Special Topic
With the millennium came a conceptual shift in theapproach to facial rejuvenation, from subtractivesurgical methods toward additive volume restora-
tion techniques. Understanding the importance of volumeloss to aging features has recalibrated the manner in whichthe maturing face is treated. While surgical interventionremains vital, replenishing volume to attain a more youth-ful appearance is at the forefront of aesthetic science. Facialfillers, injectable therapeutic materials for soft tissue aug-mentation, are an ideal way of restoring facial volume andcontour. Facial fillers appeal to a broad spectrum ofpatients, from those seeking minimal cosmetic enhance-ment to those seeking an effective complement to facial sur-gery. As such, facial filler injections are some of the mostcommonly performed cosmetic procedures.1 With injectableproduct features including convenient office treatments;quick, reliable results; and minimal downtime, there hasbeen an explosion in the number of commercially availablefillers. While many filler materials have shown promise,others have been disregarded or even criminalized.Considering the numerous filler types and brands currentlyavailable in the United States and worldwide, decidingwhich facial filler to use, when to use it and why, can be acomplex process. With a solid understanding of filler prod-ucts, appropriate filler selection, prudent patient selection,and proper injection techniques, the aesthetic surgeon canexpect satisfied patients with effective volume correction.Here, we will review the biology of the leading filler com-pounds and the components of successful filler treatments,including product selection and injection techniques.
FACIAL FILLERS AND THE AGING PROCESSDuring the aging process, the face loses fat and volumewhile the skin loses collagen and elasticity.2 Accentuatedby full cheeks and curves in youth, the aging facebecomes framed by bony contours wrapped with thinskin, lending a deflated and fallen appearance (Figure 1).
Understanding the aging process is crucial to attain-ing optimal results with facial rejuvenation procedures.For those with thin skin and volume loss, tightly retract-ing the facial skin through surgical intervention may notbe the best treatment.
Performance of an inappropriate surgical proceduremay produce an artificial-looking, “wind tunnel” appear-ance. Replenishing facial volume or augmenting a surgi-cal procedure with filler technologies would be a betterapproach in these patients. The placement of injectablefillers in the treatment of lines, wrinkles, and areas ofvolume depletion can achieve excellent aesthetic resultswith limited or no downtime and without the potentialmorbidity of surgery.
Selecting the Most Appropriate FillerA wide variety of filler materials and brands are current-ly available, with a seemingly endless flow of new andemerging products (Table 1). But many of the “latest andgreatest” products do not prove to be safe or effective,and they eventually fall by the wayside. Sometimes it isonly after the products have been in the marketplace formonths to years, and after many patients have beentreated, that physicians come to the realization that theproducts have failed to deliver the anticipated results.Understanding the biology of current filler compoundsthat have been approved by the U.S. Food and DrugAdministration (FDA) facilitates the best treatment selec-tion. We include silicone in our discussion, although its
Volume 28 • Number 3 • May/June 2008 • 335Aesthetic Surgery Journal
Over the last decade, there has been a shift in the way aesthetic surgeons approach facial rejuvenation. Withrecognition of the value of volume enhancement in achieving a more youthful appearance, as well as the easeof office procedures offering minimal downtime and predictable results, there has been a concomitant explo-sion in the soft tissue filler market. Given the vast array of filler products currently available, the decision ofwhich facial filler to use in specific situations can be complicated and confusing. A physician’s selection of facialfiller(s) should be based on a solid understanding of the various filler products, appropriate patient selection,and the physician’s proficiency in injection techniques. We present a review of the most widely used fillers,offering guidance on patient selection and effective injection techniques. (Aesthetic Surg J 2008;28:335–347.)
Dr. Dayan is Clinical Assistant Professor of Otolaryngology,University of Illinois, Chicago, IL. Dr. Bassichis is ClinicalAssistant Professor of Otolaryngology, University of TexasSouthwestern Medical Center, Dallas, TX.
Facial Dermal Fillers: Selection ofAppropriate Products and Techniques
Steven H. Dayan, MD; and Benjamin A. Bassichis, MD
335-347_YMAJ532_Dayan_CP 5/7/08 1:45 PM Page 335
cosmetic use is off-label, because of its history as a fill-ing agent and the continued interest of some physiciansin its potential as an effective treatment.
PRODUCTS
Hyaluronic AcidsOf the available hyaluronic acid (HA) fillers, Restylane(Medicis, Scottsdale, AZ) was the first to receiveapproval by the FDA (in December 2003) for the correc-tion of moderate to severe facial wrinkles and folds,such as nasolabial folds.3 In a study by Narins et al,4
Restylane was found to be superior to Zyplast (InamedAesthetics, Santa Barbara, CA) in 60% of patients 6months posttreatment with a smaller volume ofRestylane required to reach full correction as comparedwith Zyplast. Other HA fillers currently approved by theFDA for cosmetic use include Captique (Allergan Inc,Irvine, CA), Juvederm (Allergan), and the animal-derived Hylaform (Allergan). Restylane has an HA con-centration of 20 mg/mL with a particle size of 400 �m,3
making it a more viscous product than the FDA-approved animal-derived HA with 6 mg/mL HA. It hadoriginally been postulated that Restylane’s physical vol-ume was the sole cause for the volumetric improvement.However, a recent study revealed that Restylane operatesas an effective dermal filler by physically stretching der-mal fibroblasts, which induces de novo collagen forma-tion while inhibiting the breakdown of existingcollagen.5 These data contribute to anecdotal reports ofa cumulative Restylane effect in which subsequent treat-ments require less material than initial treatments toachieve the desired soft tissue correction.
