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Query: UMLS:C0004352 (
autism
)
32,579
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
RG-1068 is a synthetic form of the natural human hormone
secretin
under development by RepliGen for the potential treatment of
autism
. RG-1068 received Fast Track designation for the treatment of pediatric
autism
in September 2001, and in February 2002, it entered phase III clinical trials.
...
PMID:RG-1068 RepliGen. 1262 32
In a subgroup of children with
autism
-spectrum like conditions symptoms seem to appear as a 'regression' (in normal development). It has been postulated that the onset of such autistic symptoms may involve an autoimmune response against the central nervous system and that the antigenic determinant could possibly be gastrointestinal in origin. It has been suggested that the presence of the measles virus and 'autistic enterocolitis' demonstrates the possibility that the MMR triple vaccine may be mediating the inflammation with possible production of antibodies against the virus containing vaccine. Such an antibody may share antigenic determinant to molecules found in the gut. We propose that this may be
secretin
or its receptor, found in the gut as well as in the central nervous system. The antibody response to the gut may also conceivably occur in the brain at a critical time in development. The modulation of development by
secretin
may be a static event possibly occurring at a specific time in early childhood development and if it involves an autoimmune response then a disruption in development may result. These hypothesized events can only occur if the MMR vaccine shares antigenic determinants that resemble
secretin
or any of its receptor types and remains to be studied.
...
PMID:Does the MMR vaccine and secretin or its receptor share an antigenic epitope? 1271 Aug 97
The recent suggestion that
secretin
may be useful in treating
autism
and schizophrenia has begun to focus attention on the mechanisms underlying this gut-brain peptide's actions in the central nervous system (CNS). In vitro autoradiographic localization of (125)I-
secretin
binding sites in rat brain shows the highest binding density in the nucleus tractus solitarius (NTS). Recent evidence suggests that intravenous infusion of
secretin
causes fos activation in NTS, a relay station playing important roles in the central regulation of autonomic functions. In this study, whole cell patch-clamp recordings were obtained from 127 NTS neurons in rat medullary slices. The mean resting membrane potential of these neurons was -54.7 +/- 0.3 mV, the mean input resistance was 3.7 +/- 0.2 GOmega, and the action potential amplitude of these neurons was always >70 mV. Current-clamp studies showed that bath application of
secretin
depolarized the majority (80.8%; 42/52) of NTS neurons tested, whereas the remaining cells were either unaffected (17.3%; 9/52) or hyperpolarized (1.9%; 1/52). These depolarizing effects were maintained in the presence of 5 microM TTX and found to be concentration dependent from 10(-12) to 10(-7) M. Using voltage-clamp techniques, we also identified modulatory actions of
secretin
on specific ion channels. Our results demonstrate that while
secretin
is without effect on net whole cell potassium currents, it activates a nonselective cationic conductance (NSCC). These results show that NTS neurons are activated by
secretin
as a consequence of activation of a NSCC and support the emerging view that
secretin
can act as a neuropeptide within the CNS.
...
PMID:Secretin depolarizes nucleus tractus solitarius neurons through activation of a nonselective cationic conductance. 1471 95
Autism
is a complex neurological disorder that severely impacts a child's ability to communicate and interact socially. Many treatments have attempted to alleviate the symptoms of
autism
, but with limited success. After reports of improvements in autistic children who received
secretin
, this hormone became popular as a possible treatment for
autism
. Since then, the interest in
secretin
has greatly increased, as well as the demand for
secretin
by parents of autistic children. However, there is still limited experimental evidence that supports its effectiveness. Many biological studies and clinical trials were conducted to test the effectiveness of
secretin
in treating
autism
. This review discusses the autistic disorder, instruments used in the trials, and reports the findings of some of these studies.
...
PMID:The effectiveness of secretin in the management of autism. 1499 34
There are specific challenges to studying the design of pharmacologic trials in child/adolescent and adult
autism
, such as subject stratification and parallel versus crossover designs. This article describes how optimal study design is influenced by subject selection and outcome measures chosen. Lessons learned in study design from the Research Units on Pediatric Psychopharmacology
Autism
Network trial with risperidone, Seaver Center trials with fluoxetine and valproate, Dartmouth trials with amantadine, and National Institutes of Health
secretin
trials are highlighted. The Internet System for Assessing Autistic Children system for managing multicenter clinical trials in
autism
and statistical issues in
autism
research are also described.
...
PMID:Impact of recent findings on study design of future autism clinical trials. 1499 75
In preliminary uncontrolled studies, intravenous injection of the gastrointestinal peptide
secretin
produced improvements in the symptoms of
autism
. Because of the phenotypic overlap between
autism
and some aspects of schizophrenia, we performed a pilot study of
secretin
for treatment refractory schizophrenia. Twenty-two patients were randomized to a single intravenous dose of porcine
secretin
or placebo. Patients were evaluated with the Positive and Negative Symptom Scale for Schizophrenia (PANSS) and the Clinical Global Impression Scale (CGI) at baseline, 2 days after
secretin
infusion and weekly for 4 weeks. There were no statistically significant differences between drug- and placebo-treated patients with repeated measures analysis of variance (ANOVA). However, several patients treated with
secretin
experienced clinically meaningful, but transient, reductions in symptoms and a greater percentage of patients treated with
secretin
were rated as improved with the CGI. Further study of brain hypocretins and molecules affecting this system are warranted in schizophrenia.
