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Thyroid News
BACK
Edited
by GEORG HENNEMANN, MD
Refence
values of serum TSH in humans:
Confusing
data!
Two recent publications report 95% reference values for serum TSH of which
the upper-normal level differ considerable. Thus while the NACB guide lines
suggest a limit of 2.5mU/L (see below),
Jensen et al. (see below) find a value that
is not different from the ones that we still use i.e. 4 mU/L.
What is the consequence for clinicians from this confusing situation? Should
we change TSH reference values or not? Maybe people should get together to
sort out the differences, so that hopefully we soon know where we stand.
NACB guide lines 2002:
Laboratory Support for the Diagnosis and Monitoring of Thyroid Disease.
Laurence M. Demers LM and Spencer CA, pp34
TSH Upper Reference Limits-Over the last two decades, the upper reference limit for TSH has
steadily declined from ~10 to approximately ~4.0-4.5 mIU/L. This decrease
reflects a number of factors including the improved sensitivity and
specificity of current monoclonal antibody based immunometric assays, the
recognition that normal TSH values are log-distributed and importantly,
improvements in the sensitivity and specificity of the thyroid antibody
tests that are used to pre-screen subjects. The recent follow-up study of
the Whickham cohort has found that individuals with a serum TSH >2.0 mIU/L
at their primary evaluation had an increased odds ratio of developing
hypothyroidism over the next 20 years, especially if thyroid antibodies were
elevated (35). An increased odds-ratio for hypothyroidism was even
seen in antibody-negative subjects. It is likely that such subjects had low
levels of thyroid antibodies that could not be detected by the insensitive
microsomal antibody agglutination tests used in the initial study (207).
Even the current sensitive TPOAb immunoassays may not identify all
individuals with occult thyroid insufficiency. In the future, it is likely
that the upper limit of the serum TSH euthyroid reference range will be
reduced to 2.5 mIU/L because >95% of rigorously screened normal euthyroid
volunteers have serum TSH values between 0.4 and 2.5 mIU/L.
(b) TSH Lower Reference Limits -Before the immunometric assay era, TSH methods were too insensitive
to detect values in the lower end of the reference range (209).
Current methods however, are capable of measuring TSH at the lower end and
now cite lower limits between 0.2 and 0.4 mIU/L (202). As the
sensitivity of the methods has improved, there has been an increased
interest in defining the true lower limit of normal to better determine the
presence of mild (subclinical) hyperthyroidism. Current studies suggest
that TSH values in the 0.1 to 0.4 mIU/L range may represent thyroid hormone
excess and in elderly patients might be associated with an increased risk of
atrial fibrillation, and cardiovascular mortality (36,37). It is
therefore important to carefully exclude subjects with a goiter and any
illness or stress in the normal cohort selected for reference range study.
Clinical Chemistry and Laboratory
Medicine 42,
(7)
(2004)
Esther Jensen,
Per Hyltoft Petersen, Ole Blaabjerg, Pia Skov Hansen, Thomas H. Brix,
Kirsten Ohm Kyvik and Laszlo Hegedüs
Establishment of a serum thyroid stimulating hormone (TSH) reference
interval in healthy adults. The importance of environmental factors,
including thyroid antibodies
It has
previously been shown that thyroid antibodies affect thyroid stimulating
hormone (TSH) concentrations in men and women and that TSH levels are
predictive of future thyroid disease. We investigated the validity of the
National Academy of Clinical Biochemistry (NACB) guidelines regarding the
TSH reference interval by studying 1512 individuals. Two hundred and fifty
had at least one thyroid antibody, 121 were taking medications other than
estrogens and occasional analgesics, and 105 reported a family history of
thyroid disease. Serum TSH, thyroid peroxidase antibodies (TPOab) and
thyroglobulin antibodies (Tgab) were determined on AutoDELFIA and TSHRab by
a radioreceptor assay (RRA) from Brahms Diagnostica. For individuals without
thyroid antibodies and other risk factors, no effect of age and gender was
seen for serum TSH. Neither medication nor the presence of Tgab alone had
any influence on serum TSH. TPOab alone or in combination with Tgab were
associated with an increased serum TSH level. The ‘cumulative percentage
distributions’ of subgroups, as well as the combined population, was ln-Gaussian
distributed. The central 95% of the population was within the 95% CI in
rankit-plots. Consequently, a common reference interval for serum TSH of
0.58–4.07 mIU/l for all adults between 17 and 66 years of age was
established. This reference interval is much higher than expected from the
NACB guidelines.
