PPA when compared with controls 
[20], and is one of the most frequent symptoms 
reported in all types of PPA [9].

�� Aberrant motor behaviors
Aberrant motor behaviors are present in PPA, 
although they appear to be less frequent than 
other neuropsychiatric symptoms [9,20,22] and 
less severe than similar symptoms in bvFTD 
[18] (except one study that did not find any 
difference in the frequency between PPA and 
bvFTD [22]).

�� Night-time behaviors
PPA patients seem to have a relatively low fre­
quency of night­time behaviors (in one study the 
frequency was similar to that of controls) [20], 
although the frequency increases over time [22].

�� Appetite/eating behaviors
Compared with controls, changes in eating 
behaviors are more evident in PPA patients [20]. 
Over 3 years of longitudinal follow­up, hyper­
orality significantly increased over time in PPA 
patients [21]. This symptom (sweet food pref­
erence) was also highly associated with FTLD 
pathology rather than AD pathology in PPA [23].

�� Insight
PPA patients are better than bvFTD and AD 
patients at estimating their ability to perform 
tasks such as memory tasks. However, relative to 
other general or physical characteristics, such as 
weight or eyesight, their estimation of behavio­
ral symptoms is less accurate [11,12,24]. For exam­
ple, PPA patients may lack insight into loss of 
empathic concern and apathy [13].

�� Obsessive–compulsive spectrum 
symptoms
Compulsive and repetitive behaviors are quite 
common in the PPA­S subtype of PPA. In fact, 
the study by Snowden et al. showed that simple 
motor stereotypies such as lip smacking, hand 
rubbing and foot tapping were as common in 
PPA­S as those in bvFTD, and complex routines, 
verbal stereotypies and repetitive themes were 
more frequent in PPA­S than bvFTD patients 
[6]. In the same study, more than 90% of PPA­S 
patients exhibited some form of repetitive theme 

Neuropsychiatric symptoms in primary progressive aphasia REVIEW

future science group www.futuremedicine.com 139



and more than 70% of them were reported to 
have verbal stereotypies. Furthermore, PPA­S 
patients exhibited obsessive and compulsive 
symptoms, such as excessive worrying and 
performing the same tasks again and again, 
more frequently than bvFTD patients. Similar 
observations were reported by Bozeat et al. [7].

�� Loss of empathy
Loss of empathy, selfishness and no sense of 
embarrassment were ubiquitously found in 
PPA­S patients [6].

�� Personality changes
Personality changes are a classic symptom early 
in the course of bvFTD. By contrast, to fulfill 
diagnostic criteria for PPA, a patient must be 
largely free of these symptoms during the first 
2 years of the disease [1]. However, one recent 
study demonstrated that PPA­S is accompanied 
by subtle or overt changes in personality (domi­
nance, warmth and extraversion) even during 
the early stages [15]. Other symptoms common in 
PPA-S, such as selfishness, lack of empathy and 
disinhibition, may also be viewed as personality 
changes [6].

Neuropsychiatric symptoms across PPA 
subtypes
Taken together, the literature suggests that 
PPA­S patients commonly exhibit neuro­
psychiatric symptoms, often relatively early 
and in a fairly stereotypical fashion. Many of 
these symptoms are similar to those of bvFTD, 
including loss of empathy, changes in eating 
behavior, compulsive behavior and disinhibi­
tion. Although these symptoms are highly 
consistent with FTD, depending on when they 
begin and how they are reported by inform­
ants, it may be difficult for the clinician to 
be confident in assigning a subtype diagno­
sis (i.e., bvFTD vs PPA­S vs SD). In fact, in 
the Neary et al. diagnostic criteria for FTD, 
features considered supportive of a diagnosis 
of SD included loss of sympathy or empathy 
and narrowed preoccupations (mental rigid­
ity) [25]. Aberrant motor behavior is also com­
monly reported in some studies; in our experi­
ence this often includes elaborate movements 
related to repetitive or compulsive behaviors, 
although there has been little focused study of 
this topic. Depression is also reported as com­
mon in PPA­S in some studies; in our experi­
ence, however, at least some patients say certain 

phrases repetitively (i.e., catchphrases) that 
appear to express negative emotion (e.g., “I feel 
so stupid” or “I used to know that and now 
I just don’t know anything”), but with mini­
mal affective behavior consistent with depres­
sion, and a structured interview with some of 
these patients’ caregivers reveals little behav­
ior in daily life that appears consistent with a 
diagnosis of depression.