Juvederm, a similar non–animal-based HA with aslightly higher concentration of HA (24 mg/mL) and
more extensive cross-linking, was approved by the FDAin June 2006. The additional cross-linking is thought toincrease longevity, and recent reports have shown thisproduct to persist up to 12 months.6 Whereas the HAparticles in Restylane are uniformly shaped, Juvedermparticles are randomly shaped. This is postulated to beresponsible for Juvederm’s smooth gel-like consistency.Some physicians describe this product as flowing fromthe syringe with more ease and fluidity and causing lessbruising. Much like the rivalry between Coke and Pepsi,there are those who prefer the alternate brand.Additionally, Juvederm was approved by the FDA inthinner (Ultra) and thicker (Ultra Plus) versions forgreater injection subtlety and variety. With greater parti-cle size and a slightly higher percentage of cross-linkingthan Ultra, Juvederm Ultra Plus is designated for deeper,volumizing injections.
Perlane (QMed, Eatontown, NJ), a thicker, larger-par-ticle version of Restylane, was approved by the FDA inJanuary 2007. Perlane differs from Restylane only in itsparticle size (940 vs 1090 �m), although the concentra-tion of HA remains constant in both products (20mg/mL).7 As larger particle size suspensions, Perlaneand Juvederm Ultra Plus have less total surface area sub-ject to attack by the body, and are theoretically moreresistant to degradation. Because these products arethicker, Juvederm Ultra Plus and Perlane are designed tobe injected deeper into the dermis or subdermis for vol-ume correction and contouring capabilities.
The hydrophilic nature of HA allows it to maintain itsshape using the body’s own moisture. One gram of HAcan bind up to 6 L of water.8 As a component of theextracellular matrix, intrinsic HA functions include spacefilling, lubrication, shock absorption, and protein exclu-sion. Over time, the injected hyaluronic gel is slowlyabsorbed by the surrounding tissues and disappears by aprocess called isovolumetric degradation.9 As the HAgradually degrades, each molecule binds more waterand, eventually, the same volume can be maintainedwith less HA. This provides a natural appearing volumecorrection and cosmetic persistence until the product isalmost completely degraded.
The chemical and molecular composition of naturalHA is conserved throughout all living organisms; there-fore, HA fillers do not possess species or tissue specifici-ty. This means that there is a negligible potential ofeliciting humoral or cell-mediated immune reactions.Restylane, Perlane, and Juvederm are HA dermal fillersderived from bacterial fermentation in cultures of aStreptococcus species. Because these products are not ofanimal origin, there is almost no risk of contaminationwith animal allergens, pathogens, or xenogenic diseaseduring the manufacturing process.10 Restylane, Perlane,and Juvederm lead the market in HA fillers. Other HAshave not demonstrated similar longevity or reliabilityand are rarely used. Predictable and natural results cou-pled with minimal risk and downtime have contributedsignificantly to their growing worldwide popularity.
336 • Volume 28 • Number 3 • May/June 2008 Aesthetic Surgery Journal
Figure 1. The aging face has lost volume and skin elasticity.
335-347_YMAJ532_Dayan_CP 5/7/08 1:45 PM Page 336
Volume 28 • Number 3 • May/June 2008 • 337Facial Dermal Fillers
Tab
le 1
.Fac
ial f
iller
s
Fille
rFu
nctio
nUs
esPr
osCo
nsCo
mm
ents
Colla
gen-
base
d pr
oduc
ts
Hum
an-d
eriv
ed, b
ioen
gine
ered
An
ywhe
re; e
ffect
ive
cont
ourin
g Im
med
iate
resu
lts w
ith n
o Li
mite
d lo
ngev
ity
An F
DA-a
ppro
ved
colla
gen
derm
al
(Cos
mod
erm
and
Cos
mop
last
)co
llage
n in
ject
ed to
fill
facia
l ag
ent (
lips,
fine
etch
ed li
nes)
dow
ntim
e; fo
rmul
ated
with
(la
sts 3
mon
ths)
fille
r tha
t doe
s not
requ
ire a
skin
test
wrin
kles
lidoc
aine
for p
atie
nt c
omfo
rt
Hyal
uron
ic ac
id (R
esty
lane
, N
on–a
nim
al-d
eriv
ed h
yalu
roni
c Vo
lum
e an
d co
ntou
ring
Resu
lts a
re im
med
iate
and
last
May
be
visib
le o
r pal
pate
d if
Stim
ulat
es d
e no
vo c
olla
gen
Perla
ne, J
uved
erm
, Cap
tique
) ac
id e
ngin
eere
d to
resis
t (p
erio
rbita
l, na
sola
bial
, lip
s, 6–
18 m
onth
s; re
vers
ible
inje
cted
supe
rficia
lly; l
ess
form
atio
n; F
DA-a
ppro
ved
for
degr
adat
ion
for w
rinkl
e fil
ler
chee
ks, e
tc.)
