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is a significant concern for physicians. Central
precocious puberty (CPP), which is mediated
through the hypothalamic pituitary gonadal axis, has
- z& G- i/ r/ w( J% ]9 Ca higher incidence of organic central nervous system
lesions in boys.1,2 Virilization in boys, as manifested
" Z5 m8 _2 L% Y, c+ [' S7 s7 `by enlargement of the penis, development of pubic
hair, and facial acne without enlargement of testi-
+ y1 u& w3 v1 o6 z% Z2 K" Wcles, suggests peripheral or pseudopuberty.1-3 We
report a 16-month-old boy who presented with the
3 r4 M# o& ^8 p* H; w, Cenlargement of the phallus and pubic hair develop-
' L, j' }. t, L- mment without testicular enlargement, which was due
1 g: ]( E2 A0 B# F8 P* ~  B* @! ^to the unintentional exposure to androgen gel used by
the father. The family initially concealed this infor-
mation, resulting in an extensive work-up for this
& a/ v8 U" Z8 s$ Z4 u" U+ Fchild. Given the widespread and easy availability of
testosterone gel and cream, we believe this is proba-
& ]: _+ ]( o4 i+ V' mbly more common than the rare case report in the
literature.4
+ \4 R1 F/ x, e. o; L& IPatient Report
A 16-month-old white child was referred to the
2 n' s2 l6 K* k* Z6 G& T$ {endocrine clinic by his pediatrician with the concern
$ V" l! t1 _! _" hof early sexual development. His mother noticed
1 t, \0 R# e8 N/ T1 t* Glight colored pubic hair development when he was
From the 1Division of Pediatric Endocrinology, 2University of
South Alabama Medical Center, Mobile, Alabama.
3 u/ w* i) c: o" X3 j2 Z, s) |Address correspondence to: Samar K. Bhowmick, MD, FACE,
Professor of Pediatrics, University of South Alabama, College of
Medicine, 2451 Fillingim St. Mastin 212, Mobile, AL 36617-2297;
e-mail: [email protected].
about 6 to 7 months old, which progressively became
. j  U0 V, F7 s8 V7 {3 y' pdarker. She was also concerned about the enlarge-
ment of his penis and frequent erections. The child
was the product of a full-term normal delivery, with
a birth weight of 7 lb 14 oz, and birth length of
2 L* d- L0 _* c7 n. ]7 ^20 inches. He was breast-fed throughout the first year
, `2 [6 x7 {9 Jof life and was still receiving breast milk along with
2 {1 N9 D: H5 N; N+ D$ H5 zsolid food. He had no hospitalizations or surgery,
and his psychosocial and psychomotor development
was age appropriate.
The family history was remarkable for the father,
who was diagnosed with hypothyroidism at age 16,
% Q8 b2 |9 U9 V2 U  @8 W' Ywhich was treated with thyroxine. The father’s
. U2 ]' k! G" L* V* \height was 6 feet, and he went through a somewhat
$ y. Q% e6 Z. P. D+ fearly puberty and had stopped growing by age 14.
* F: |4 k+ H$ f0 S' JThe father denied taking any other medication. The
child’s mother was in good health. Her menarche
was at 11 years of age, and her height was at 5 feet
& L: c1 ]0 b& E' y( X5 inches. There was no other family history of pre-
, V1 T1 e2 K( X2 ecocious sexual development in the first-degree rela-
  L" s2 C; P0 y7 f0 Ztives. There were no siblings.
Physical Examination
The physical examination revealed a very active,
( h( y: ]! M. e: x& g/ Kplayful, and healthy boy. The vital signs documented
a blood pressure of 85/50 mm Hg, his length was
( T5 p% s! R; _90 cm (>97th percentile), and his weight was 14.4 kg
(also >97th percentile). The observed yearly growth
velocity was 30 cm (12 inches). The examination of
3 O. m. ~: p7 d, q0 ~8 _' _the neck revealed no thyroid enlargement.
The genitourinary examination was remarkable for
enlargement of the penis, with a stretched length of
8 cm and a width of 2 cm. The glans penis was very well
developed. The pubic hair was Tanner II, mostly around
( i' |2 }5 R3 x/ c) r6 T$ y540
- a& g. u% H/ ]  `$ f3 j/ o! Rat University of Manchester Library on May 25, 2015 cpj.sagepub.com Downloaded from
the base of the phallus and was dark and curled. The
testicular volume was prepubertal at 2 mL each.
