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. 2020 Jan 29;12(2):154. doi: 10.3390/v12020154

Table 5.

The overview of polysaccharides with anti-HSV activity.

Compound Antiherpetic and Cytotoxicity Assays, Strains, Cells, and Reference Agents Results Additional Information Source
PSP-B2 polysaccharide from Prunellae Spica (Prunella vulgaris L.) Vero cells, HSV-1, HSV-2
PRA
ACV HSV-1 IC50 0.78 µM, HSV-2 1.32 μM
HSV-1 IC50 69 μg/mL
HSV-2 IC50 49 μg/mL
No cytotoxicity even at 1600 μg/mL [84]
Eucheuma gelatinae (seaweed) polysaccharide Vero cells, HSV-1
PRA
ACV EC50 HSV-1(strain F), HSV-2 (strain 333), HSV-1 (strain 106), HSV-1 (strain 153), and HSV-1 (strain blue) 0.78, 0.71, 9.60, 21.11, and 23.50 μg/mL, respectively
HSV-1/F, HSV-2/333, HSV-1/106, HSV-1/153, and HSV-1/blue EC50 0.65, 2.12, 1.11, 1.24, and 1.48 μg/mL, respectively Effect via activity on early HSV-1 infection. Inhibition of viral DNA synthesis. [85]
Sulfated polysaccharide SP-III from Sargassum latifolium Vero cells, HSV-1
PRA
SP-III 33% and 81% inhibition at 20 μg/mL and 40 μg/mL, respectively. Glucuronic acid, mannose, glucose, xylose and fucose. [86]
Sulfated polysaccharide SP-2a from Sargassum patens (Kütz.) Agardh Vero cells, HSV-1 (15577 strain, clinical strain, DM2.1 strain-ACV resistant)
PRA
Determination of extracellular virucidal activity
Time of addition experiment
Virus adsorption assay
Inhibition of replication of both the acyclovir-sensitive and -resistant strains of HSV-1, in a dose-dependent manner, EC50 1.5–5.3 μg/mL Fucose, xylose, mannose, glucose, galactose, galactosamine
Extracellular virucidal activity only against the ACV-sensitive strains.
This compound might inhibit the attachment of the virus to its host cell.
[87]
ST-F polysaccharide from marine brown algae Sargassum trichophyllum Vero cells, HSV-2 (UW264 strain)
PRA
Time of addition experiment
Added to the medium during infection and throughout the incubation (Experiment A) or immediately after viral infection (Experiment B), IC50 18 and 410 μg/mL, respectively. SI > 280 and >12 for A and B, respectively. (Fucose and galactose)
The main antiviral target of ST-F might be virus adsorption and/or penetration step(s) on the host cell surface.
Low cytotoxicity
[88]
SPs -
sulfated polysaccharides from brown sea algae Sargassum fluitans and red sea algae Solieria filiformis
Vero cells, HSV-1
Neutral red dye method
ACV EC50 15.4 ± 5.6 μg/mL
S. fluitans EC50 42.8 ± 4.3 μg/mL and S. filiformis EC50 136.0 ± 12 μg/mL
Without cytotoxicity (1–200 μg/mL)
The activity observed suggests that the degree of sulfation, molecular weight, and carbohydrate nature of these polysaccharides may affect the activity [89]
Polysaccharide fractions C1p and C4p from chlorophyta Ulva armoricana Vero cells, HSV-1 (wild-type strain 17, sensitive to ACV)
CPE
ACV EC50 0.3 µg/mL
EC50 373.0 ± 20.7 and 320.9 ± 6 µg/mL Activities correlated to amounts of rhamnose, uronic acids and degree of sulfation. [90]
Sp-Am polysaccharide from Acanthophora muscoides Vero cells, HSV-1, HSV-2
CPE
HSV-1 IC50 1.63 μg/mL, SI = 3.5
HSV-2 IC50 3.5 μg/mL, SI = 99.9
Sulfated polysaccharides from marine seaweeds
The possible mechanism of the effect - the inhibition of virus adsorption.
[91]
SP-Gb polysaccharide from Gracila riabirdiae HSV-1 IC50 0.75 μg/mL, SI = 1.25
HSV-2 IC50 82.2 μg/mL, SI = 94.40
SP-Sf polysaccharide from Solieria filiformis HSV-1 IC50 0.6 μg/mL, SI = 1.6
HSV-2 IC50 74.9 μg/mL, SI = 97.5
PSC polysaccharide from marine seaweed Sphaerococcus coronopifolius Vero cells, HSV-1 (wild type strain 17, sensitive to ACV)
CPE
Time of addition assay
Virus adsorption assay
ACV SI ˃ 500
EC50 4.1 μg/mL, SI = 61 Galactose, 3,6-anhydrogalactose, uronic acids, sulfated
The adsorption step of HSV-1 to the host cell possible mechanism of action.