TSH response to TRH in bipolar depression
There have been reports in the literature about the hypothalamic-pituitary-thyroid (HPT)-axis in psychiatric patients, suggesting that it may be abnormal. The present study (see below) has the advantage that it is performed in a well defined group of patients, i.e. with bipolar affective disorder, that repeated HPT-axis function tests were done in a prospective manner over a period of no less than 3 years. Tests were done every 3 months and at the same time mood ratings were collected. The authors find an inverse correlation between the TSH response to TRH and the severity of mood derangement. The authors can not rule out an influence of lithium therapy on the results but argue that this is unlikely. The mechanism of this relationship is unknown but could point to a supra-hypothalamic regulation of the HPT-axis. It would be interesting to evaluate if this type of regulation is a general phenomenon, i.e. to test the HPT-axis in non-psychiatric healthy subjects versus changes in mood over a period of time.
Relationship between mood and TSH response to TRH stimulation in bipolar affective disorder Psychoneuroendocrinology. 2004 Aug;29(7):917-924. J. K. Larsen , J. Faber, E. M. Christensen, B. B. Bendsen, K. Solstad, A. Gjerris and K. Siersbæk-Nielsen
Abstract -Moderate to severe depression and mania are associated with a reduced thyroid stimulating hormone (TSH) response to TSH releasing hormone (TRH). Continued reduction of this response after clinical recovery seems indicative of early relapse. The aim of the present study was to test the relationship between mild changes in mood and the TSH response to TRH stimulation in patients with bipolar affective disorder. Nineteen outpatients with bipolar affective disorder were followed prospectively for three years. Every third month, mood symptoms were rated using the 17-item Hamilton Depression Rating Scale (HAMD-17) and the Bech-Rafaelsen Mania Scale (BRMS). A TRH test was performed in connection with each rating session (IV injection of 200 μg TRH), and serum TSH was measured at 0, 20, and 60 min. The maximum TSH response (D-max TSH) and the temporal change in D-max TSH between succeeding rating sessions (DD-max TSH) were determined. Psychometric rating and TRH data were obtained for a total of 198 examinations. The temporal change in mood symptom rating score was negatively correlated with the temporal change in D-max TSH, thus suggesting that increasing severity of mood symptoms was related to a reduced TSH response to TRH stimulation. The temporal change in TSH response to TRH stimulation correlated with the actual score on an overall index of symptom severity. In conclusion, milder fluctuations in mood in bipolar affective disorder seem to correlate with the TSH response to TRH stimulation: Increasing severity of mood symptoms seems to be associated with reduced TSH response.
Improved cytological differentiation between benign and malignant follicular
thyroid tissue, using molecular markers (12 May 2004)
A common problem in clinical practice is the evaluation and management of
thyroid tumors with a follicular pattern. Cytology obtained by FNA cannot
differentiate between follicular thyroid adenoma (FTA) and follicular
thyroid carcinoma (FTC). Therefore most guidelines recommend that a nodule
diagnosed as having a follicular pattern should be surgically removed to
provide an accurate diagnosis. Overall, only 8–17% of these cytologically
suspicious nodules are indeed malignant on histology. A large percentage of
patients would, therefore, benefit greatly from improved diagnosis of FNA
material. Accurate molecular markers based on genes expressed differentially
between FTC and FTA would be one means of improving the accuracy of
diagnoses made from FNA.
Janete M. Cerutti,
et al, abstract see below,
analyzed the gene-expression profile in normal thyroid tissue, follicular
adenoma tissue (FTA), and follicular carcinoma tissue (FTC). They selected
twelve transcripts that were highly expressed in the FTC library, and five
that were expressed only in FTA and normal-thyroid libraries. These
marker-transcripts were tested in 23 specimens of FTC, FTA and normal
thyroid tissue, in order to evaluate if differences in expression profile
could improve cytological differentiation between FTA and FTC.
ABSTRACT A preoperative diagnostic test
that distinguishes benign from malignant thyroid carcinoma based on gene
expression
Janete M. Cerutti,1,2 Rosana Delcelo,3 Marcelo João Amadei,1
Claudia Nakabashi,1 Rui M.B. Maciel,1 Bercedis Peterson,4
Jennifer Shoemaker,4 and Gregory J. Riggins5
J Clin Invest. 2004 April 15; 113 (8): 1234–1242
Accurate
diagnosis of thyroid tumors is challenging. A particular problem is
distinguishing between follicular thyroid carcinoma (FTC) and benign
follicular thyroid adenoma (FTA), where histology of fine-needle aspirates
is not conclusive. It is often necessary to remove healthy thyroid to rule
out carcinoma. In order to find markers to improve diagnosis, we quantified
gene transcript expression from FTC, FTA, and normal thyroid, revealing 73
differentially expressed transcripts (P ≤ 0.0001). Using an
independent set of 23 FTCs, FTAs, and matched normal thyroids, 17 genes with
large expression differences were tested by real-time RT-PCR. Four genes (DDIT3,
ARG2, ITM1, and C1orf24) differed between the two
classes FTC and FTA, and a linear combination of expression levels
distinguished FTC from FTA with an estimated predictive accuracy of 0.83.
