Human Leptin Deficiency Caused by a Missense Mutation: Multiple Endocrine Defects, Decreased Sympathetic Tone, and Immune System Dysfunction Indicate New Targets for Leptin Action, Greater Central than Peripheral Resistance to the Effects of Leptin, and Spontaneous Correction of Leptin-Mediated Defects
We have previously demonstrated that genetically based leptin deficiency due to a missense leptin gene mutation in a highly consanguineous extended Turkish pedigree is associated with morbid obesity and hypogonadism. We have now performed detailed assessments of endocrine, sympathetic, and immune fu...
Gespeichert in:
Veröffentlicht in: | The journal of clinical endocrinology and metabolism 1999-10, Vol.84 (10), p.3686-3695 |
---|---|
Hauptverfasser: | , , |
Format: | Artikel |
Sprache: | eng |
Online-Zugang: | Volltext |
Tags: |
Tag hinzufügen
Keine Tags, Fügen Sie den ersten Tag hinzu!
|
Zusammenfassung: | We have previously demonstrated that genetically based leptin
deficiency due to a missense leptin gene mutation in a highly
consanguineous extended Turkish pedigree is associated with morbid
obesity and hypogonadism. We have now performed detailed assessments of
endocrine, sympathetic, and immune function. We have also identified a
new adult female homozygous patient in this extended family who is
severely obese and amenorrheic. In this family all wild-type and
heterozygous individuals have normal body weight. Seven obese members
of this family, whom we presume to have been leptin deficient, died
during childhood. There are several findings that indicate potentially
novel targets for leptin action in humans. Four homozygous patients (1
adult male, 2 adult females, and 1 child) have sympathetic system
dysfunction, whereas all heterozygous subjects have normal sympathetic
system function. Despite sympathetic system dysfunction and postural
hypotension, 1 of 3 homozygous adult patients has impaired
renin-aldosterone function. The patients also exhibit alterations in GH
and PTH-calcium function, and 1 of them has decreased bone mineral
density. Despite their obesity, these patients do not have risk factors
for cardiovascular disease, such as hypertension, impairments in lipid
metabolism, or hyperglycemia. These data support the hypothesis that
the obese may have central, but not peripheral, resistance to the
effects of leptin and that hyperglycemia may mediate the cardiovascular
morbidity of the obese who are not leptin deficient. Furthermore, these
data indicate that there may be several new targets for leptin action
in human physiology. Such new targets may lead to novel pharmacological
strategies for the use of leptin agonists and antagonists in the
treatment of human disease. All 19 normal weight individuals in this
family are alive, whereas 7 of 11 obese individuals died in childhood
after infections. The odds ratio for mortality in the context of this
obesity phenotype is 25.4, indicating that this mutation severely
impairs key biological functions during childhood, negatively impacting
on survival. We found that only the obese child in this family had
thyroid function abnormalities. The oldest homozygous female patient
started to menstruate, albeit with a luteal phase defect, 7 months ago,
after a delay of over 20 yr, whereas the younger adult subjects are
still hypogonadic. Thus, we conclude that due to their long life span,
humans who survive the nega |
---|---|
ISSN: | 0021-972X 1945-7197 |
DOI: | 10.1210/jcem.84.10.5999 |