[92]
PBT polysaccharide from marine seaweed Boergeseniella thuyoides EC50 17.2 μg/mL, SI = 14.5
Sulfated xylogalactofucans and alginic acids from brown algae Laminaria angustata RC-37 cells, HSV-1 (KOS)
PRA
Time of addition assay
Virus adsorption assay
Virucidal assay
IC50 0.21–25 μg/mL, SI ˃ 40 ˃ 3225
Possible inhibiting HSV attachment to cells by direct interaction with viral particles. [93]
SU1F1 polysaccharide from green algae Enteromorpha compressa HEp-2 cells, HSV-1 (clinical isolate)
PRA
Time-of-addition assay
Inhibition of adsorption assay
Inhibition of penetration assay
Virucidal assay
Acyclovir IC50 2100 μg/mL, SI = 1.21
IC50 28.25 μg/mL, SI = 35.3 Chemically altered- sulfated ulvan
Broad mechanism of action.
[94]
Sulfated fucoidans (S1-S3) from marine brown alga Padina tetrastomatica Vero cells, HSV-1 (strains F and B2006), HSV-2 (strain MS)
PRA
Virucidal assay
Effect of treatment period on the antiviral activity
HSV-1 and HSV-2 with IC50 in range of 0.30–1.05 μg/mL
B2006 S3 IC50 0.6 μg/mL
Active during the virus adsorption period
Degree of sulfation affects the activity
[95]
Polysaccharides from brown seaweed Stoechospermum marginatum Vero cells, HSV-1 (strains F, TK- B2006 and filed strains, syncytial variants arising after selection with a natural carrageenan, syn 13-8 and 14-1), HSV-2 (MS)
PRA
HSV-1 (F) EC50 1.15-50 μg/mL, SI = ˃20 ˃ 869
HSV-2 (MS) EC50 0.78 μg/mL, SI= 0.57 ˃50
F3 B2006, Field, 13-8 and 14-1 strains EC50 0.95, 1.52, 4.52 μg/mL, SI ˃1053, ˃658, ˃221, ˃176
Sulfated fucans
Active during the virus adsorption period.
No direct virucidal activity.
No correlation between the antiviral and anticoagulant activity.
[96]
CiWE CiF3 polysaccharides from brown seaweed Cystoseira indica Vero cells, HSV-1 (strain F), HSV-2 (strain MS)
PRA
IC50 values in the range of 0.5–2.8 μg/mL Sulfated fucans
Degree of sulfation affects the activity.
No correlation between the antiviral and anticoagulant activity.
[97]
Sulfated polysaccharide (fucoidan) from brown algae Undaria pinnatifida (Mekabu) Vero cells, HSV-1 (strain HF), HSV-2 (strain UW-268)
PRA
A) 1 h after the viral infection, B) immediately after infection
HSV-1 IC50 and SI A) 2.5 μg/mL, ˃800; B) 14 μg/mL, ˃140
HSV-2 IC50 and SI A) 2.6 μg/mL, ˃770; B) 5.1 μg/mL, ˃390
Fucose, galactose
Other viruses tested.
[98]
Polysaccharides (GiWE and F3) from red seaweed Grateloupia indica Vero cells, HSV-1 (strain F, TK- B2006 and filed strains, syncytial variants arising after selection with natural carrageenan, syn 13-8 and 14-1), HSV-2 (MS)
PRA
HSV-1 (F) IC50 0.27 μg/mL and HSV-2 (MS), IC50 0.31 μg/mL
F3 B2006, Field, 13-8 and 14-1 strains EC50 0.89, 0.87, 1.06, 0.81 μg/mL, SI ˃ 1123, ˃1149, ˃943, ˃1234
No direct virucidal activity at 40 μg/mL
Sulfated galactans
Degree of sulfation affects the activity.
Possible ability to interfere with the replication cycle.
[99]
Polysaccharide from Schizymenia binderi Vero cells, HSV-1 (strains F, TK (B2006), (Field)), HSV-2 (G)
PRA
EC50 0.21-0.76 μg/mL
SI > 1000 for all assays
No cytotoxicity at 1000 μg/mL
Sulfated galactan
Interference with the initial adsorption of viruses to cells, no virucidal activity at 100 μg/mL.