effe
ctiv
e fo
r tre
atin
g fil
ling
mod
erat
e to
seve
re w
rinkl
esan
d vo
lum
e re
plac
emen
tlip
oatro
phy
or v
ery
larg
e ar
ound
the
nose
and
mou
th; a
ll vo
lum
e co
rrec
tion
othe
r use
s con
sider
ed o
ff-la
bel;
no ri
sk o
f ani
mal
-bas
ed d
iseas
e tra
nsm
issio
n
Calci
um h
ydro
xyla
patit
e M
icros
pher
es o
f cal
cium
Vo
lum
e en
hanc
er (n
asol
abia
l Bi
ocom
patib
le a
nd u
ltim
atel
y Cl
umpi
ng, l
umpi
ng, a
nd
Do N
OT
use
Radi
esse
in th
e lip
s; (R
adie
sse)
hydr
oxyl
apat
ite in
ducin
g an
d ch
eeks
)bi
odeg
rada
ble;
long
-last
ing
nodu
les c
an a
ppea
r whe
n FD
A-ap
prov
ed fo
r fac
ial
prod
uctio
n of
col
lage
n(1
2 m
onth
s and
may
be
inje
cted
into
the
lips
lipoa
troph
y an
d m
oder
ate-
to-s
ever
ebe
yond
); m
olda
ble
wrin
kles
aro
und
the
mou
th
Poly
-L-la
ctic
acid
(Scu
lptra
Sy
nthe
tic m
ater
ial i
s inj
ecte
d Vo
lum
e en
hanc
er (n
asol
abia
l, Lo
ng-la
stin
g (1
8–24
mos
)Re
sults
not
imm
edia
te, m
ay
In a
clin
ical s
tudy
of S
culp
tra, t
he
and
New
Fill
)in
to th
e fa
ce, c
ausin
g bo
dych
eeks
, and
tem
ples
)re
quire
mul
tiple
trea
tmen
ts;
treat
men
t res
ults
last
ed fo
r up
to
to p
rodu
ce it
s ow
n co
llage
nsk
in n
odul
es a
nd g
ranu
lom
atou
s 2
year
s afte
r the
firs
t tre
atm
ent
reac
tions
pos
sible
sess
ion;
FDA
-app
rove
d fo
r fac
ial
lipoa
troph
y
Fat t
rans
fer
Fat c
ells
are
harv
este
d fro
m o
ne
Volu
me
augm
enta
tion
(che
eks,
Mos
t nat
ural
fille
r; fa
t can
be
For v
olum
e re
plac
emen
t, le
ss
“Pre
dict
ably
unp
redi
ctab
le”
part
of th
e bo
dy a
nd in
ject
edpe
riorb
ital,
and
tem
ple)
; not
st
ored
for t
ouch
-ups
effe
ctiv
e at
fine
r con
tour
ing;
in
to th
e fa
ce to
repl
enish
us
ed fo
r fin
er c
onto
urin
gdu
ratio
n is
unpr
edict
able
: vo
lum
e6
mon
ths–
10 y
rs
Silic
one
(Sili
kon
1000
and
Hi
ghly
refin
ed si
licon
e oi
l is
Volu
me
repl
acem
ent a
nd
Perm
anen
tCa
nnot
be
rem
oved
afte
r bei
ng
Bew
are
of b
lack
mar
ket
Adap
tosil
500
0)in
ject
ed u
sing
micr
odro
plet
co
ntou
ring
inje
cted
non-
med
ical s
ilico
ne; o
ff-la
bel
tech
niqu
eco
smet
ic us
e
Poly
met
hylm
etha
cryl
ate
PMM
A m
icros
pher
es
FDA-
appr
oved
for n
asol
abia
l Pe
rman
ent
Num
erou
s inj
ectio
ns n
eede
d fo
r Be
caus
e of
the
bovin
e co
llage
n (P
MM
A; A
rteco
ll an
d Ar
tefil
l)su
rrou
nded
by
colla
gen
fold
s, de
ep w
rinkl
esvo
lum
e; a
llerg
ic re
actio
ns
com
pone
nt, a
llerg
y sk
in te
stin
g is
poss
ible
; req
uire
s 3 m
onth
s for
re
quire
d; P
MM
A do
es n
ot b
reak
fu
ll ef
fect
s; so
met
imes
visi
ble
dow
nun
der s
kin
FDA,
U.S
. Foo
d an
d D
rug
Adm
inis
tratio
n.Ad
apto
sil 5
000
is m
anuf
actu
red
by B
ausc
h Lo
mb
(Roc
hest
er, N
Y). A
rteco
ll is
man
ufac
ture
d by
Arte
s (S
an D
iego
, CA)
. Cap
tique
, Cos
mod
erm
, Cos
mop
last
, Hyl
afor
m, a
nd J
uved
erm
are
man
ufac
ture
d by
Alle
gan,
Inc
(Irv
ine,
CA)
. New
Fill
is m
anuf
actu
red
by A
shfo
rd A
esth
etic
s (B
russ
els,
Bel
gium
). P
erla
ne is
man
ufac
ture
d by
QM
ed (
Eato
ntow
n, N
J). R
adie
sse
is m
anuf
actu
red
by B
iofo
rm M
edic
al (
San
Mat
eo, C
A). R
esty
lane
is m
anuf
actu
red
byM
edic
is (
Scot
tsda
le, A
Z). S
culp
tra is
man
ufac
ture
d by
San
ofi-A
vent
is (
Brid
gew
ater
, NJ)
. Sili
kon
1000
is m
anuf
actu
red
by A
lcon
(Fo
rt W
orth
, TX)
. Zyp
last
is m
anuf
actu
red
by In
amed
Aes
thet
ics
(San
ta B
arba
ra, C
A).