...
PMID:Secretin for refractory schizophrenia. 1506 Dec 51
Secretin
, a gastrointestinal (GI) peptide, may offer therapeutic benefit in
autism
. Autistic features can also be present in schizophrenia and a recent study suggested a role for adjunctive
secretin
in treatment-resistant schizophrenia. The current report describes one patient with undifferentiated schizophrenia and prominent autistic features who received a single dose of
secretin
and demonstrated substantial yet transient improvement. The case illustrates the potential role of
secretin
as a novel adjunctive treatment strategy in schizophrenic patients with autistic features.
...
PMID:Secretin in a patient with treatment-resistant schizophrenia and prominent autistic features. 1506 Dec 52
In recent years, VIP/PACAP/
secretin
family has special interest. Family members are vasoactive intestinal peptide (VIP), pituitary adenylate cyclase-activating polypeptide (PACAP),
secretin
, glucagon, glucagon like peptide-1 (GLP(1)), GLP(2), gastric inhibitory peptide (GIP), growth hormone releasing hormone (GHRH or GRF), and peptide histidine methionine (PHM). Most of the family members present both in central nervous system (CNS) and in various peripheral tissues. The family members that are released into blood from periphery, especially gut, circulate the brain and they can cross the blood brain barrier. On the other hand, some of the members of this family that present in the brain, can cross from brain to blood and reach the peripheral targets. VIP,
secretin
, GLP(1), and PACAP 27 are transported into the brain by transmembrane diffusion, a non-saturable mechanism. However, uptake of PACAP 38 into the brain is saturable mechanism. While there is no report for the passage of GIP, GLP(2), and PHM, there is only one report that shows, glucagon and GHRH can cross the BBB. The passage of VIP/PACAP/
secretin
family members opens up new horizon for understanding of CNS effects of peripherally administrated peptides. There is much hope that those peptides may prove to be useful in the treatment of serious neurological diseases such as Alzheimer's disease, amyotropic lateral sclerosis, Parkinson's disease, AIDS related neuropathy, diabetic neuropathy,
autism
, stroke and nerve injury. Their benefits in various pathophysiologic conditions undoubtly motivate the development of a novel drug design for future therapeutics.
...
PMID:Passage of VIP/PACAP/secretin family across the blood-brain barrier: therapeutic effects. 1513 84
1. This study aims (1) to determine whether
secretin
is synthesized centrally, specifically by the HPA axis and (2) to discuss, on the basis of the findings in this and previous studies,
secretin
's possible neuroregulatory role in
autism
. 2. An immunocytochemical technique with single-cell resolution was performed in 12 age/weight-matched male rats pretreated with stereotaxic microinjection of colchicine (0.6 microg/kg) or vehicle into the lateral ventricle. Following 2-day survival, rats were anesthetized and perfused for immunocytochemistry. Brain segments were blocked and alternate frozen 30-microm sections incubated in rabbit antibodies against
secretin
, vasoactive intestinal peptide, glucagon, or pituitary-adenylate-cyclase-activating peptide. Adjacent sections were processed for Nissl stain. Preadsorption studies were performed with members of the
secretin
peptide family to demonstrate primary antibody specificity. 3. Specificity of
secretin
immunoreactivity (ir) was verified by clear-cut preadsorption control data and relatively high concentrations and distinct topographic localization of
secretin
ir to paraventricular/supraoptic and intercalated hypothalamic nuclei.
Secretin
levels were upregulated by colchicine, an exemplar of homeostatic stressors, as compared with low constitutive expression in untreated rats. 4. This study provides the first direct immunocytochemical demonstration of secretinergic immunoreactivity in the forebrain and offers evidence that the hypothalamus, like the gut, is capable of synthesizing
secretin
.
Secretin
's dual expression by gut and brain
secretin
cells, as well as its overlapping central distribution with other stress-adaptation neurohormones, especially oxytocin, indicates that it is stress-sensitive. A neuroregulatory relationship between the peripheral and central stress response systems is suggested, as is a dual role for
secretin
in conditioning both of those stress-adaptation systems. Colchicine-induced upregulation of
secretin
indicates that
secretin
may be synthesized on demand in response to stress, a possible mechanism of action that may underlie
secretin
's role in
autism
.
...
PMID:Secretin: hypothalamic distribution and hypothesized neuroregulatory role in autism. 1517 37
In 1998, Horvath et al. (1998) observed a marked improvement in speech, eye contact, and attention in autistic children five weeks after treatment with
secretin
, which ocurred in the course of an endoscopic investigation. Since
autism
is hypothesized to be a hypoglutamatergic disorder we investigated the in vivo effects of
secretin
on extracellular amino acids in the rat brain. Studies were carried out on freely moving rats with microdialysis probes in the hippocampus. Amino acids were examined using tandem mass spectroscopy and HPLC/fluorometric detection. Following
secretin
injection (8.7 microg/kg i.p.), considerable increases in microdialysate glutamate and gamma-aminobutyric acid (GABA) levels were observed; other amino acids were not affected. The observed increased microdialysate concentrations of glutamate and GABA following
secretin
application may explain the results of the Horvath study.
...
PMID:Effects of secretin on extracellular amino acid concentrations in rat hippocampus. 1520 7
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