Study In-vitro and in-silico of ethylacetate extract and fractions of soft coral Lobophytum sp. towards Artemia salina Brine Shrim (BSLT)

Sahidin Sahidin; Adryan Fristiohady; Wahyuni Wahyuni; Arfan Arfan; Baru Sadarun; Nur Syifa Rahmatika; Agung Wibawa Mahatva Yodha; Nur Upik En Masrika; Andini Sundowo; Sofa Fajriah

doi:10.1051/bioconf/20237404004

All issues

Volume 74 (2023)

BIO Web Conf., 74 (2023) 04004

Abstract

Open Access

Issue		BIO Web Conf. Volume 74, 2023 The 12^th International and National Seminar of Fisheries and Marine Science (ISFM XII 2023)


Article Number		04004
Number of page(s)		12
Section		Marine, Fisheries Biotechnology, Ocenography, and Fishing Technologie
DOI		https://doi.org/10.1051/bioconf/20237404004
Published online		13 November 2023

BIO Web of Conferences 74, 04004 (2023)

Study In-vitro and in-silico of ethylacetate extract and fractions of soft coral Lobophytum sp. towards Artemia salina Brine Shrim (BSLT)

Sahidin Sahidin¹^*, Adryan Fristiohady¹, Wahyuni¹, Arfan¹, Baru Sadarun², Nur Syifa Rahmatika³, Agung Wibawa Mahatva Yodha⁴, Nur Upik En Masrika⁵, Andini Sundowo⁶ and Sofa Fajriah⁷

¹ Faculty of Pharmacy, Universitas Halu Oleo, Kendari, INDONESIA
² Faculty of Marine Sciences and Fisheries, Universitas Halu oleo, Kendari, INDONESIA
³ Faculty of Medicine, Universitas Halu Oleo, Kendari, INDONESIA
⁴ Health Polytechnics of Bina Husada, Kendari, INDONESIA
⁵ Faculty of Medicine, Universitas Khairun, Ternate, INDONESIA
⁶ Research Centre for Chemistry
⁷ Research Centre for Pharmaceutical Ingredient and Traditional medicine, BRIN, Kawasan Puspitek, Tangerang Selatan 15314, Banten, INDONESIA

^* Corresponding author: sahidin02@uho.ac.id

Abstract

The article aims to describe the findings of chemical and pharmaceutical aspects of Lobophytum sp. from Southeast Sulawesi, Indonesia. Ethylacetate extract was fractionated by Vacuum liquid chromatography (VLC). Toxicity was evaluated by BSLT test, and the phytochemical screening and LCMSMS method were used to determine the chemical composition and molecular docking for in-silico study. The results showed that the ethylacetate extract was produced seven fractions namely Fraction A-G. The weight of each fraction was A (12.8% w/w), B (9.7%), C (10.1%), D (2.0%), E (7.0%), F (25, 3%) and G (11.5%). The toxicity potency of Fraction B is the most toxic with LC50 (mg/L) 26.70 ± 0.58. LCMSMS data indicated that the fraction B contains 19L-glukocyl-14-deoxy-11,12-didehydrographoside, 3-isoazmalicine, abietraticine, arachidonic acid, neociwujiaphenol, oxyphyliacinol, saurufuran B and some unidentified compounds with molecular formulas C₃₇H₄₆O₇, C₃₅H₄₄O₅, and C₂₀H₂₆O₂. Based on computational simulations, Ar-Abietatriene and 3-Isoajmalicine have the potential to inhibit CDK-6. These compounds hinder the progression of the cell cycle and the proliferation of cancer cells by forming molecular interactions with residues Ile19, Val27, Ala41, Val77, Phe98, Val101, Leu152, and Ala162. This suggests their potential as anticancer agents. Thus, Fraction B can be continued for the anticancer evaluation.

This is an Open Access article distributed under the terms of the Creative Commons Attribution License 4.0, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

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