Furthermore, immunohistochemistry for DDIT3 and ARG2 showed consistent
staining for carcinoma in an independent set 59 follicular tumors (estimated
concordance, 0.76; 95% confidence interval, [0.59, 0.93]). A simple test
based on a combination of these markers might improve preoperative diagnosis
of thyroid nodules, allowing better treatment decisions and reducing
long-term health costs.
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Subclinical thyroid disease: to treat or not to treat?
The
controversy lingers on!
Surks MI, Ortiz E, Daniels
GH, Sawin CT, Col NF, Cobin RH, Franklyn JA, Hershman JM, Burman KD,
Denke MA, Gorman C, Cooper RS, Weissman NJ.
JAMA. 2004 Jan 14; 291(2): 228-38.
Subclinical thyroid disease: scientific review and guidelines for
diagnosis and management.
ABSTRACT -CONTEXT:
Patients with serum thyroid-stimulating hormone (TSH) levels outside the
reference range and levels of free thyroxine (FT4) and triiodothyronine
(T3) within the reference range are common in clinical practice. The
necessity for further evaluation, possible treatment, and the urgency of
treatment have not been clearly established. OBJECTIVES: To define
subclinical thyroid disease, review its epidemiology, recommend an
appropriate evaluation, explore the risks and benefits of treatment and
consequences of nontreatment, and determine whether population-based
screening is warranted. DATA SOURCES: MEDLINE, EMBASE, Biosis, the
Agency for Healthcare Research and Quality, National Guideline Clearing
House, the Cochrane Database of Systematic Reviews and Controlled Trials
Register, and several National Health Services (UK) databases were
searched for articles on subclinical thyroid disease published between
1995 and 2002. Articles published before 1995 were recommended by expert
consultants. STUDY SELECTION AND DATA EXTRACTION: A total of 195
English-language or translated papers were reviewed. Editorials,
individual case studies, studies enrolling fewer than 10 patients, and
nonsystematic reviews were excluded. Information related to authorship,
year of publication, number of subjects, study design, and results were
extracted and formed the basis for an evidence report, consisting of
tables and summaries of each subject area. DATA SYNTHESIS: The strength
of the evidence that untreated subclinical thyroid disease is associated
with clinical symptoms and adverse clinical outcomes was assessed and
recommendations for clinical practice developed. Data relating the
progression of subclinical to overt hypothyroidism were rated as good,
but data relating treatment to prevention of progression were inadequate
to determine a treatment benefit. Data relating a serum TSH level higher
than 10 mIU/L to elevations in serum cholesterol were rated as fair but
data relating to benefits of treatment were rated as insufficient. All
other associations of symptoms and benefit of treatment were rated as
insufficient or absent. Data relating a serum TSH concentration lower
than 0.1 mIU/L to the presence of atrial fibrillation and progression to
overt hyperthyroidism were rated as good, but no data supported
treatment to prevent these outcomes. Data relating restoration of the
TSH level to within the reference range with improvements in bone
mineral density were rated as fair. Data addressing all other
associations of subclinical hyperthyroid disease and adverse clinical
outcomes or treatment benefits were rated as insufficient or absent.
Subclinical hypothyroid disease in pregnancy is a special case and
aggressive case finding and treatment in pregnant women can be
justified. CONCLUSIONS: Data supporting associations of subclinical
thyroid disease with symptoms or adverse clinical outcomes or benefits
of treatment are few. The consequences of subclinical thyroid disease
(serum TSH 0.1-0.45 mIU/L or 4.5-10.0 mIU/L) are minimal and we
recommend against routine treatment of patients with TSH levels in these
ranges. There is insufficient evidence to support population-based
screening. Aggressive case finding is appropriate in pregnant women,
women older than 60 years, and others at high risk for thyroid
dysfunction. |
McDermott MT, Woodmansee WW, Haugen BR, Smart
A, Ridgway EC Thyroid 13,1133-39,2004
The management of subclinical
hyperthyroidism by thyroid specialists
ABSTRACT
More experience with recombinant human thyrotropin.
The group from Nijmegen, The Netherlands, who have extensive
experience with RAJ treatment of nodular goiter, now show that pre-treatment
with a low dose rhTSH allows about 50% reduction of the therapeutic RAJ dose
without affecting percentage reduction of thyroid volume, see abstract 1.
The group from Frankfurt, Germany, show that effective half-life
of 131I in patients treated for thyroid carcinoma is shortened when
pre-treated with hrTSH. See abstract 2.
| Abstract 1.
