metricas
covid
Buscar en
Annals of Hepatology
Toda la web
Inicio Annals of Hepatology OP-8 SECOND LINE THERAPY IN PATIENTS WITH PRIMARY BILIARY CHOLANGITIS AND INADEC...
Journal Information
Vol. 29. Issue S3.
Abstracts of the 2024 Annual Meeting of the ALEH
(December 2024)
Share
Share
Download PDF
More article options
Vol. 29. Issue S3.
Abstracts of the 2024 Annual Meeting of the ALEH
(December 2024)
Full text access
OP-8 SECOND LINE THERAPY IN PATIENTS WITH PRIMARY BILIARY CHOLANGITIS AND INADECUATE RESPONSE: ARE WE CHOOSING THE RIGHT TARGET POPULATION FOR CLINICALS TRIALS?
Visits
31
Daniela De La Viña1, Natalia Sobenko1, Eduardo Mullen1, Ignacio Lucero1, Juan Carlos Bandi1, Maria Alejandra Villamil1
1 HOSPITAL ITALIANO DE BUENOS AIRES, BUENOS AIRES, Argentina
This item has received
Article information
Abstract
Full Text
Download PDF
Statistics
Tables (1)
Special issue
This article is part of special issue:
Vol. 29. Issue S3

Abstracts of the 2024 Annual Meeting of the ALEH

More info
Conflict of interest

No

Introduction and Objectives

Identification of primary biliary cholangitis (PBC) patients who could benefit from second line therapy is uncertain. Most trials rely on 12 month UDCA response assessed by POISE criteria.

Evaluate eligible patients and identify epidemiological-clinical and histological findings that may adversely influence response.

Patients / Materials and Methods

Among 614 patients with established diagnosis of PBC (Jan/16 and Dec/23) 279 were unable to normalize alkaline phosphatase (ALP) and BT after 12 months of UDCA. 107/279 (38.3 %) fulfilled elegibility criteria for second line trials (ALP >1.67, bilirubin <2 and non significant portal hypertension) were analyzed. Fibrosis, bile duct loss, cholangitic and hepatitis activity were obtained in 92/107 patients (Scheuer and Nakanuma scores). All samples were stained with cytokeratin 7. Elastography was done in all patients.

Results and Discussion

Characteristics of patients who fulfilled POISE criteria are described in Table 1. Mean MELD was higher in cirrhotic (9.0vs7.1, p<.001) and correlated with liver events (9.6vs7.0, p<.001). 43/92 patients had moderate-severe ductopenia in histological samples, and it was significantly more frequent in <45 years (66%vs32%, p.008). Moderate-severe portal inflammation with interface hepatitis and lobular spilling was observed in 52/92 samples (56.5%), irrespective of age and correlated with fibrosis. ALP was significantly higher in patients with ductopenia (437.9±207.8vs319.2±162.0, p.01). Elastography correlated with cirrhosis and liver events (10.4vs22.9, p<0.001) but not with inflammation or ductopenia.

Conclusions

A significant proportion of patients unresponsive to UDCA were not eligible for second line trials. Poise criteria eligibility was associated with the presence of ductopenia and advanced fibrosis, particularly in young patients. The presence of moderate to severe portal inflammation is suggestive of ongoing disease activity. Elastography and MELD score correlate with cirrhosis and development of liver events. These findings suggest that we are selecting for second line trials a significant proportion of patients with adverse findings for response. Adverse histological findings might suggest early second line intervention.

Full Text

Baseline characteristics  Patients (n=92) 
Age, mean (years)  55.9 (± 11.8) 
Female, num (%)  93 (22.4) 
< 45 years, num (%)  22 (22.4%) 
Associated autoimmune disease, num (%)  16 (17.3) 
Pruritus, num (%)  51 (55.1) 
ALP, mean (UI/L)  366.7 (± 192.5) 
GGT, mean (UI/L)  366.6 (± 326.2) 
ALT, mean (UI/L)  64.7 (± 43.6) 
TB, mean (mg/dL)  1.7 (± 4.6) 
Elastography >9.6 kPa, num (%)  42 (50%) 
MELD score, mean  7.4 (± 1.8) 
Cirrhotic, num (%)  17 (16) 
Moderate to severe portal inflammation with interface hepatitis and lobular spilling, num (%)  52 (56.5) 
AMA, num (%)  80 (86) 
Sp100, num (%)  9 (9.7) 
GP210, num (%)  8 (8.6) 
Under UDCA treatment, num (%)  89 (96.7) 

Abbreviations: ALP: alkaline phosfatase, gGT: gamma-glutamyl-transferase, ALT: alanine-transferase, TB: total bilirrubine, AMA: anti-mitochondrial antibody, UDCA ursodeoxycholic acid.

Characteristics of non responders patients

Download PDF
Article options
es en pt

¿Es usted profesional sanitario apto para prescribir o dispensar medicamentos?

Are you a health professional able to prescribe or dispense drugs?

Você é um profissional de saúde habilitado a prescrever ou dispensar medicamentos

Quizás le interese:
10.1016/j.aohep.2023.101039
No mostrar más