335-347_YMAJ532_Dayan_CP 5/7/08 1:45 PM Page 337
338 • Volume 28 • Number 3 • May/June 2008 Aesthetic Surgery Journal
Calcium HydroxylapatiteRadiesse (Bioform Medical, San Mateo, CA) wasapproved by the FDA in December 2006 for the correc-tion of facial wrinkles and folds, such as nasolabialfolds, and for the correction of facial lipoatrophy associ-ated with HIV. Radiesse is composed of calcium hydrox-ylapatite (CaHA) microspheres (25–45 �m) surroundedby a 70% methylcellulose carrier that dissipates quicklyin vivo, leaving the CaHA microsphere as a scaffoldingto promote collagen in-growth.11 Radiesse has a goodsafety record and stimulates only minimal foreign bodyreaction secondary to the spherical shape of the product,which incites less inflammation then an irregularlyshaped product.12,13 Granulomatous reactions andmigration of the product are unlikely.14 The calcium andphosphate minerals comprising Radiesse microspheresare the same as found in bone. While there was an ini-tial discussion about potential osteoneogenesis afterinjection, these concerns have been demonstrated asunfounded15 because osteoneogenesis has never beenreported in more than 6 years of clinical use. The prod-uct is faintly visible on radiographs but has not beenreported to obscure radiographic interpretation. Afterimplantation, this product is slightly more malleablethan HA. Additionally, the same volume goes further,because a lower volume of CaHA is needed to fill thesame defect as compared with HA. Importantly, CaHA isnot recommended for lip augmentation, because anunacceptable number of labial nodules have been report-ed from the product clumping together.16
Collagen-Based ProductsCosmoderm and Cosmoplast (Allergan) are human-derived, bioengineered collagen implants from a singlecell line of fibroblasts screened for viral and bacterialpathogens. Approved by the FDA in March 2003, theseproducts have a limited and waning role in the fillermarket. Because these products are of human origin,allergy skin testing is not required. Both of theseinjectable products are packaged with lidocaine (to pro-vide anesthesia), making regional nerve blocks generallyunnecessary. Although rare, complications with collageninjections have been reported, including vascular necro-sis following glabellar collagen injections.17,18 However,the most significant issues with collagen products havebeen their lack of longevity and their potential for abumpy, irregular outcome. A new porcine-based collagenproduct called Evolence (ColbarLife Sciences, Herzliya,Israel) may help to restore collagen’s reputation in thefiller market. With results lasting up to 18 months in66% of treated patients,19 Evolence is anticipated toreceive approval by the FDA in the near future.
SiliconeWhile silicone is not currently approved for cosmetic useby the FDA, it is used by some practitioners nevertheless.Silicone has a history shrouded in controversy.20
Currently, the 2 brands most commonly used off-label are
Silikon 1000 (Alcon, Fort Worth, TX) and Adaptosil 5000(Bausch Lomb, Rochester, NY). Both of these productsare approved by the FDA for ophthalmic use, but havebeen injected for soft tissue cosmetic augmentation. Thecentisokes (Cs) designation of the silicone preparationsrefers to the compound’s viscosity. A Cs of 1000 is highlyviscous and can be difficult to depress through a 30-gauge needle (by comparison, water has a viscosity of100 Cs). Reports of serious and troubling complicationsafter cosmetic silicone injections include granulomas,surface deformities, lymph vessel blockage, rosacea-likereaction, delayed hypersensitivity, migration, embolism,and blindness.21–25 However, severe complications maybe mostly avoided if pure silicone, as opposed to adulter-ated versions, is used with proper technique and indica-tions.26 Some practitioners have reported long-termeffective and safe experiences with silicone.27–29 Siliconeinjections are very technique-sensitive and require deepproduct placement. Overly superficial injections mayresult in excessive fibrosis, nodules, ridging, beading, andhypertrophic scar–like elevations.30 A serial droplet injec-tion technique may provide the best aesthetic results forcorrecting fine lines, wrinkles, and acne scarring with sil-icone. Undercorrection with multiple treatments spaced 2to 3 months apart is recommended, because the injectedsilicone droplets continue to be coated with the patient’sown collagen for up to 3 months.26 The technique ofmicrodroplets allows a monocellular fibrotic capsule toencompass each silicone particle, creating a microparti-cle. The collagen coating of the microparticles preventsmigration and allows for a stable implant with permanentresults.31 However, uncertain long-term risks remain aconcern with silicone injections.
PolymethylmethacrylateA novel filler agent approved by the FDA for cosmeticuse in January 2007 was originally marketed as Artecoll(Artes, San Diego, CA) in Europe and Canada and isnow approved in the United States as Artefill. Artefill iscomprised of smooth round polymethymethacrylate(PMMA) microspheres (30 to 42 �m diameter) sur-rounded by bovine collagen. Because of the bovine col-lagen component, allergy skin testing is required beforecorrection.32 The PMMA spheres provide permanentcorrection, because the bovine collagen is replacedwithin 3 months by host connective tissue. After 7months, it has been demonstrated that there are veryfew differences between the collagen fibers around theimplant and those of the surrounding connective tis-sue.33 Patient satisfaction outcomes have been favor-able, with one study reporting high levels of patientsatisfaction (89%).34 The complication rate was 7%,with nodule formation in the lip the most commonlyreported issue.35 It is crucial to bear in mind thatArtecoll/Artefill results are permanent and are thereforeexquisitely technique-sensitive. Multiple treatments areprudent, with extra care being taken in placement ofthe product in or around the lips, where nodule forma-
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Volume 28 • Number 3 • May/June 2008 • 339Facial Dermal Fillers
tion is more likely. Appropriate patient selection andinjection techniques are of paramount importancewhen injecting any permanent filler products.