The Journal of Clinical Endocrinology & Metabolism Vol. 88, No. 7
3121-3129
Pretreatment with a Single, Low Dose of Recombinant Human
Thyrotropin Allows Dose Reduction of Radioiodine Therapy in Patients
with Nodular Goiter
Willy-Anne Nieuwlaat, Dyde A. Huysmans, Harrie C. van den Bosch, C. G.
(Fred) Sweep, H. Alec Ross, Frans H. Corstens and Ad R. Hermus
.
In patients with nodular goiter, radioiodine (131I) therapy
results in a mean reduction in thyroid volume (TV) of approximately
40% after 1 yr. We have demonstrated that pretreatment with a single,
low dose of recombinant human TSH (rhTSH) doubles 24-h radioactive
iodine uptake (RAIU) in these patients. We have now studied the safety
and efficacy of therapy with a reduced dose of 131I after pretreatment
with rhTSH.
Twenty-two patients with nodular goiter received 131I therapy, 24 h
after im administration of 0.01 (n = 12) or 0.03 (n = 10) mg rhTSH. In
preceding diagnostic studies using tracer doses of 131I, 24-h RAIU
without and with rhTSH pretreatment (either 0.01 or 0.03 mg) were
compared. Therapeutic doses of 131I were adjusted to the rhTSH-induced
increases in 24-h RAIU and were aimed at 100 µCi/g thyroid tissue
retained at 24 h. Pretreatment with rhTSH allowed dose reduction of
131I therapy by a factor of 1.9 ± 0.5 in the 0.01-mg and by a factor
of 2.4 ± 0.4 in the 0.03-mg rhTSH group (P < 0.05, 0.01 vs. 0.03 mg
rhTSH). Before and 1 yr after therapy, TV and the smallest
cross-sectional area of the tracheal lumen were measured with magnetic
resonance imaging. During the year of follow-up, serum TSH, free T4
(FT4), T3, and TSH receptor antibodies were measured at regular
intervals.
TV before therapy was 143 ± 54 ml in the 0.01-mg group and 103 ± 44 ml
in the 0.03-mg rhTSH group. One year after treatment, TV reduction was
35 ± 14% (0.01 mg rhTSH) and 41 ± 12% (0.03 mg rhTSH). In both groups,
smallest cross-sectional area of the tracheal lumen increased
significantly. In the 0.01-mg rhTSH group, serum FT4 rose, after 131I
treatment, from 15.8 ± 2.8 to 23.2 ± 4.4 pM. In the 0.03-mg rhTSH
group, serum FT4 rose from 15.5 ± 2.5 to 23.5 ± 5.1 pM. Individual
peak FT4 levels, reached between 1 and 28 d after 131I treatment, were
above the normal range in 12 patients. TSH receptor antibodies were
negative in all patients before therapy and became positive in 4
patients. Hyperthyroidism developed in 3 of these 4 patients between
23 and 25 wk after therapy.
In conclusion, in patients with nodular goiter pretreatment with a
single, low dose of rhTSH allowed approximately 50–60% reduction of
the therapeutic dose of radioiodine without compromising the efficacy
of TV reduction.
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| Abstract 2. J Nucl Med 2003 44: 1065-1068
rhTSH Stimulation Before Radioiodine Therapy in Thyroid Cancer Reduces the
Effective Half-Life of 131I
Christian Menzel, MD, PhD, Wolfgang T. Kranert, ScD, Natascha Döbert, MD,
Michaela Diehl, MD, Thomas Fietz, ScD, Nadja Hamscho, MD, Uwe Berner, MD and
Frank Grünwald, MD, PhD
Recombinant human thyroid-stimulating hormone (rhTSH) is effectively used
for exogenous thyroid-stimulating hormone (TSH) stimulation before
diagnostic 131I scintigraphy. It is not yet widely used for preparation of
patients receiving a therapeutic amount of radioiodine.
Methods: The results
of 64 consecutive therapeutic applications of rhTSH with regard to clinical
tolerance and side effects were evaluated in comparison with 163 radioiodine
therapies (RITs) done on patients with hypothyroidism after thyroxine
withdrawal during the same period. All therapies—applying 1.1–10 GBq of
131I—used a standardized protocol of patient preparation and activity
application. RITs were followed by daily whole-body uptake measurements for
2–6 d, and a biexponential curve fit was used to obtain a short initial and
afterward a long effective half-life of 131I. Patients after rhTSH were
evaluated as a whole group (group A, n = 64) and as a subset of that group
with normal thyroglobulin (hTG) levels (group D, n = 18). Patients after
endogenous TSH stimulation were evaluated as a whole group (group B, n =
163), as a subset of that group excluding all ablative RITs (group C, n =
113), and as a subset of that subset with normal hTG levels (group E, n =
87).