The skin was moist and smooth and somewhat
oily. No axillary hair was noted. There were no
- N$ G- t# Z1 Z! X( f1 M# xabnormal skin pigmentations or café-au-lait spots.
Neurologic evaluation showed deep tendon reflex 2+
bilateral and symmetrical. There was no suggestion
9 n+ S5 G9 X6 z3 e, I$ @: {/ xof papilledema.
! h6 _+ f( y. O, Z7 B# dLaboratory Evaluation
The bone age was consistent with 28 months by
using the standard of Greulich and Pyle at a chrono-
7 n+ b5 w* x: M1 e+ Elogic age of 16 months (advanced).5 Chromosomal
karyotype was 46XY. The thyroid function test
showed a free T4 of 1.69 ng/dL, and thyroid stimu-
5 g0 B" E& L0 q4 [lating hormone level was 1.3 µIU/mL (both normal).
& U' H6 U, k8 S# CThe concentrations of serum electrolytes, blood
urea nitrogen, creatinine, and calcium all were
within normal range for his age. The concentration
0 z; D( C+ L: \' m( m2 pof serum 17-hydroxyprogesterone was 16 ng/dL
(normal, 3 to 90 ng/dL), androstenedione was 20
# M( A) {7 Z' y" bng/dL (normal, 18 to 80 ng/dL), dehydroepiandros-
: ^3 P/ @& g$ T5 ?" jterone was 38 ng/dL (normal, 50 to 760 ng/dL),
  ~/ ~7 c+ i* C9 L# d5 P/ |desoxycorticosterone was 4.3 ng/dL (normal, 7 to
49ng/dL), 11-desoxycortisol (specific compound S)
* [+ R. L' p, @# j. H. awas 43 ng/dL (normal, 10 to 156 ng/dL), serum cor-
tisol was 7.6 µg/dL (normal, 2.8 to 23 µg/dL), total
testosterone was 60 ng/dL (normal <3 to 10 ng/dL),
! o7 T) j. r4 fand β-human chorionic gonadotropin was less than
5 mIU/mL (normal <5 mIU/mL). Serum follicular
stimulating hormone and leuteinizing hormone
  l  B2 q% c% W0 X. u' Z+ ?! cconcentrations were less than 0.05 mIU/mL
(prepubertal).
) ~" z1 x4 F  N1 iThe parents were notified about the laboratory
results and were informed that all of the tests were
, A& H1 ~( n0 L: N% o9 T0 j0 vnormal except the testosterone level was high. The
follow-up visit was arranged within a few weeks to
obtain testicular and abdominal sonograms; how-
- q+ B% G, i* j  |2 C5 Y7 G+ Zever, the family did not return for 4 months.
Physical examination at this time revealed that the
" ?/ ^$ k4 l  N: Hchild had grown 2.5 cm in 4 months and had gained
2 kg of weight. Physical examination remained
unchanged. Surprisingly, the pubic hair almost com-
pletely disappeared except for a few vellous hairs at
the base of the phallus. Testicular volume was still 2
mL, and the size of the penis remained unchanged.
8 L& ^' q+ s# ?0 `The mother also said that the boy was no longer hav-
  c# w+ f% T! Z5 ~+ x2 j4 f! }; King frequent erections.
Both parents were again questioned about use of
any ointment/creams that they may have applied to
the child’s skin. This time the father admitted the
" I9 a7 W' @0 o6 qTopical Testosterone Exposure / Bhowmick et al 541
use of testosterone gel twice daily that he was apply-
' V  p8 T/ w% T" D* u, u) eing over his own shoulders, chest, and back area for
; p4 F+ o! ~3 c$ S/ Z, Ca year. The father also revealed he was embarrassed
to disclose that he was using a testosterone gel pre-
scribed by his family physician for decreased libido
" Q6 T+ Y4 H* Dsecondary to depression.
, \8 f" M3 I( n- T# J( AThe child slept in the same bed with parents.