Poly-L-lactic acidThe poly-L-lactic acid Sculptra (PLLA; Sanofi-Aventis,Bridgewater NJ) provides a semipermanent correctionand was approved by the FDA in 2004 for use in HIVfacial lipoatrophy. Sculptra works by providing a volu-mizing effect with results lasting up to 2 years after thefirst treatment, but with multiple treatments often neededto achieve complete correction. As a major component ofVicryl suture (Ethicon Inc, Sommerville NJ), PLLA wasformulated into an injectible filler and marketed underthe name “New Fill” in Europe in 1999. The 40 to 63 �mPLLA particles are suspended in a sodium oxymethycel-lulose carrier. Histologically, Sculptra causes formation ofmicroscopic nodules of multinucleated giant cells in thesubcutaneous tissues.11 Unlike HA fillers, the effects ofPLLA are gradually achieved as Sculptra induces anexpansion of dermal thickness. The substance is degrad-ed by conversion to lactic acid monomers that are subse-quently metabolized to glucose and CO2.
36,37 Beforeapproval by the FDA, studies in the HIV populationrevealed good results, documenting increased skin thick-ness with visible improvement in the signs of facial lipoa-trophy.36,38,39 Adverse events include palpable butnonvisible nodules that can be effectively dissipated withdaily massage.40 Concerns over delayed-type hypersensi-tivity reactions occurring months following injections41
may be hindering its widespread acceptance as a cosmet-ic agent (Figure 2). Overall, the delayed results, pain oninjection, and high price contribute to a product that isnot as “user-friendly” as some of the other materialsused for HIV lipoatrophy and aesthetic correction.
Fat TransferAs a usually abundant substance with no risk for immuno-logic rejection, fat is traditionally noted for its unreliablepersistency. However, recent advancements in preparation,harvesting, and injection techniques provide for longer last-ing and more predictable results.42–45 A patient’s own fat isan ideal volume source because there are no allergic reac-
tions, it is readily available, relatively inexpensive, and canbe used to effectively augment facial volume. Fat transfer asa volume correction technique is becoming an increasinglypopular method among many cosmetic physicians forachieving a natural appearing facial rejuvenation, especiallywhen performed simultaneously with a surgical procedure.However, fat transfer can also be performed in the office.
Substantial skill and experience are necessary toachieve good and consistent results with fat transfer. Ifused well, fat is an excellent filler material; however, theresults of fat transfer remain predictably unpredictable,lasting from 6 months to 10 years. Repeat injections ofstored, initially harvested fat may be necessary to main-tain the desired fullness of the treated areas.
PATIENT EVALUATION AND SELECTIONThe choice of which filler to use and when to use it isprimarily dependent on the patient rather than the prod-uct. Astute patient selection exponentially enhances aes-thetic results and patient satisfaction. The following aresome important questions to consider when determiningwhich filler to use.What has or has not made the patient happy in thepast? If a patient has been pleased with their currentfiller regimen, there is no reason to change the fillerunless there is significant cosmetic or safety advantageto using a different product. It is not recommended to re-administer a product with which the patient has beenpreviously dissatisfied. In this situation, it is best toattempt an alternate treatment or product or simply notto retreat at all. Realistic patient expectations are para-mount to all successful injection procedures.Does the patient demand either permanent orreversible products? Certain patients insist on treat-ment with a permanent filler although a temporary fillermay be the more judicious recommendation. If thepatient is an appropriate candidate with significant tem-porary filler experience, a permanent filler may be anoption. In contrast, patients new to filler therapy are besttreated with reversible, nonpermanent agents. As such,the patient and physician have flexibility in terms oftreatment volume, repetition, reversibility, and ability tomodify and customize the outcome as needed.
Figure 2. Granulomatous reaction 12 months after 3 poly-L-lactic acid treatments.
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340 • Volume 28 • Number 3 • May/June 2008 Aesthetic Surgery Journal
Can the patient tolerate downtime? Patients who can-not tolerate excess posttreatment downtime are not idealcandidates for larger semipermanent volumizer and fattransfer procedures. These treatments are placed deeperin the dermis with larger-gauge needles and can result inmore significant bruising and swelling. For patients whorequire rapid recovery, the thinner HA products or evencollagen based products may be better choices.Is the patient undergoing simultaneous surgery? Forthe patient who is undergoing surgery simultaneously,fat transfer is often an excellent option. It is abundantand easy to harvest while the patient is under anesthe-sia. A sterile controlled environment is assured.Additionally, fat transfer usually involves more down-time than the off-the-shelf injectable products and mostpatients undergoing surgery are expecting at least aweek of recovery time.Is the patient older? Older people tend to have a mini-mized immune response to a foreign body injection.Therefore, a permanent product, which may cause anintense inflammatory response in a younger patient, ismore appropriately offered to an older person.Additionally, in the event of a complication requiringskin excision of the permanent product, it is easier tocamouflage a scar in the expected creases of an olderpatient’s face than in the mildly blemished to unblem-ished thicker skin of a younger patient.Is the patient’s skin thick or thin? Thick skin tends tobetter accept the deep semipermanent volumizers,resulting in a better outcome and greater longevity. Thinskin can appear lumpy when injected with thicker HAproducts. Often, a customized treatment using 2 or 3 dif-ferent products on the same patient in different areascan achieve optimal correction.
FILLER SELECTION AND PLACEMENT BASED ONANATOMIC REGION OR DEFECTThe goal is to find the best match for the patients’ prob-lem with the optimal choice of filler therapy. Astutediagnostic skills, combined with an in-depth understand-ing of filler materials and their properties, will yield suc-cessful treatment outcomes.