[100]
Polysaccharide from red seaweed Gigartina skottsbergii Vero cells, HSV-1 (strains F, TK (B2006), (Field), clinical isolates 1213 LCR/94, 374 LCR/94 and 1180 BE/94), HSV-2 (G, clinical isolate 244 BE/94)
PRA
1C3 HSV-1 (F) and HSV-2 (G) EC50 0.7 and 0.5 µg/mL, respectively, SI ˃ 1408 and ˃2128
1T1 HSV-1 (F) and HSV-2 (G) EC50 0.6 and 0.4 µg/mL, respectively, SI ˃ 1538 and ˃2439
Clinical isolates EC50 0.19–2.18 µg/mL
Carrageenans
Lack of anticoagulant activity
No virucidal activity, effect on virus adsorption
[101]
Proteoglycan GLPG from Ganoderma lucidum (Agaromycetes)—lingzhi mushroom Vero cells, HSV-1, HSV-2
CPE
Virus yield inhibition assay
HSV-1 and HSV-2 EC50 48 and 56 µg/mL, respectively, SI ˃ 42 and >36
No cytotoxicity at 2000 µg/mL
Proteoglycan GLPG (carbohydrate: protein ratio of 10.4: 1)
The antiviral activity may be due to its inhibiting HSV attachment to cells, in addition, its inhibition of viral penetration would augment its antiviral activity.
[102]
Polysaccharide RP from Portulaca oleracea Vero cells, HSV-2 (UW268 strain)
PRA
Time-of-addition assay
Virus adsorption and penetration assay
A: RP added during infection and throughout the incubation thereafter
B: RP added immediately after viral infection.
A: EC50 210 µg/mL, SI = 33
B: EC50 320 µg/mL, SI = 22
Pectic polysaccharide (RP)
Activity against influenza virus tested on MDCK cells.
[103]
Polysaccharide SPLCf from Caesalpinia ferrera HEp-2 cells, HSV-1 (clinical isolate)
PRA
Time-of-addition assay
Inhibition of adsorption assay
Inhibition of penetration
Virucidal activity
HSV-1 cell to cell spread assay
ACV IC50 2100 μg/mL, SI >1.21
IC50 405 μg/mL, SI > 7.4. Sulfated polysaccharide
SPLCf showed the effect on several stages of the HSV replication—virus adsorption, the effect on virus particles and the expression of viral protein.
[104]
Polysaccharides (ANP, AAP) from Acanthopanax sciadophylloides Vero cells, HSV-2 (UW264 strain)
PRA
In vivo anti-HSV-2 effects on female BALB/c mice
ACV
In vivo: Polysaccharides (1 mg/20 μL) or ACV (0.2 mg/20 μL) administered intravaginally twice per day from 3 days before infection to 7 days post-infection.
ANP and AAP IC50 52 and 620 μg/mL when added to the medium during infection and throughout the incubation thereafter
HSV-2 IC50 67 and 580 μg/mL when added to the medium immediately after infection.
Acanthopanax sciadophylloides
Virus titers in the vaginal region were decreased by the administration of AAP.
[105]
Acidic polysaccharide (nostoflan) from terrestrial cyanobacterium Nostoc flagelliforme Vero cells, HSV-1 (HF strain) and HSV-2 (UW268 strain)
PRA
A: added during infection and throughout the incubation thereafter
B: added immediately after viral infection
A: HSV-1 IC50 0.37 μg/mL, SI = 13000
A: HSV-2 IC50 2.9 μg/mL, SI = 2700
B: HSV-1 IC50 ˃100 μg/mL, SI = <49
B: HSV-2 IC50 7.7 μg/mL, SI = 1000
Other antiviral activity tested.
No anti-thrombin activity.
[106]
Polysaccharide sulfate fraction from Caulerpa racemosa Vero cells, HSV-1 strain F, TK- B2006 and field strains), HSV-2 G strain)
PRA
HSV-1 (strain F, TK- B2006 and field strains) EC50 4.2, 2.4, 2.2 µg/mL, SI ˃ 238, ˃417, ˃454
HSV-2 (strain G) EC50 3.0 µg/mL, SI ˃ 333
No cytotoxic effects up to 1000 µg/mL
Galactose, glucose, arabinose, and xylose as the major components. [107]