The father would hug the baby and hold him on his
) M# P! w9 S% Y( b8 lchest for a considerable period of time, causing sig-
8 \8 h, n( {/ p& W! F1 r" mnificant bare skin contact between baby and father.
  s' I% Z# G8 U/ \/ c9 ]0 i& uThe father also admitted that after the phone call,
8 ]& K1 e  U. X7 Hwhen he learned the testosterone level in the baby
, B# K6 E7 [; c+ {was high, he then read the product information
8 c4 U/ x- g! F) m, N' E+ {5 Rpacket and concluded that it was most likely the rea-
son for the child’s virilization. At that time, they
! N% D! B% w- A% a, d6 Ldecided to put the baby in a separate bed, and the
* O( C7 P1 k$ b; P# mfather was not hugging him with bare skin and had
, h1 B* d6 d. C" k) c3 l$ Y1 y6 Z* dbeen using protective clothing. A repeat testosterone
$ o8 C: V( h' R, N6 M3 Ktest was ordered, but the family did not go to the
laboratory to obtain the test.
Discussion
& x+ ^4 f- b: \% G5 |: kPrecocious puberty in boys is defined as secondary
sexual development before 9 years of age.1,4
+ t9 w  R0 P6 ]% KPrecocious puberty is termed as central (true) when
it is caused by the premature activation of hypo-
thalamic pituitary gonadal axis. CPP is more com-
mon in girls than in boys.1,3 Most boys with CPP
4 q4 Q. T; M( a) l: o2 [may have a central nervous system lesion that is
responsible for the early activation of the hypothal-
1 D2 X0 ^6 N5 y  X( ]) Wamic pituitary gonadal axis.1-3 Thus, greater empha-
sis has been given to neuroradiologic imaging in
* N& P: I2 u: c8 f" b( K9 I) lboys with precocious puberty. In addition to viril-
ization, the clinical hallmark of CPP is the symmet-
9 c1 J; y" P- Y7 p0 j7 Nrical testicular growth secondary to stimulation by
& d7 y) t* s9 N# t( I8 Ngonadotropins.1,3
Gonadotropin-independent peripheral preco-
2 n2 i8 r" Z. r$ B% kcious puberty in boys also results from inappropriate
androgenic stimulation from either endogenous or
  A8 |/ h: O* x& D" k% k2 wexogenous sources, nonpituitary gonadotropin stim-
ulation, and rare activating mutations.3 Virilizing
7 I8 B8 i5 J+ o) y, @4 E* tcongenital adrenal hyperplasia producing excessive
adrenal androgens is a common cause of precocious
* T8 [1 Y" v* ?: e4 Y3 Gpuberty in boys.3,4
" C# s" ^7 f; h: O% S6 P+ WThe most common form of congenital adrenal
* G* p3 P6 i8 g0 Yhyperplasia is the 21-hydroxylase enzyme deficiency.
The 11-β hydroxylase deficiency may also result in
. X" b1 b1 V$ N5 b) Cexcessive adrenal androgen production, and rarely,
. b! j) O: A( u# }/ a; zan adrenal tumor may also cause adrenal androgen
excess.1,3
: O3 B; b3 v# l- l' i" j" Tat University of Manchester Library on May 25, 2015 cpj.sagepub.com Downloaded from
2 z$ f; F* ^7 u# |7 g* X. t7 _542 Clinical Pediatrics / Vol. 46, No. 6, July 2007
A unique entity of male-limited gonadotropin-
independent precocious puberty, which is also known
as testotoxicosis, may cause precocious puberty at a
very young age. The physical findings in these boys
4 u0 S, L! ^( Q' b  q8 T  L5 zwith this disorder are full pubertal development,
including bilateral testicular growth, similar to boys
  ]: N' P7 B. S+ u  G! twith CPP. The gonadotropin levels in this disorder
, U6 I# I$ z6 W( ~% Uare suppressed to prepubertal levels and do not show
pubertal response of gonadotropin after gonadotropin-
* u& o! [- l: l/ Q' A! F8 H" vreleasing hormone stimulation. This is a sex-linked
autosomal dominant disorder that affects only
males; therefore, other male members of the family
may have similar precocious puberty.3
In our patient, physical examination was incon-
sistent with true precocious puberty since his testi-
: M) T/ o+ k# Q& [cles were prepubertal in size. However, testotoxicosis
was in the differential diagnosis because his father
started puberty somewhat early, and occasionally,
testicular enlargement is not that evident in the
beginning of this process.1 In the absence of a neg-
  t0 D$ P" o8 S, d2 oative initial history of androgen exposure, our
biggest concern was virilizing adrenal hyperplasia,
either 21-hydroxylase deficiency or 11-β hydroxylase
deficiency. Those diagnoses were excluded by find-
% k2 k, I7 G6 I4 a2 U. Fing the normal level of adrenal steroids.