Fine Etched Lines: Cosmoderm and SiliconeTo erase fine, superficially etched facial lines, a productthat can be placed superficially and not show through theskin is best. The consistency of collagen-based productsmakes them an excellent treatment for this circumstance(Figure 3). Unfortunately, their longevity (8 to 12 weeks),is not ideal. In experienced hands, silicone injections canachieve excellent aesthetic results (Figure 4). However,these permanent results are balanced against the risk ofdelayed hypersensitivity reactions and increased compli-cations.46 As such, silicone treatments are best limited toolder patients with previous experience with injectables.Importantly, as mentioned earlier, use of liquid siliconefor cosmetic purposes is currently off-label.
Superficial Facial Lines and Creases: Restylaneand Juvederm UltraFor medium-depth fine lines and creases, HA products canachieve excellent results. The product is placed just beneaththe dermis to provide lasting and predictable results. Whentreating superficially, make sure the product is placed in thedeep dermis. Superficial placement may be visible throughthe skin, worsening the patient’s appearance.
Deeper Facial Lines, Folds, and Creases: Perlane,Juvederm Ultra Plus, Radiesse, and FatFor deeper lines and creases, the more robust volumiz-ers, such as the larger particle HAs and CaHA, can effec-tively fill deeper facial lines and crevices. These productsare injected deep in the dermis or subdermis to fill thedefect completely (Figure 5).
Lip Augmentation: Restylane and JuvedermSuccessful lip augmentation requires significant skill andaesthetic expertise. One author uses thinner HAs todefine the vermilion border and lift the oral commissure(Figure 6). Larger volumizing HAs can be used for creat-ing a full pouty lip.
Periorbital Treatments: Juvederm and RestylaneThinner and conservative deposition of HA in the perior-bital region can achieve a satisfactory result in appropri-
A B
Figure 3. A, Pretreatment view of a 57-year–old woman. B, Posttreatment view 8 weeks following collagen placement into the fine radial rhytidsof the upper lip, providing a limited but successful correction of the fine lines.
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ate patients (Figure 7).47 Unfortunately, this treatment isoften administered to a poorly selected patient and inexcessive or inadequate volumes. Undertreatment anddeep placement are important to achieving a good resultin the periorbital region. Patients with thick skin, signifi-cant cheek pad ptosis, hollowing out of the infraorbitalrim/nasojugal groove, and minimal pseudoherniation oforbital fat are the best candidates. Effective periorbitaltreatment is achieved by placing no more than 0.25 mLfiller per side, injecting deep along the orbital rim in aserial depot manner. Fortunately, if the results are notacceptable, the volume augmenting effects of HA can bereversed by injecting 15 to 20 units of hyaluronidase(Amphadase; Amphastar Pharmaceuticals, RanchoCucamonga, CA) or Vitrase (Ista Pharmaceuticals,Irvine, CA) into the overcorrected area.48
Midface and Lower Face Volume Enhancement:Radiesse, Perlane, Juvederm Ultra Plus, and FatThese products nicely replace volume in the midface,cheeks, and prejowl sulcus (Figure 8). Newer intraoral injec-tion techniques greatly decrease pain, posttreatment ecchy-moses, and edema (Figure 9). The product is placed deeplyin the subcutaneous tissues and along the supraperiostealplane. After injection, the product is manually molded to
achieve the desired contour. Large volumes of product arenecessary in order to appreciate the enhancement.
ANESTHESIA FOR FILLER TREATMENTSAnesthesia is essential for most patients undergoing fillertreatments; only rarely does a patient not require it. Thetype of anesthesia, whether a local nerve block or a topi-cal anesthetic, is chosen according to the area to be treat-ed and the pain threshold level of the patient. Painperception is also location-dependent; for example, the liparea is very sensitive, and a local nerve block is almostalways required while treatment under the eyes is barelyfelt with a sharp, thin needle and a topical anesthetic.
Topical AnestheticsTopical anesthetics are commonly comprised of beta-caine, lidocaine, and tetracaine in various combinations.Many pharmacies will compound the products to a high-er concentration than what is available over the counter.ELA Max (Ferndale Laboratories, Ferndale, MI) is avail-able over the counter.
IcingIcing is a low cost, easy, and safe method for bluntingthe pain response. Some pain will still be felt during the
A BFigure 4. A, Pretreatment view of a 67-year–old woman. B, Posttreatment view following 2 silicone treatments (separated by 8 weeks) to theupper lip rhytids.
A B
Figure 5. A, Pretreatment view of a 55-year–old woman. B, Posttreatment view 3 months after complete correction with calcium hydroxylapatiteto nasolabial folds and prejowl sulcus.
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filler injection despite the precooling, but patients mayprefer this method to a medicated anesthetic. Placing anice cube or two in a clean surgical glove and then allow-ing the patient to hold it over the planned area of injec-tion for 1 to 2 minutes is usually adequate. The same icecan be used immediately posttreatment to help reducebruising and edema. Caution is advised to not overex-pose the skin to the cold, because a burn might result.
Topical Refrigerant SprayTopical dichlortetrafluoroethane and ethyl chloride skinrefrigerant spray (Pain Ease; Gebauer Co, Cleveland, OH)can be applied to the treatment area 30 to 60 secondsbefore needle insertion for topical skin anesthesia (Figure10). Such spray is perceived by the skin as very cold and
desensitizes topical nerves immediately upon application.Superficial skin pain response is significantly thwarted;however, the deeper dermal pain fibers still respond. Thespray is not intended for use on oral mucosa and isoffered only for use on the cheek and nasolabial folds.Caution should be exercised in use for those at risk forinflammatory or reactive hyperpigmentation.