In PPA­G, neuropsychiatric symptoms are 
less frequent initially, but as the illness pro­
gresses it becomes increasingly common to see 
apathy, depression or irritability. In some cases 
these symptoms are present early in the illness, 
which may lead to misdiagnosis as a primary 
psychiatric disorder (commonly depression).

In PPA­L, neuropsychiatric symptoms are 
relatively infrequent early on, but increase as 
the illness progresses and include agitation, 
anxiety, irritability and apathy. In many cases 
the clinical phenomenology of neuropsychiatric 
symptoms appears similar to that seen in AD.

Neuroanatomic substrates of 
neuropsychiatric symptoms in PPA
A predominantly right­sided distribution of 
frontal and temporal areas has been implicated 
in the pathogenesis of many behavioral symp­
toms in FTD, such as apathy, disinhibition and 
abnormal eating behavior [26–29]. Right anterior 
temporal lobe atrophy is correlated with disin­
hibition and depression [8]. Right orbitofrontal, 
insular and striatal atrophy is correlated with 
eating disorders [30] and right ventromedial pre­
frontal cortex with aberrant motor behaviors, 
eating disorders and disinhibition [8,26]. In the 
study by Rohrer and Warren, anxiety, apathy, 
irritability and appetite changes were correlated 
with right hemisphere atrophy in PPA [9]. In 
PPA­S, atrophy is usually reported to be pre­
dominant in the left temporal pole and ventral 
left temporal lobe, but many patients exhibit 
subtle atrophy or hypometabolism in orbital 
and ventromedial prefrontal regions, as well as 
the ventral anterior insula and striatum; fur­
thermore, a lesser but nontrivial degree of right 
hemisphere involvement is common [31,32]. Right 
frontal abnormalities have also been observed 
in nonfluent aphasia [33–35]. In our experience, 
there is often at least subtle atrophy in homolo­
gous regions of the right hemisphere in PPA at 
baseline assessment; right hemisphere structures 
commonly become involved as the condition 
progresses (Figure 1).

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Management of neuropsychiatric 
symptoms in PPA
Given the heterogeneity of the underlying 
pathology in FTD, and the wide range of clini­
cal phenotypes involving behavioral/psychiatric, 
cognitive and motor symptoms, clinical trials 
with a homogeneous group of patients are sparse 
[36]. The selection of outcome measures is also 
challenging. General behavioral rating scales 
such as the Comprehensive Psychiatric Rating 
Scale (CPRS) do not capture all the behavioral 
abnormalities of FTD. While the NPI [37], the 
NPI-questionnaire and the Behavioral Pathology 
in Alzheimer’s Disease (BEHAVE­AD) [38] scales 
are aimed at a general dementia population 
rather than specifically at the FTD spectrum, 
they have been employed as outcome measures in 
some trials in FTD. Symptoms that commonly 
present in FTD, such as obsessive–compulsive 
spectrum behaviors, personality changes and 
lack of empathy, are not captured by these scales. 
The FBI and Cambridge Behavioral Inventory 
(CBI) were developed to more specifically cap­
ture the behavioral features of FTD [7,39,40], but 
to date they have only been used in a handful 
of trials. Table 3 lists some instruments that are 
used to measure behavioral/psychiatric symp­
toms in patients with dementia. Knopman et al. 
studied the validity of different cognitive and 
behavioral tests as outcome measures in a popu­
lation of patients with FTD [41]. They found that 
while the Modified CDR and Clinical Global 
Impression of Change scale demonstrated 
decline in the majority of patients, almost a third 
of patients improved on behavioral scales (NPI 
and FBI), suggesting that these instruments 
may not be ideal for use as outcome measures 
in FTD. Nevertheless, they may be of use in 
trials of interventions targeting specific types 
of symptoms, particularly if such trials recruit 
patients with more prominent neuropsychiatric 
symptoms at baseline.

