New insights into the pathophysiology of achalasia and implications for future treatment

Furuzawa‐Carballeda, Janette; Torres-Landa, Samuel; Valdovinos, Miguel A.; Coss‐Adame, Enrique; Campo, Luis A. Martin Del; Torres‐Villalobos, Gonzalo

doi:10.3748/wjg.v22.i35.7892

Cited by 83 publications

(105 citation statements)

References 94 publications

(163 reference statements)

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“…In humans, esophageal motility disorders are better classified allowing for identification of patients with conditions that may benefit from targeted intervention . Achalasia, a primary esophageal motility disorder in people, results from a selective loss of inhibitory myenteric neurons leading to a failure of the LES to relax in response to pharyngeal swallowing and impaired esophageal peristalsis . It represents a rare cause of ME that responds to targeted intervention and is considered distinct from conditions that cause esophageal hypomotility without functional LES obstruction.…”

Section: Discussionmentioning

confidence: 99%

“…7 Achalasia, a primary esophageal motility disorder in people, results from a selective loss of inhibitory myenteric neurons leading to a failure of the LES to relax in response to pharyngeal swallowing and impaired esophageal peristalsis. 24 It represents a rare cause of ME that responds to targeted intervention and is considered distinct from conditions that cause esophageal hypomotility without functional LES obstruction. This condition has been suspected in dogs, with a few case reports over the last 4 decades and most presumptive diagnoses being made without manometry or dynamic imaging studies.…”

Section: Discussionmentioning

confidence: 99%

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Mechanical dilation, botulinum toxin A injection, and surgical myotomy with fundoplication for treatment of lower esophageal sphincter achalasia‐like syndrome in dogs

Grobman

Hutcheson

Lever

et al. 2019

Veterinary Internal Medicne

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Background Megaesophagus (ME) carries a poor long‐term prognosis in dogs. In people, lower esophageal sphincter (LES) achalasia is a rare cause of ME that may respond to targeted intervention. Dogs with lower esophageal sphincter achalasia‐like syndrome (LES‐AS) have been described recently, warranting investigation of analogous targeted treatment. Hypothesis/Objectives Evaluate response of dogs with LES‐AS to LES mechanical dilation and botulinum toxin A (BTA) injections, with or without surgical myotomy and fundoplication. We hypothesized that clinical and videofluoroscopic swallow study (VFSS) features of LES‐AS would improve after treatment targeting functional LES obstruction. Animals Fourteen client‐owned dogs with LES‐AS diagnosed by VFSS. Methods Retrospective study. Dogs diagnosed with LES‐AS underwent treatment between April 2015 and December 2017. Outcome measures included client perception of clinical severity, body weight (BW), body condition score (BCS), regurgitation frequency, and VFSS parameters (ME, esophageal motility, gastric filling). Dogs with positive responses were considered candidates for LES myotomy with fundoplication. Results By a median IQR of 21 (IQR, 14‐25) days after mechanical dilation and BTA, clients reported clinical improvement in 100% of dogs, BW increased 20.4% (IQR, 12.7%‐25%), pre‐ and post‐treatment BCS was 3 (IQR, 3‐4) and 5 (IQR, 4‐5), respectively, and frequency of regurgitation decreased by 80% (IQR, 50%‐85%). Duration of effect was 40 (IQR, 17‐53) days. Despite clinical improvement, ME and abnormal esophageal motility persisted in 14 dogs. Six dogs subsequently underwent myotomy and fundoplication and maintained improvement observed after mechanical dilation and BTA. Conclusions and Clinical Importance Dogs with LES‐AS experienced significant, temporary, clinical improvement after mechanical dilation and BTA. Preliminary results suggest myotomy with fundoplication provide lasting clinical benefit despite persistence of ME.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Mechanical dilation, botulinum toxin A injection, and surgical myotomy with fundoplication for treatment of lower esophageal sphincter achalasia‐like syndrome in dogs

Grobman

Hutcheson

Lever

et al. 2019

Veterinary Internal Medicne

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“…However, when HSV-1 is reactivated, IFN-γ and IL-2 production is increased, and infected neurons are lysed 17 . Thus, latency and active replication of HSV-1, but not cytomegalovirus or Epstein-Barr virus, has been detected along the myenteric plexus of achalasia patients 10,18,19 . Our group 12 ( Fig.…”

Section: Infection Agentsmentioning

confidence: 93%

Infectious agents as potential triggers for autoimmunity in achalasia

Furuzawa‐Carballeda¹,

Coss‐Adame²,

Valdovinos³

et al. 2020

NGL

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“…The pathophysiological mechanism of achalasia remains unknown. However, several studies suggest that it involves an interaction between inflammatory and autoimmune responses, such as viral infections, in genetically susceptible individuals . The proposed pathogens in triggering the inflammatory response in achalasia, include herpes simplex virus (HSV), varicella‐zoster, measles, and human papillomavirus .…”

Section: Introductionmentioning

confidence: 99%

Triosephosphate isomerase, carbonic anhydrase, and creatinine kinase‐brain isoform are possible antigen targets in patients with achalasia

Hernández‐Ramírez

Olivares-Martínez

Núñez‐Álvarez

et al. 2020

Neurogastroenterology Motil

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Background: Idiopathic achalasia is an uncommon esophageal motor disorder. The disease involves interaction between inflammatory and autoimmune responses. However, the antigens related to the disease are still unknown. Aim: To identify the possible antigen targets in muscle biopsies from lower esophageal sphincter (LES) of achalasia patients. Methods: Esophageal biopsies of patients with type I and type II achalasia and esophagogastric junction outflow obstruction (EGJOO) were analyzed. Lower esophageal sphincter muscle biopsy from a Healthy organ Donor (HD) was included as control for two-dimensional gel electrophoresis. Immunoblotting of muscle from LES lysate with sera of type I, type II achalasia, or type III achalasia, sera of EGJOO and sera of healthy subjects (HS) was performed. The target proteins of the serum were identified by mass spectrometry Matrix-assited laser desorption/ionization time-of-flight (MALDI-TOF).Key Results: The proteomic map of muscle from LES tissue lysates of type I, and type II achalasia, EGJOO, and HD were analyzed and divided into three important regions.We found a difference in the concentration of certain spots. Further, we observed the serum reactivity of type I achalasia and type II achalasia against 45 and 25 kDa bands of type I achalasia tissue. Serum of type III achalasia and EGJOO mainly recognized 25 kDa band. Bands correspond to triosephosphate isomerase (TPI) (25 kDa), carbonic anhydrase (CA) (25 kDa) and creatinine kinase-brain (CKB) isoform (45 kDa). Conclusions and Inferences:We identify three antigen targets, TPI, CA, and CKB isoform, which are recognized by sera from patients with achalasia. K E Y W O R D Sachalasia, carbonic anhydrase, creatinine kinase-brain, lower esophageal sphincter muscle, mass spectrometry MALDI-TOF, proteomic, triosephosphate isomerase

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New insights into the pathophysiology of achalasia and implications for future treatment

Cited by 83 publications

References 94 publications

Mechanical dilation, botulinum toxin A injection, and surgical myotomy with fundoplication for treatment of lower esophageal sphincter achalasia‐like syndrome in dogs

Mechanical dilation, botulinum toxin A injection, and surgical myotomy with fundoplication for treatment of lower esophageal sphincter achalasia‐like syndrome in dogs

Infectious agents as potential triggers for autoimmunity in achalasia

Triosephosphate isomerase, carbonic anhydrase, and creatinine kinase‐brain isoform are possible antigen targets in patients with achalasia

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