  Y0 M2 y$ V* i6 G5 LThe diagnosis of exogenous androgens was strongly
8 k+ J+ `+ t0 a, d8 u( X* C" msuspected in a follow-up visit after 4 months because
the physical examination revealed the complete disap-
' O! n9 \* k& s2 p" }pearance of pubic hair, normal growth velocity, and
( Y# G$ }1 }1 t) x7 Bdecreased erections. The father admitted using a testos-
% J" e+ {  ?. C0 z" u: Zterone gel, which he concealed at first visit. He was
using it rather frequently, twice a day. The Physicians’
Desk Reference, or package insert of this product, gel or
cream, cautions about dermal testosterone transfer to
unprotected females through direct skin exposure.
9 @. u3 V$ F; S5 f/ B0 S0 {0 sSerum testosterone level was found to be 2 times the
baseline value in those females who were exposed to
even 15 minutes of direct skin contact with their male
. b$ t# b% ^- z" ]% wpartners.6 However, when a shirt covered the applica-
" A6 _" j; G8 p$ \' ction site, this testosterone transfer was prevented.
% w) T$ _9 R6 w; `5 n% DOur patient’s testosterone level was 60 ng/mL,
which was clearly high. Some studies suggest that
dermal conversion of testosterone to dihydrotestos-
6 \% k# n& P1 l( Eterone, which is a more potent metabolite, is more
active in young children exposed to testosterone
1 c0 s8 C% t! n/ Jexogenously7; however, we did not measure a dihy-
drotestosterone level in our patient. In addition to
9 E8 {& B1 }* k* E5 i' i& I+ N  uvirilization, exposure to exogenous testosterone in
- t7 ^3 r0 Z. e  r* B: q0 Jchildren results in an increase in growth velocity and
5 D4 |8 g' c; w" m) Oadvanced bone age, as seen in our patient.
The long-term effect of androgen exposure during
5 `1 @" S1 [, k2 ?2 A1 O' j0 Tearly childhood on pubertal development and final
, Q) ^; F" H2 e% _& Gadult height are not fully known and always remain
" [3 i: i0 e: a" ea concern. Children treated with short-term testos-
terone injection or topical androgen may exhibit some
7 }9 x3 D* F  \. P2 l) K1 Aacceleration of the skeletal maturation; however, after
4 {! D; [, V. p+ Ocessation of treatment, the rate of bone maturation
decelerates and gradually returns to normal.8,9
+ c" I, L8 {# X# v# u- t4 D: ~There are conflicting reports and controversy
over the effect of early androgen exposure on adult
9 W" J9 G! ~1 @penile length.10,11 Some reports suggest subnormal
adult penile length, apparently because of downreg-
; c; I. V" k8 I6 ~- a& j$ `ulation of androgen receptor number.10,12 However,
/ t4 R1 d4 O" g! W( {Sutherland et al13 did not find a correlation between
childhood testosterone exposure and reduced adult
; @. e0 I3 r( U( _penile length in clinical studies.
4 s& d6 x# i9 r4 UNonetheless, we do not believe our patient is
going to experience any of the untoward effects from
testosterone exposure as mentioned earlier because
/ O$ a& p' H  n7 m. f1 Nthe exposure was not for a prolonged period of time.
Although the bone age was advanced at the time of
diagnosis, the child had a normal growth velocity at
the follow-up visit. It is hoped that his final adult
height will not be affected.
Although rarely reported, the widespread avail-
2 y4 J; B8 U0 ~  J# l( f8 wability of androgen products in our society may
: v" i1 O+ o% q  l1 V( s0 ?indeed cause more virilization in male or female
children than one would realize. Exposure to andro-
gen products must be considered and specific ques-
& q9 a9 b" j* E0 m3 ctioning about the use of a testosterone product or
gel should be asked of the family members during
the evaluation of any children who present with vir-
ilization or peripheral precocious puberty. The diag-
nosis can be established by just a few tests and by
+ y  @. ]' x' k. nappropriate history. The inability to obtain such a
history, or failure to ask the specific questions, may
result in extensive, unnecessary, and expensive
investigation. The primary care physician should be
aware of this fact, because most of these children
7 F* x" B' V  Y# y* Fmay initially present in their practice. The Physicians’
Desk Reference and package insert should also put a
- c; O& Q: L- W3 Q' O3 }2 f7 uwarning about the virilizing effect on a male or
female child who might come in contact with some-
one using any of these products.
