Introduction: Despite the growing number of highly efficacious biologics and chemical drugs for ulcerative colitis (UC), steroid-free disease control is still difficult to achieve in subgroups of patients due to refractoriness, adverse events, primary or secondary failure. New treatments are therefore still required in order to optimize clinical management of patients with UC. Areas covered: The efficacy and safety of both currently available and newly developed small molecules have been summarized. The PubMed database and clinicaltrials.gov were considered in order to search for phase 2b and 3 trials on new chemical drugs for UC. The study drugs reviewed included Janus kinases (JAK) and sphingosine-1-phosphate receptor (S1Pr) inhibitors, α4 integrin antagonist, and micro-RNA-124 upregulators. Expert Opinion: Rapidity of onset, low immunogenicity, and safety are the main characteristics of small molecules currently available or under evaluation for treatment patients with UC. Among the currently available chemical drugs, the selective JAK and the S1Pr inhibitors are characterized by a good safety profile combined with the ability to induce clinical remission in UC. A relatively low frequency of endoscopic improvement and healing currently appears associated with their use, being higher in UC patients treated with S1Pr inhibitor Etrasimod. Overall, additional new safe and effective drugs are still required in order to optimize disease control in a larger majority of UC patients.

Neri, B., Mancone, R., Fiorillo, M., Schiavone, S.c., De Cristofaro, E., Migliozzi, S., et al. (2024). Comprehensive overview of novel chemical drugs for ulcerative colitis: focusing on phase 3 and beyond. EXPERT OPINION ON PHARMACOTHERAPY, 25(5), 485-499 [10.1080/14656566.2024.2339926].

Comprehensive overview of novel chemical drugs for ulcerative colitis: focusing on phase 3 and beyond

Neri, Benedetto;Mancone, Roberto;Fiorillo, Mariasofia;Schiavone, Sara Concetta;De Cristofaro, Elena;Migliozzi, Stefano;Biancone, Livia
2024-04-01

Abstract

Introduction: Despite the growing number of highly efficacious biologics and chemical drugs for ulcerative colitis (UC), steroid-free disease control is still difficult to achieve in subgroups of patients due to refractoriness, adverse events, primary or secondary failure. New treatments are therefore still required in order to optimize clinical management of patients with UC. Areas covered: The efficacy and safety of both currently available and newly developed small molecules have been summarized. The PubMed database and clinicaltrials.gov were considered in order to search for phase 2b and 3 trials on new chemical drugs for UC. The study drugs reviewed included Janus kinases (JAK) and sphingosine-1-phosphate receptor (S1Pr) inhibitors, α4 integrin antagonist, and micro-RNA-124 upregulators. Expert Opinion: Rapidity of onset, low immunogenicity, and safety are the main characteristics of small molecules currently available or under evaluation for treatment patients with UC. Among the currently available chemical drugs, the selective JAK and the S1Pr inhibitors are characterized by a good safety profile combined with the ability to induce clinical remission in UC. A relatively low frequency of endoscopic improvement and healing currently appears associated with their use, being higher in UC patients treated with S1Pr inhibitor Etrasimod. Overall, additional new safe and effective drugs are still required in order to optimize disease control in a larger majority of UC patients.
apr-2024
Pubblicato
Rilevanza internazionale
Recensione
Esperti anonimi
Settore MED/12
Settore MEDS-10/A - Gastroenterologia
English
JAK; Mi-RNA-124; S1Pr; chemical drugs; clinical trials; small molecules; ulcerative colitis; α4 integrin
Neri, B., Mancone, R., Fiorillo, M., Schiavone, S.c., De Cristofaro, E., Migliozzi, S., et al. (2024). Comprehensive overview of novel chemical drugs for ulcerative colitis: focusing on phase 3 and beyond. EXPERT OPINION ON PHARMACOTHERAPY, 25(5), 485-499 [10.1080/14656566.2024.2339926].
Neri, B; Mancone, R; Fiorillo, M; Schiavone, Sc; De Cristofaro, E; Migliozzi, S; Biancone, L
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/396531
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