In clinical practice, neuropsychiatric symp­
toms do not often resolve completely, yet over 
time, their frequency or severity may intensify 
or attenuate. It is critical to try to use valid 
scales to monitor these symptoms over time, 
particularly if empirical management strategies 
are attempted. The management of symptoms 
should be tailored to individual patients and 
caregivers. Education of caregivers (as well as 
patients if possible) about the safety issues and 
the nature of the neuropsychiatric symptoms is 
an important first step in management. Referral 

of families to the Association for Frontotemporal 
Degeneration and the Alzheimer’s Association 
will provide further information and help fami­
lies connect with the existing support groups. 
One reasonable strategy for prioritizing the 
goals of management is to choose one symptom 
at a time to focus on (usually the most disa­
bling symptom). A multidisciplinary care plan 
involving a psychiatrist or neurologist, or geri­
atrician specializing in these symptoms, a social 
worker, and, if possible, a nurse practitioner or 
psych ologist can assist families in developing 
behavioral strategies and providing psycho social 
support [42]. Most symptoms are best managed 
by behavioral interventions. However, if the 

Right

Right

Lateral

Lateral

Medial

Medial

Left

Left

Figure 1. Cortical atrophy in a mixed sample of patients with primary 
progressive aphasia. (A) Baseline cortical atrophy and (B) progression of atrophy 
after 2 years, illustrating not only the spread within the left hemisphere, but also 
the increasing degree of atrophy within right hemisphere structures. Red–yellow 
indicate localization of thinner cortex in the group of primary progressive aphasia 
patients compared with the matched control group.

Neuropsychiatric symptoms in primary progressive aphasia REVIEW

future science group www.futuremedicine.com 141



response is inadequate or symptoms are promi­
nent, empirical pharmacological treatments can 
be tried.

To date, no published studies report on clini­
cal trials attempting to treat neuropsychiatric 
symptoms specifically in a PPA sample. However, 
as is apparent from this literature review, these 
symptoms are not uncommon in PPA and 
despite the lack of adequate research­based evi­
dence, we need to manage the neuro psychiatric 
symptoms of these patients in day­to­day clini­
cal practice. Therefore, we must look to studies 
in bvFTD patients, mixed samples of FTD or 
other dementia patients for guidance. Below we 
summarize the results of clinical trials that have 
measured behavioral or psychiatric symptoms as 
outcomes in patients with FTD, organized by 
the type of pharmacological agent tested.

�� Antidepressants
A randomized double-blind study in 26 subjects 
with bvFTD using trazodone demonstrated a 
decrease in NPI scores by improvement of irrita­
bility, agitation, depression and eating disorders 
[43]. Data regarding paroxetine are conflicting; 
while one study did not find any improvement 

in the NPI or CBI of patients with bvFTD 
(n = 10) [4 4], two others showed an improve­
ment in behavioral symptoms [45,46]. In one ran­
domized study, eight bvFTD patients per group 
received 20 mg paroxetine or 1200 mg piracetam 
for 14 months. Patients treated with paroxetine 
showed an improvement in behavioral symptoms 
reflected by a reduction of caregivers’ distress 
[45]. In another study, 11 patients with bvFTD 
were treated with fluoxetine, sertraline or parox­
etine for 3 months. After treatment, disinhibi­
tion, depressive symptoms, carbohydrate craving 
and compulsions all showed improvement in at 
least half of the subjects in whom they had been 
present [46]. In four PPA­S patients with hostile 
behavior, sertraline reduced aggressive behaviors 
and total NPI questionnaire scores [47].

Two case series studied the efficacy of moclobe­
mide and selegiline in managing behavioral symp­
toms in FTD. Six patients with bvFTD treated 
with moclobemide for 14 days showed variable 
improvement in depression, aggressive symp­
toms, irritability, distractibility, mental rigidity, 
and stereo typy of speech and perseveration [48]. 
In three bvFTD patients, selegiline improved 
NPI scores and demonstrated some benefit on 

Table 3. Neuropsychiatric and behavioral scales used in dementia.

Scales Symptoms measured Ref.

