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  4. Gut Mycobiota Dysbiosis Is Associated with Melanoma and Response to Anti–PD-1 Therapy
 
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Gut Mycobiota Dysbiosis Is Associated with Melanoma and Response to Anti–PD-1 Therapy

Type
Journal article
Language
English
Date issued
2024
Author
Szóstak, Natalia
Handschuh, Luiza
Samelak-Czajka, Anna
Tomela, Katarzyna
Pietrzak, Bernadeta 
Schmidt, Marcin 
Galus, Łukasz
Mackiewicz, Jacek
Mackiewicz, Andrzej
Kozlowski, Piotr
Philips, Anna
Faculty
Wydział Nauk o Żywności i Żywieniu
PBN discipline
food and nutrition technology
Journal
Cancer immunology research
ISSN
2326-6066
DOI
10.1158/2326-6066.CIR-23-0592
Web address
https://aacrjournals.org/cancerimmunolres/article/12/4/427/741948/Gut-Mycobiota-Dysbiosis-Is-Associated-with
Volume
12
Number
4
Pages from-to
427-439
Abstract (EN)
Recent research indicates that gut microbiota may be vital in the advancement of melanoma. In this study, we found that melanoma patients exhibited a distinct gut mycobiota structure compared with healthy participants. Candida albicans, Candida dubliniensis, and Neurospora crassa were more abundant in samples from patients with melanoma, whereas Saccharomyces cerevisiae and Debaryomyces hansenii were less abundant. During anti–PD-1 treatment, the relative amount of Malassezia restricta and C. albicans increased. A higher level of Saccharomyces paradoxus was associated with a positive response to anti–PD-1 treatment, whereas a higher level of Tetrapisispora blattae was associated with a lack of clinical benefits. High levels of M. restricta and C. albicans, elevated serum lactate dehydrogenase, and being overweight were linked to increased risk of melanoma progression and poorer response to anti–PD-1 treatment. Thus, this study has revealed melanoma-associated mycobiome dysbiosis, characterized by altered fungal composition and fungi species associated with a higher risk of melanoma progression, identifying a role for the gut mycobiome in melanoma progression.
License
cc-by-nc-ndcc-by-nc-nd CC-BY-NC-ND - Attribution-NonCommercial-NoDerivatives
Open access date
February 5, 2024
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