Local Nerve BlocksLocal nerve blocks49 are frequently necessary perioral-ly, especially for lip injections. Injectable anestheticchoices include lidocaine, with or without epineph-rine, which are both painful upon injection. This canbe blunted by placing a topical intraoral anesthetic,such as Denti-Care topical anesthetic gel, with 20%
A BFigure 8. A, Pretreatment view of a 58-year–old woman demonstrates a prominent prejowl sulcus depression. B, Posttreatment view 2 monthsafter large-particle hyaluronic acid placed deeply into prejowl sulcus.
A BFigure 7. A, Pretreatment view of a 52-year–old woman demonstrating infraorbital hollow accentuated by aging. B, Posttreatment view 6 monthsafter placement of hyaluronic acid into infraorbital hollows.
A B
Figure 6. A, Pretreatment view of a 51-year–old woman. B, Posttreatment view 13 months after HA placement in lips. C, Placement of hyaluron-ic acid into vermilion border.
C
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Benzocaine (Medicom, Lachine, Québec, Canada) toalleviate the discomfort associated with mucosal injec-tions. However, the burning sensation is still noted asthe anesthetic product is injected, likely because of theacidic nature of the agent.
Epinephrine in the anesthetic may help to reduce bruis-ing; however, if epinephrine is included, the anesthetic effectmay persist for 8 to 10 hours. This can be an uncomfortableexperience for many patients because of the lack of oral sen-sation and can reduce oral competency. Septocaine articainehydrochloride 4% with epinephrine (Septodont Inc, NewCastle, DE) is favored by many dentists and is an excellentalternative to lidocaine. Even with its epinephrine content,its duration of effect is limited to 2 hours. Additionally, theSeptocaine has a higher pH, thereby minimizing the burningsensation upon injection. Rarely, persistent paresthesias havebeen reported with Septocaine injections, specifically withmandibular injections. Caution is recommended to preventdirect injection of the neural foramen.50
Local Nerve Block TechniquesA Septocaine ampule is placed into a stainless steel den-tal injector syringe with a 27-gauge, 1.25-in needle(Kendall Tyco Healthcare Group LP, Mansfield, MA). Acotton-tipped applicator with topical local anesthesia isplaced on the buccal or gingival labial sulcus for 3 to 5minutes (Denti-Care topical anesthetic gel). The needleis placed just above the canine at a 30° angle up to thecanine fossa, with the bone of the anterior maxillarywall just lateral to the nasal–alar insertion. The needle isdirected down to the bone and approximately 0.3 mL ofanesthesia is injected. Distraction devices, such as avibrating massager placed on the maxillary eminence,can significantly minimize injection discomfort (Figure11). Injections are made bilaterally to achieve anesthesiato the entire upper lip within about 2 minutes.Alternatively, the injections can be accomplished tran-scutaneously (Figure 12). This technique is easier andmore reliable when first learning nerve blocks, but it isalso associated with a greater discomfort to the patient.
For lower lip anesthesia, following retraction of thelower lip, the second premolar is located and the needle
is inserted into the gingivolabial sulcus, about 0.5 inbeneath and onto the bone of the mandible.Approximately 0.2 mL of anesthetic is injected bilateral-ly to anesthetize the entire lower lip and chin area(Figure 13). Because mandibular injections are slightlymore painful then the maxillary injections, a distractiondevice placed on the mentum will significantly bluntpain perception (Figure 14).
Some physicians utilize a micro–nerve block tech-nique, in which small aliquots of anesthetic are injectedalong the mucosal border of the lip near the gingival sul-cus. Microblocks have the advantage of not producing asdeep a regional anesthetic. However, this technique maytake longer to perform and the potential for incompleteanesthesia is greater.
INJECTION TECHNIQUESTo achieve successful filler treatments, there are a vari-ety of different techniques used including threading,serial droplet, and fanning methods.
The Threading MethodProbably the most popular technique, threading is bestused for treating the vermilion border. Threading is atechnique which involves depositing the product as theneedle is withdrawn from the tissue. In this technique,the needle is inserted to its hub, taking care that the nee-dle is in the very deepest portion of the dermis or in thesubdermal tissues. If the skin dimples down with down-ward pressure on the needle, then the needle is in thedermis. If the needle can be visualized through the skin,then it is too superficial and will generally not producean aesthetically pleasing effect. If there is little resistanceto the needle and the product upon injection, then theneedle is in the subcutaneous tissue.
The Serial Droplet MethodThis technique is commonly mentioned with siliconeinjection. It is described as placing the needle into thedeep dermis (or deeper) and depositing a very minimalamount of product, approximately 0.01 to 0.03 mL.Multiple serial droplets are placed along the wrinkle, a
Figure 9. Intraoral injection technique for midface correction withlarge-particle hyaluronic acid.
Figure 10. Topical anesthetic spray is used to desensitize the skin.
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technique that can lead to beading and a dull needle,necessitating multiple needle replacements. Thismethod is best utilized for treating the glabellar creases(Figure 15) and for placement along the inferior orbitalrim in treating periorbital hollows.
The Fanning MethodThe fanning method is the preferred manner for achiev-ing superior, natural appearing, and longer-lastingresults. However, the amount of product that is used isdependent on the depth of the crease, the patient’sdesired outcome, and the patient’s financial preferences.The fanning method is appropriate for placement of theproduct in the immediate subdermis or subcutaneoustissues. It is very difficult (if not impossible) to perform
the fanning technique in heavily resistant dermal tissues.Because the subdermal tissues are less resistant, allow-ing for more diffusion, more product is usually neededfor complete correction with fanning as compared withother techniques.