Results: rhTSH-stimulated patients showed significantly higher TSH
values than did endogenously stimulated patients (P < 0.001). Furthermore,
the effective half-life of 131I was significantly prolonged after endogenous
stimulation (e.g., 0.43 d for group A vs. 0. 54 d for group B, P < 0.001).
All rhTSH applications were tolerated well and without serious side effects.
The only side effects were 2 cases of nausea and headache.
Conclusion: The
use of rhTSH for stimulation of TSH before RIT is safe but also
significantly reduces the effective half-life of 131I. This is mainly due to
a reduced renal iodine clearance in the hypothyroid state, but the
bioavailability of radioiodine may be slightly overestimated because of
larger amounts of intestinal 131I after endogenous TSH stimulation.
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WAIT AND SEE FOR PAPILLARY MICROCARCINOMA?
Treatment of thyroid papillary carcinoma's less than 10 mm in diameter
(termed papillary microcarcinoma, formerly occult carcinoma) is being
debated increasingly. Since the introduction of the ultrasound in
medicine, imaging of the thyroid is frequently performed and is
sufficiently sensitive to detect nodules of > 3 mm in diameter. It has
been known for a long time that in routine autopsy of the thyroid,
microcarcinoma's of the papillary type are frequently found. Thus, Fukanga
and Yatani (Cancer 36: 1095-9,1975) report a worldwide geographical
variation in frequency of these tumours between 5% and 24%. Many of these
tumours seem to be biologically inactive and hence the controversy about
the treatment if such nodules are "accidentally" detected.
Yashiro et al, (Thyroid 13:381-387, 2003) now
report that patients with papillary microcarcinoma's may choose between
surgical treatment or observation, even if these tumours are multifocal
and/or involve lymph nodes, as they rarely become clinically apparent.
ABSTRACT:
FUTURE USE OF CYTO-GENETICS IN THE DIAGNOSIS OF
PAPILLARY THYROID CARCINOMA?
An activating
mutation in the BRAF gene has found to be associated with the majority of
papillary thyroid cancers (69%), according to a report in the Journal of
the National Cancer Institute (abstract see below).The
BRAF gene product activates the mitogen-activated protein kinase (MAPK)
pathway, resulting in abnormal proliferation and differentiation in many
human cancers, the authors explain. BRAF has previously been shown to be
activated in 80% of malignant melanoma tumors and in colon carcinoma. The
authors screened for the common BRAF T1796A mutation in over 300 cancer
specimens -- 214 lung, 126 head and neck, 54 thyroid, 27 bladder, 38
cervical, and 17 prostate cancers.
Twenty-four of 35 (69%) papillary thyroid
carcinomas contained the BRAF mutation, the authors report. In contrast,
no BRAF mutations were identified in samples from 13 patients with
follicular thyroid carcinoma, three patients with medullary thyroid
carcinoma, three patients with Hurthle cell carcinoma, or 20 patients with
benign thyroid conditions.
ABSTRACT
BRAF
Mutation in Papillary Thyroid Carcinoma
. Yoram Cohen, Mingzhao Xing,
Elizabeth Mambo, Zhongmin Guo, Guogun Wu, Barry Trink, Uziel Beller,
William H. Westra, Paul W. Ladenson, David Sidransky , J Natl Cancer Inst
95:625-627,2003.
The BRAF gene has been found to be activated by mutation in human
cancers, predominantly in malignant melanoma. We tested 476
primary tumors, including 214 lung, 126 head and neck, 54 thyroid,
27 bladder, 38 cervical, and 17 prostate cancers, for the BRAF
T1796A mutation by polymerase chain reaction (PCR)–restriction enzyme
analysis of BRAF exon 15. In 24 (69%) of the 35 papillary thyroid
carcinomas examined, we found a missense thymine (T) adenine
(A) transversion at nucleotide 1796 in the BRAF gene (T1796A). The
T1796A mutation was detected in four lung cancers and in six
head and neck cancers but not in bladder, cervical, or prostate cancers.
Our data suggest that activating BRAF mutations may be an
important event in the development of papillary thyroid cancer.
OVEREXPRESIION OF DEIODINASES
IN TUMOROUS TISSUES
B. W. Kim, et al, J Clin
Endocrinol Metab, 88,594-598,2003, describe 3 patients with follicular
thyroid carcinoma and elevated plasma T3 to T4 ratio, due to
overexpression of type II deiodinase in carcinomatous tissue, leading to
increased T4 to T3 conversion ( see abstract below).
The same group published ( NEJM 343,185-189,2000) overt
hypothyroidism in infants with massive haemangiomas due to increased
expression of type III deiodinase in these tissues, resulting
accelerated inactivation of thyroid hormone for which the infants thyroid
could not compensate.