References
: @; F* u, `; S% M/ y1. Styne DM. The testes: disorder of sexual differentiation
and puberty in the male. In: Sperling MA, ed. Pediatric
Endocrinology. 2nd ed. Philadelphia, PA: WB Saunders;
! ?8 r5 S! d4 {& T- f$ R- t7 _2002: 565-628.
2. Rivarola M, Belgorosky A, Mendilaharzu H, et al. Precocious
3 {/ O2 D7 _* H/ L5 }4 U6 gpuberty in children with tumours of the suprasellar pineal
at University of Manchester Library on May 25, 2015 cpj.sagepub.com Downloaded from
+ U+ F9 b  W  FTopical Testosterone Exposure / Bhowmick et al 543
& v7 L5 U* |) Z% Y) dareas: organic central precocious puberty. Acta Paediatr.
2001;90:751-756.
) J1 e0 [5 [' P- h! ^3. Lee PA. Puberty and its disorders. In: Lifshitz F, ed.
Pediatric Endocrinology. 4th ed. New York, NY: Marcel
$ t; D1 t2 \" O: c+ X. o* N7 u0 c" EDekker Inc; 2003:211-238.
4. Yu YM, Punyasavatsu N, Elder D, D’Ercole AJ. Sexual
development in a two-year-old boy induced by topical
$ ^, C9 Z% m: |) k% a( C* S+ |0 Bexposure to testosterone. Pediatrics. 1999;104:e23.
5. Greulich WW, Pyle SI, eds. Radiographic Atlas of
  y0 R6 s; q* lSkeletal Development of the Hand and Wrist. 2nd ed.
0 Y5 P, O% i& P& g7 O. E. jStanford, CA: Stanford University Press; 1959.
/ C7 C# f/ p) k# N2 g# V: Z3 o' q6. Physicians’ Desk Reference. Androgel 1% testosterone,
+ o" V4 g  F: h. \Unimed Pharmaceutical Inc. Montvale, NJ: Medical
Economics Company, Inc; 2004:3239-3241.
7. Klugo RC, Cerny JC. Response of micropenis to topical
- n4 @; V8 B% I1 Utestosterone and gonadotropin. J Urol. 1978;119:
. |3 b) }( ^& N; ~* p  w667-668.
8. Guthrie RD, Smith DW, Graham CB. Testosterone
treatment for micropenis during early childhood. J Pediatr.
1973;83:247-252.
9 U  J  w. r! X( |+ C# c9. Jacobs SC, Kaplan GW, Gittes RF. Topical testosterone
5 x6 x" h3 d3 s6 v# Ctherapy for penile growth. Urol. 1975;6:708-710.
10. Husmann DA, Cain MP. Microphallus: eventual phallic
! B2 n/ e( h3 xsize is dependent on the timing of androgen administra-
tion. J Urol. 1994;152:734-739.
1 ^/ p& Z5 _+ i- @+ _* i6 v. k/ `. ^11. McMahon DR, Kramer SA, Husmann DA. Micropenis:
does early treatment with testosterone do more harm
than good? J Urol. 1995;154:825-829.
' S. S1 C/ A4 e# {12. Takane KK, George FW, Wilson JD. Androgen receptor
7 g  s$ C2 w" U5 `6 N2 lof rat penis is down-regulated by androgen. Am J Physiol.
1990;258:E46-E50.
2 i: {# V, }, n- ~  V9 ~) {0 Q13. Sutherland RS, Kogan BA, Baskin LS, et al. The effect
of prepubertal androgen exposure on adult penile
length. J Urol. 1996;156:783-787.

xuejingri

絕對的好貼！謝謝啊！逐字逐圖地看完這個帖子以後，我的心久久不能平靜，感恩啊！

wlm12345

看起来不错啊，继续欣赏看看