In the fanning method, the needle is placed justbelow the dermis at a 30° angle with the bevel positionirrelevant. The needle is passed back and forth underthe fold, extending approximately 2 mm lateral to 2 mmmedial to the fold (Figure 16). The product is depositedboth as the needle is inserted and withdrawn, filling inan approximately 4-mm wide band of product with thefold in the center. The product should be depositedslowly and steadily. Injecting HA at 0.3 mL/min or slow-er has been determined to result in less ecchymoses.51 Inmost patients, it will take at least 1 mL of filler per foldto achieve a satisfactory result. It is important to achievecomplete correction but to stop at the desired cosmeti-cally appealing endpoint and refrain from overcorrec-tion. Results tend to improve over the next couple ofweeks as inflammation subsides and as the product “set-tles” into the fold.
Figure 11. Intraoral injection with Septocaine is used to achieveanesthesia to upper lip. Vibrating distraction device is used to bluntdiscomfort with injection of anesthetic.
Figure 13. Inferior mental nerve block with injection of Septocainenear the mental foramen.
Figure 14. Vibrating distraction device on the mentum blunts the dis-comfort of injection.
Figure 12. Transcutaneous injection of anesthetic down to anteriorface of maxilla.
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DISCUSSION
Using appropriate patient selection, filler choices, andinjection techniques, filler outcomes and patient satisfac-tion can be optimized. Two important ingredients of suc-cess are: (1) treating to complete correction and (2)appropriate placement of the filler material in the dermis.
In terms of complete correction, patient satisfactionfollowing a filler treatment may be dependent onwhether or not a complete aesthetic correction wasachieved. Frequently, previously treated patients whoare unsatisfied with their result were shown to have
been inadequately treated or undertreated. It is likelythat if more product had been initially placed into thearea of desired correction, the patient would have beenmore satisfied. Other than periorbitally (where undercor-rection is the rule), when complete correction is attainedthe patient is more likely to be pleased, subsequentlyreturn, and refer other patients (Figure 17). Anecdotally,experienced injectors have recognized that if completecorrection is initially accomplished, the correction per-sists longer. In all cosmetic procedures, the objective isto satisfy the patient. In fact, if the patient appears to bedifficult to satisfy, it may be wise to discourage the treat-ment rather than produce an unhappy patient.
In terms of the appropriate placement of filler materi-al in the dermis, in contrast to initial teachings andpackage inserts, it is the authors’ experience that fillermaterials should not be placed in the dermis but, rather,deeper, for a more lasting and aesthetically naturalresult. Placement in the subdermis lifts the crease orfold, whereas product placed into the dermis can resultin a “worm-like” blue line under the skin. This “tindleeffect” is not only unsightly, but tell-tale evidence of afiller treatment. Fortunately, this misplaced product canbe easily removed by nicking the skin with an 18-gaugeneedle and expressing the product (Figure 18). Filler canbe removed in this fashion at any point following injec-tion, from immediately after placement to months post-treatment. Occasionally, for large volume correction (i.e.,cheeks and prejowl sulcus), the product is placed deeperinto the subcutaneous tissues. At this level, thehydrophilic properties of the HA will diffusely expand inthe area of desired correction. However, a significant vol-ume of product may be necessary before the correctionis appreciated.
As recently described, it is postulated that the stretchplaced on the tissues by HA fillers stimulated dermal
A B
Figure 15. A, Pretreatment view of a 35-year–old man. B, Posttreatment view 1 year after placing hyaluronic acid via a serial droplet method intothe glabellar creases.
Figure 16. Filler is placed in a lane extending 2 mm lateral and 2 mmmedial to the nasolabial fold in a fanning method.
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fibroblasts to produce collagen. While this study exam-ined Restylane, this phenomenon may be relevant to allfacial fillers.4 Future studies focusing on correctionlongevity will likely elucidate variables contributing tooptimal filler treatments.
CONCLUSIONCurrent trends in facial rejuvenation have made a shifttoward volume replacement complementing, or in lieu of,surgically advancing the skin and supporting ptotic tis-sues. Contemporary patients overwhelmingly request min-imally invasive alternatives for achieving a rejuvenatedappearance. Fillers can meet many of their desires, withconcomitant high safety profiles and minimized down-time. With the rapidly evolving filler market, it is vital forphysicians to make educated and thoughtful choicesbefore broadly applying novel products. With today’scommercially available materials, the aesthetic physician’sarmamentarium of facial fillers can be appropriately andeffectively used to achieve significant cosmetic outcomes.Which products are ultimately used in a successfulpatient–filler scenario is dependent on the patient’s aes-thetic needs in combination with the physician’s knowl-edge of current facial fillers and injection expertise. ◗
DISCLOSURES
The authors have received an unrestricted educational grant fromMedicis and are both on the National Educational Faculty forAllergan. Dr. Dayan has received research grant support fromBioform, Allergan, and Medicis.
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Accepted for publication March 6, 2008.
Reprint requests: Steven H. Dayan, MD, FACS, Clinical Assistant Professor,University of Illinois, 845 N Michigan Ave, Ste 923, Chicago, IL 60611. E-mail: [email protected]
Copyright © 2008 by The American Society for Aesthetic Plastic Surgery, Inc.
1090-820X/$34.00
doi:10.1016/j.asj.2008.03.004
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