It would be interesting to study plasma T3/T4 ratios in patients with
different tumors to study further the phenomenon of overexpression of
deiodinases affecting the thyroid hormone profile.
Abstract
Thyroid function is normally undisturbed in patients
with thyroid carcinoma. We have identified three patients with
large or widely metastatic follicular thyroid carcinoma who had
a persistently increased ratio of serum T3 to T4
in the absence of autonomous production of T3 by the
tumor. To investigate the possibility of tumor-mediated T4
to T3 conversion, we assayed types 1 and 2
iodothyronine selenodeiodinase (D1 and D2) activity in a 965-g follicular
thyroid carcinoma resected from one of these patients. The Vmax
for D2 was 8-fold higher than in normal human thyroid tissue.
Resection of this tumor, leaving the left thyroid lobe intact,
normalized the serum T3 to T4 ratio. In two other
patients, treatment with sufficient levothyroxine to suppress
TSH was associated with a high normal T3 and a
subnormal free T4 index. In one, concomitant
administration of the D1 inhibitors, propylthiouracil and
propranolol, did not decrease the elevated serum T3 to T4
ratio. These data illustrate that increased T4 to T3
conversion in follicular thyroid carcinomas, probably by D2,
can cause a significant perturbation in peripheral thyroid
hormone concentrations.
An hitherto un-recognized side
effect of 131I
treatment
Nasolacrimal Drainage System
Obstruction from Radioactive Iodine Therapy for Thyroid Carcinoma
Richard T.
Kloos, Vani Duvuuri, Sissy M. Jhiang, Kenneth V. Cahill, Jill A. Foster
and John A. Burns
Abstract-Ophthalmic complications of 131I
therapy, including ocular dryness, have been recently
investigated and described. However, nasolacrimal drainage
system obstruction (NDSO), complicating 131I therapy, has
not been previously well appreciated or characterized. One of
our patients developed bilateral complete nasolacrimal duct obstruction
after 131I therapy that prompted awareness of this potential
complication. Over 16 months, 423 patients with epithelial-derived thyroid
cancer were provided routine clinical care; 390 of these patients
had received 131I ablation or therapy, and 10 patients subsequently
reported epiphora. All had evidence of NDSO disease after a
mean cumulative 131I dose of 17,279 ± 2,923 MBq (467
± 79 mCi), with a mean individual 131I dose of 6,660 ±
555 MBq (180 ± 15 mCi). Symptoms appeared 6.5 ± 1.4 (range,
3–16) months after the last 131I dose, whereas the
mean time from symptom onset to correct diagnosis was 18 ± 5
months. A causal relationship between 131I administration
and NDSO is strongly suspected. Patients reporting epiphora
should be evaluated promptly by an oculoplastic surgeon.
L-T4
substitution revisited.
(1 Nov 02)
There is growing interest if not concern amongst thyroidologists about the
way we substitute for thyroid failure. The standard treatment consist of
L-T4 substitution in a dose that normalizes serum TSH. The question
however is if this regimen is still correct. In this respect there are
several points that have to be discussed.
- Organs
depend differently for T3-nuclear occupancy on T3 extracted form the
plasma and T3 that is locally produced from T4. In hypothyroid rats all
organs are in a euthyroid state only
if the serum T4/T3 ratio is kept normal by subcutaneous
administration of T4/T3 in an amount and ratio as produced by the
intact thyroid (Escobar-Morreale
HF, et al. Endocrinology 1996; 137: 2490-2502.) As thyroid
hormone metabolism and action in humans and rats is similar in many
aspects, this phenomenon may also be true man. Substitution of thyroid
function in hypothyroid patients using T4 only, results in an elevated
T4/T3 serum ratio, because the thyroidal contribution to plasma T3 is
lacking. Bunevicius
R, et al (New Engl J Med 1999; 340: 424-29.) reported that in
hypothyroid subjects when substituted with a combination of T4 and T3,
cognitive function was better than when treated with T4 only. Alevizaki
et al, (see: Abstracts ETA, 2002: www.hotthyroidology.com
or J Endocrinol Invest, 25, suppl to 7, 77, 2002) demonstrate that
substitution with T4 only, such that serum TSH is normal, results in
serum T3 and SHBG concentrations that are lowered, suggesting
hypothyroidism at the level of the liver.
However A Levitt and J Silverberg reported at the American
Thyroid Assoc. annual meeting (Program, Annual Meeting, p.112, Oct
10-13, 2002)
that T4 alone, or T4 plus T3 in 15/1 ratio given twice daily,
were overall equivalent
in a double blind 3-6 month evaluation.
- There
are recent suggestions that we have to re-define the normal serum TSH
range.