NPI and NPI-Q Delusions, hallucinations, agitation/aggression, depression/dysphoria, anxiety, elation/euphoria, 
apathy/indifference, disinhibition, irritability, aberrant motor behavior, night-time behaviors and eating/appetite 
behaviors (NPI is a caregiver/informant interview; NPI-Q is a self-administered questionnaire with written 
instructions)

[37,63]

FBI Apathy, aspontaneity, indifference/emotional flatness, inflexibility, disorganization, inattention, personal neglect, 
loss of insight, preservation, obsession (stereotypy), hoarding, inappropriateness, poor judgment and impulsivity, 
restlessness/roaming, irritability, aggression, hyperorality/food fads, hypersexuality and utilization behavior

[39]

FRS Lack of interest, lack of normal affection, confusion in unusual surroundings, restlessness, impulsivity and lack of 
judgment

[12]

CBI Challenging behaviors (uncooperative, threatens to harm self/others), disinhibition, eating habits, sleep, 
stereotypic and motor behaviors, motivation and insight/awareness

[7]

BEHAVE-AD Paranoid and delusional ideation, hallucinations, activity disturbances, aggressiveness, diurnal rhythm 
disturbances, affective disturbances, anxieties and phobias 

[4]

NPI-C Delusions, hallucinations, agitation, aggression†, dysphoria, anxiety, elation/euphoria, apathy, disinhibition, 
irritability/lability, motor disorders, sleep disorders, appetite and eating disorders, and aberrant vocalization

[8]

FTD Inventory Behavioral disinhibition, violation of social norms, apathy, hypomania-like behaviors, loss of interpersonal 
warmth or empathy, loss of insight, decline in personal hygiene and grooming, mental rigidity and inflexibility, 
distractibility and impersistence, hyperorality and dietary changes, compulsive and stereotyped behavior, and 
environmental dependency

[64]

GDS (short form) Satisfaction with life, dropping activities or interests, feeling life is empty, getting bored, being in good spirits, 
being afraid that something bad is going to happen, feeling happy, feeling helpless, preference to stay at home, 
having problems with memory, thinking it is wonderful to be alive, feeling worthless, feeling full of energy, feeling 
hopeless and thinking most people are better off than they are

[59]

†Note that aggression has been separated from agitation.
BEHAVE-AD: Behavioral Pathology in Alzheimer’s Disease; CBI: Cambridge Behavioral Inventory; FBI: Frontal Behavioral Inventory; FRS: Frontotemporal Dementia Rating Scale; 
FTD: Frontotemporal dementia; GDS: Geriatric Depression Scale; NPI: Neuropsychiatry Inventory; NPI-C: Neuropsychiatric Inventory–Clinician Rating Scale; NPI-Q: Neuropsychiatry 
Inventory Questionnaire.

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REVIEW Modirrousta, Price & Dickerson



cognition by reducing errors on the Stroop and 
Paced Auditory Serial Addition Task [49].

�� Cognitive enhancers
An open-label study of 21 bvFTD, 13 PPA-S 
and nine PPA patients using memantine for 26 
weeks caused a transient improvement in NPI 
scores predominantly in the bvFTD group [50,51]. 
In another case series, memantine improved 
total NPI scores in three bvFTD subjects with 
specific improvement in scores of apathy, agi­
tation and anxiety [51]. However, in a different 
study, 16­week treatment of bvFTD patients 
with memantine did not change the NPI or the 
FBI scores [52]. Unfortunately, the data from 
the most recent clinical trial of memantine 
in FTD do not look encouraging with regard 
to NPI or other outcome measures [Boxer A, 
Pers.  Comm.]. Rivastigmine reduced caregiver 
burden as well as NPI, BEHAVE-AD and 

Cornell Depression Scale scores, when given 
to bvFTD patients (n = 20) for 12 months [53]. 
On the other hand, donepezil worsened bvFTD 
patients’ (n = 12) scores on a novel scale called 
the FTD Inventory and increased disinhibition 
and compulsivity [54].

�� Atypical antipsychotics
In a case report, risperidone improved agitation, 
delusions and hallucinations in bvFTD [55]. 
Another case study demonstrated that aripepra­
zole partially restored frontal glucose metabolism 
in a bvFTD patient, which the authors interpret 
as suggesting a beneficial role in frontal func­
tions [56]. Czarnecki et al. reported that three 
patients with bvFTD developed extrapyramidal 
symptoms and tardive antecollis after treatment 
with olanzapine, risperidone or quetiapine [57]. 
It is not clear from this report whether there was 
any benefit in any of these cases.

