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Query: UMLS:C0014848 (
achalasia
)
2,804
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The primary pathophysiologic abnormality in
achalasia
is loss of intrinsic inhibitory innervation of the lower esophageal sphincter and smooth muscle segment of the esophageal body. Disease of the extrinsic (vagal) nervous system and esophageal musculature may also be present, but these are less consistent findings and could represent secondary phenomena. Inflammation within the esophageal myenteric plexus is pathognomonic of the disease, but the cause of this inflammation is uncertain. Autoimmunity and previous
viral infection
have been hypothesized, but remain unproven.
...
PMID:Etiology and pathogenesis of achalasia. 1131 60
Idiopathic
achalasia
is an inflammatory disease of unknown etiology characterized by esophageal aperistalsis and failure of LES relaxation due to loss of inhibitory nitrinergic neurons in the esophageal myenteric plexus. Proposed causes of
achalasia
include gastroesophageal junction obstruction, neuronal degeneration,
viral infection
, genetic inheritance, and autoimmune disease. Current evidence suggests that the initial insult to the esophagus, perhaps a
viral infection
or some other environmental factor, results in myenteric plexus inflammation. The inflammation then leads to an autoimmune response in a susceptible population who may be genetically predisposed. Subsequently, chronic inflammation leads to destruction of the inhibitory myenteric ganglion cells resulting in the clinical syndrome of idiopathic
achalasia
. Further studies are needed to better understand the etiology and pathogenesis of
achalasia
-such an understanding will be important in developing safe, effective, and possibly curative therapy for
achalasia
.
...
PMID:Etiology and pathogenesis of achalasia: the current understanding. 1640 59
Achalasia
cardia is one of the common causes of motor dysphagia. Though the disease was first described more than 300 years ago, exact pathogenesis of this condition still remains enigmatic. Pathophysiologically,
achalasia
cardia is caused by loss of inhibitory ganglion in the myenteric plexus of the esophagus. In the initial stage, degeneration of inhibitory nerves in the esophagus results in unopposed action of excitatory neurotransmitters such as acetylcholine, resulting in high amplitude non-peristaltic contractions (vigorous
achalasia
); progressive loss of cholinergic neurons over time results in dilation and low amplitude simultaneous contractions in the esophageal body (classic
achalasia
). Since the initial description, several studies have attempted to explore initiating agents that may cause the disease, such as
viral infection
, other environmental factors, autoimmunity, and genetic factors. Though Chagas disease, which mimics
achalasia
, is caused by an infective agent, available evidence suggests that infection may not be an independent cause of primary
achalasia
. A genetic basis for
achalasia
is supported by reports showing occurrence of disease in monozygotic twins, siblings and other first-degree relatives and occurrence in association with other genetic diseases such as Down's syndrome and Parkinson's disease. Polymorphisms in genes encoding for nitric oxide synthase, receptors for vasoactive intestinal peptide, interleukin 23 and the ALADIN gene have been reported. However, studies on larger numbers of patients and controls from different ethnic groups are needed before definite conclusions can be obtained. Currently, the disease is believed to be multi-factorial, with autoimmune mechanisms triggered by infection in a genetically predisposed individual leading to degeneration of inhibitory ganglia in the wall of the esophagus.
...
PMID:Pathogenesis of achalasia cardia. 2279 40
Achalasia
is a rare motility disorder of the oesophagus characterised by loss of enteric neurons leading to absence of peristalsis and impaired relaxation of the lower oesophageal sphincter. Although its cause remains largely unknown, ganglionitis resulting from an aberrant immune response triggered by a
viral infection
has been proposed to underlie the loss of oesophageal neurons, particularly in genetically susceptible individuals. The subsequent stasis of ingested food not only leads to symptoms of dysphagia, regurgitation, chest pain, and weight loss, but also results in an increased risk of oesophageal carcinoma. At present, pneumatic dilatation and Heller myotomy combined with an anti-reflux procedure are the treatments of choice and have comparable success rates. Per-oral endoscopic myotomy has recently been introduced as a new minimally invasive treatment for
achalasia
, but there have not yet been any randomised clinical trials comparing this option with pneumatic dilatation and Heller myotomy.
...
PMID:Achalasia. 2387 Oct 90
Achalasia
is defined by esophageal outflow obstruction from abnormal relaxation of the lower esophageal sphincter (LES) due to deranged inhibitory control. In genetically predisposed individuals, an autoimmune response to an unknown inciting agent, perhaps a
viral infection
, results in inflammation and sometimes loss of myenteric plexus ganglia and neurons. The net result is varying degrees of inhibitory dysfunction, at times associated with imbalanced and exaggerated excitatory function, with manometrically distinct
achalasia
phenotypes on high resolution manometry. There is new evidence in the current issue of this Journal suggesting that type 1
achalasia
, with esophageal outflow obstruction and absent esophageal body contractility, is an end-stage phenotype from progression of type 2
achalasia
, which is characterized by panesophageal compartmentalization of pressure in the untreated patient, and partial recovery of peristalsis after treatment. Esophageal outflow obstruction with premature peristalsis (type 3
achalasia
) or intact peristalsis may result from plexitis in the myenteric plexus but can also be encountered in other settings including chronic opioid medication usage and structural processes at the esophagogastric junction and distally. In most instances when idiopathic esophageal outflow obstruction is confirmed, some form of pharmacologic manipulation or disruption of the LES provides durable symptom relief. This review will focus on current understanding of pathophysiology, diagnosis, and principles of management of
achalasia
in light of emerging literature on the topic.
...
PMID:Achalasia: new perspectives on an old disease. 2669 Aug 70
BACKGROUND
Achalasia
, as an incurable disease is defined by the lack of normal esophageal peristalsis and loss of lower esophageal sphincter relaxation due to impaired myenteric neural plexus. The exact cause of myenteric neural cells degeneration in
achalasia
is still unknown. One hypothesis is that certain neurotropic viruses and autoimmune factors cause the inflammatory response in myenteric network, which consequently destroy neural cells. This study was designed to find the evidence of viral causes of
achalasia
. METHODS In this case-control study, 52 patients with
achalasia
and 50 controls referred to Shariati Hospital, were evaluated for the genome of neurotropic viruses, HPV, and adenovirus by polymerase chain reaction (PCR) and reverse transcription (RT) PCR techniques. RESULTS Genome assessment of neurotropic DNA viruses turned out negative in the patients, however, the genome of HSV-1 (Herpes simplex virus) was found in tissues of six controls. No neurotropic RNA viruses were observed in the tissue samples and whole blood of both the patients and controls. Among non-neurotropic viruses, adenovirus genome was positive in tissues of two out of 52 patients and three out of 50 controls. In addition, one out of 52 patients and two out of 50 controls were positive for HPV infection in tissues. CONCLUSION We could not detect any significant relationship between
achalasia
and HPV, adenovirus, and neurotropic viruses in the cases. Nevertheless, it does not exclude the hypothesis of either an alternate viral species or resolved
viral infection
as the etiology of
achalasia
.
...
PMID:Is There Any Evidence for a Viral Cause in Achalasia? 3018 80