Thus Spencer
et al, (see: Abstracts ATA 2002,
www.thyroid.org or Program
and Abstracts 74th Annual Meeting ATA, 2002, p 111.) suggest a
range between 0.4 and 2.0 mU/L, as values >2.0 mU/l may represent early
hypothyroidism. Others advise an optimal “normal” TSH range of 0.4 to
1.5 mU/L for patients substituted with T4 only.
In
summary the questions are 1)
if we should narrow the normal range for serum TSH to 0.4 and 2.0 mU/L and
2)
if substitution with L-T4 only is adequate or should be effected with a
combination preparation of T4 plus T3?
In a sense complementary to the study of Bunevicius
R, et al ( see above), Saravan
et al abstract see below, report
that
“ patients on thyroxine replacement even with a normal TSH display
significant impairment in psychological well-being compared to
controls”.
The point seems to be if the apparent
cognitive impairments detected in subjects on L-T4 substitution are due to
incorrect adjustment of serum TSH and or absent
T3 in the substitution preparation.
ABSTRACT:
Psychological well-being in patients on 'adequate' doses of l-thyroxine:
results of a large, controlled community-based questionnaire study.
Saravanan P, Chau WF, Roberts N, Vedhara K, Greenwood R, Dayan CM. Clin
Endocrinol (Oxf) 57:663-586,2002
OBJECTIVE: Over 1% of the UK population is receiving thyroid hormone
replacement with l-thyroxine (T4). However, many patients complain of
persistent lethargy and related symptoms on T4 even with normal TSH
levels. To date there has been no large study to determine whether this is
related to thyroxine replacement or coincidental psychological morbidity.
We have therefore attempted to address this issue using a large,
community-based study. DESIGN AND PATIENTS: Computerized prescribing
records of five general practices were used to identify 961 patients who
had been on thyroxine for a minimum of 4 months from a population of 63
000 (1.5%), along with age- and sex-matched controls. All 1922 individuals
were sent a two-page questionnaire, made up of the short form of the
General Health Questionnaire (GHQ-12), designed to detect minor
psychiatric disorders in the community, and a 12-question 'thyroid symptom
questionnaire' (TSQ) in the same format. A covering letter explained that
we were interested in 'how patients felt on medication' and made no direct
reference to thyroxine. MEASUREMENTS: Scores from the GHQ and TSQ were
marked for each individual using the GHQ and Likert scoring methods.
Patients' latest TSH measurements were obtained from laboratory records.
Comparisons were then made on scores for the total GHQ-12, TSQ and
individual questions between patients (P) and control (C) groups. Separate
analyses were made comparing the patients with a normal TSH (nP) and the
control group. RESULTS: Five hundred and ninety-seven (62%) of the
patients (P) and 551 (57%) of the controls (C) responded and fully
completed at least one of the two questionnaire. Three hundred and
ninety-seven responding patients (nP) had a TSH estimation performed in
the previous 12 months with the last result being in the local laboratory
normal range for TSH (0.1-5.5 or 0.2-6.0 mU/l, according to the assay
method used). The responding P, nP and C populations were well matched for
age (59.96, 59.73, 59.35 years) and sex (85%, 83%, 87% female). The number
of individuals scoring 3 or more on the GHQ-12 (indicating 'caseness') was
21% higher in P than C [185/572 (32.3%) vs. 137/535 (25.6%), P = 0.014]
and 26% higher in nP than C [131/381 (34.4%) vs. 137/535 (25.6%), P <
0.005]. Stronger differences were seen with the TSQ scores [C = 187/535
(35.0%), P = 273/583 (46.8%), P < 0.001, P vs. C; and nP = 189/381
(48.6%), P < 0.001, nP vs. C]. Differences existed in chronic drug use
and chronic disease prevalence between the control and patient groups, but
the differences in GHQ and TSQ scores between the groups remained
significant even after correction for these factors as well as age and sex
in multiple regression analysis. CONCLUSIONS: This community-based study
is the first evidence to indicate that patients on thyroxine replacement
even with a normal TSH display significant impairment in psychological
well-being compared to controls of similar age and sex. In view of the
large numbers of people on thyroxine replacement, we believe that these
differences, although not large, could contribute to significant
psychological morbidity in a substantial number of individuals.
September
2002
In 1998, Zelmanovitz et al (JCEM 83,3881,1998)
published the results of a cumulative meta-analysis (risk-difference
method) of studies assessing the effect of TSH suppression by T4 on the
volume of benign solitary thyroid nodules. Altogether 7 studies were
included in this meta-analysis. These studies met the following criteria:
prospective, controlled clinical trials with a sufficient dose
of T4 for TSH suppression, minimum follow-up of 6 months, and
nodule volume monitored by ultrasonography. They
concluded that T4 treatment would decrease nodule volume by more than 50%
in only 17% of patients and inhibit growth in a further 10%.