Proactively assess neuropsychiatric symptoms in PPA

Assess safety and identify the most disabling symptom(s) and their severity

� Educate patient and caregiver(s);
� Identify behavioral strategies for management;
� Consider referral of patient and caregiver(s) for psychosocial support;
� Consider empirical use of pharmacologic agents

Agitation, aggression

Atypical antipsychotics

Evaluate effectiveness and need for continued pharmacologic treatment every 3 months;
consider a careful trial of withdrawing psychotropic medications

SSRIs, mood
stabilizers

SSRIs, mood
stabilizers, trazodone,
moclobemide

AChEIs, memantine,
stimulants

Disinhibition

Depression, euphoria,
irritability, anxiety,
obsessive−compulsive 
spectrum symptoms

Apathy, indifference

Figure 2. Clinical algorithm for empirical assessment and management of behavioral and 
neuropsychiatric symptoms in primary progressive aphasia. 
AChEIs: Acetylcholinesterase inhibitors; PPA: Primary progressive aphasia; SSRI: Selective serotonin 
reuptake inhibitor.

Neuropsychiatric symptoms in primary progressive aphasia REVIEW

future science group www.futuremedicine.com 143



�� Miscellaneous agents
In a single case of bvFTD, quantitative EEG 
demonstrated profound greater left than right 
bi­frontotemporal slowing, which partially nor­
malized after methylphenidate administration 
[58]. In a randomized double­blind trial, methyl­
phenidate reduced risk betting in the Cambridge 
Gambling Task in bvFTD patients (n = 8) but 
had no effect on any other measures [59]. In a 
case report, topiramate reduced alcohol abuse 
in bvFTD but not other obsessive–compulsive 
tendencies [60]. A very recent study of oxytocin in 
bvFTD demonstrated preliminary data showing 
a beneficial effect on the NPI [61].

In summary, while it is helpful to have this 
small amount of literature, the small sample 
sizes (less than 20 participants), heterogeneity of 
participants and variability in outcome measures 
leave many questions about the utility of existing 
agents in the management of neuropsychiatric 
symptoms in FTD. At present, the treatment of 
these symptoms in FTD continues to be chal­
lenging and largely reliant on individualized 
empirical approaches. Figure 2 displays a diagram 
of our usual approach to the assessment and man­
agement of neuro psychiatric symptoms in FTD, 
with the caveat that ‘one size does not fit all’ in 
this or any other dementia.

Conclusion & future perspective
Although much of the scientif ic and clini­
cal literature on PPA focuses on the canonical 
language impairments, as the illness progresses 
and extends beyond brain language networks 
neuropsychiatric symptoms become more com­
mon. Furthermore, it is not infrequent for neuro­
psychiatric symptoms to be present during the 
early stages of PPA. In the PPA­S subtype, in par­
ticular, behavioral symptoms are very common 
and similar to those in bvFTD. On the other 
hand, PPA­G and PPA­L exhibit fewer behavioral 

symptoms that some have characterized, at least 
in some patients, as more reminiscent of those 
observed in AD [18].

While existing instruments are valuable, it is 
worth considering the development of new instru­
ments for the measurement of neuro psychiatric 
symptoms tailored toward PPA. It might be 
useful for studies of putative disease­modifying 
therapies to measure neuropsychiatric symptoms, 
in addition to language, as an indicator that an 
intervention can slow progression of or other­
wise ameliorate PPA. Ultimately, clinical trials 
of potential treatments aimed at improving the 
lives of PPA patients and their families need to 
focus not only on language and general cognitive 
function but also on neuropsychiatric symptoms.

Disclaimer
The content of this article is the sole responsibility of the 
authors and does not necessarily represent the official views 
of the NIH.

Acknowledgements
The authors wish to thank the patients and families who 
participated in their research. BC Dickerson would also like 
to thank D Hochberg for her continued partnership in their 
Primary Progressive Aphasia Program.

Financial & competing interests disclosure
This study was supported by NIH grants from the US 
National Institute on Aging (R01-AG029411 and 
P50-AG005134), the National Institute of Neurological 
Disorders and Stroke (R21-NS077059), the Alzheimer’s 
Association and the Sidney R Baer Jr Foundation. The 
authors have no other relevant affiliations or financial 
involvement with any organization or entity with a finan-
cial interest in or financial conflict with the subject matter 
or materials discussed in the manuscript apart from those 
disclosed.

No writing assistance was utilized in the production of 
this manuscript.

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