In a recent study by an other group, abstract
see below, a similar analysis was done using the same criteria. In
total, 7 studies were included, of which 5 were also included in the
analysis mentioned above. From the results of this
study the authors could not find a significant reduction in nodule volume.
COMMENT
It seems that it is reasonable to conclude that, although a great many
studies have entered the literature that are concerned with the effect of
TSH suppression on benign nodule volume, only a few can withstand
scientific criteria. From these few studies, in total 9, no important
effect could be found from TSH suppression on benign nodule volume. In the
opinion of the writer, Dr Georg Henneman, there is no place for
routine, TSH suppression in such patients, considering the lack of an
important effect and the risks of T4 suppressive therapy on bones and
heart.
Nevertheless, opinion (L De Groot,MD) remains divided. Many physicians advise treatment to
place TSH at the bottom of the normal range, considering 1) that in the
first study quoted 27% were found to have a positive effect after as short
a time as 6 months, 2) that long term treatment may help prevent
enlargement if not causing shrinkage, 3) the treatment may help prevent
development of other nodules, and 4) treatment can be carried out without
significant risk to the patient.
Abstract:M. Regina Castro, Pedro J. Caraballo and John C. Morris. Effectiveness of Thyroid
Hormone Suppressive Therapy in Benign Solitary Thyroid Nodules: A
Meta-Analysis. Journal of Clinical
Endocrinology and Metabolism
The effectiveness of thyroid hormone suppressive therapy in reducing
the volume of benign thyroid nodules is controversial. It is
important to clarify this therapeutic effect of thyroid hormone,
because its prolonged use needs to be carefully weighed against
its potential deleterious effects in the skeletal and cardiovascular
systems. To evaluate the best available evidence, we conducted
a systematic review and meta-analysis of the randomized controlled
trials that fulfill the following inclusion criteria: single
thyroid nodules proven benign by fine needle aspiration, treatment,
and follow-up of at least 6 months; documented suppression of
TSH; measurement of thyroid nodule volume by ultrasound; and
response to therapy defined as more than 50% volume reduction from
baseline. Six randomized clinical trials published between 1987
and 1999, with 346 patients, were included in the meta-analysis. Ninety
percent of the participants were female. Using a random effects
model, the overall effect size showed a relative risk of 1.9
(95% confidence interval, 0.95–3.81) favoring a treatment
effect. A sensitivity analysis showed significant changes in
the results.
Suppressive thyroid hormone therapy for longer than 6 months is
associated with a trend toward a reduction of more than 50% in
volume of benign thyroid nodules, without achieving statistical significance.
The results are highly sensitive to changes in the statistical
analysis, especially if the method used ignores heterogeneity
among the effect sizes. More studies are needed before this
therapy can be widely recommended.
SUPPRESSIVE THERAPY WITH LEVOTHYROXINE FOR SOLITARY THYROID
NODULES: A DOUBLE-BLIND
CONTROLLED CLINICAL STUDY AND CUMULATIVE META-ANALYSIS
Flavio Zelmanovitz, Sandra Genro, and
Jorge L. Gross(J. Clin. Endocrinol. Metab.
83:3881-3885, 1998.)
Levothyroxine suppressive treatment of solitary thyroid nodules is
controversial. A one year
prospective randomized placebo-controlled trial was conducted to evaluate
the effect of T4
on nodule volume and bone mineral density, and
meta-analyses were performed to examine the quantitative synthesis of data
from similar designed controlled trials.
Forty-five euthyroid patients (42 females, age range: 19-73 yr)
with single, colloid nodules were randomized to T4 (21 patients, 2.7 " 0.3 Fg/kg, TSH < 0.3 FIU/ml) and placebo. Ultrasonography and densitometry were performed at baseline
and repeated after treatment. Mean
nodule volume or bone mineral density did not change.
Nodule reduction more than 50% was observed in 6 of 21 treated
patients and 2 of 24 placebo patients (P = 0.12).
This study and another 6 prospective controlled trials (minimum 6
months, ultrasonographic nodule evaluation) were included in cumulative
meta-analyses (risk-difference method).
Nodule volume decreased more than 50% in a significantly higher
percentage of patients in the T4 groups (risk difference, 16.7%; 95% confidence intervals, 5.8
– 27.6%). Four trials
evaluated nodule growth with homogeneous results (Q = 0.42).
Nodule volume increased more than 50% in a significantly smaller
percentage of patients treated with T4 (risk difference, 9.7%; 95% confidence intervals, 2.0-17.4%).
In conclusion, T4 treatment is associated with decreased
nodule volume in 17% of patients and may inhibit growth in another 10%.
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