Steroidal Saponins

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Phytochemiafry, Vol. 21, No. 5. pp. 959-978, 1982. Printed in Great Britain.

0031~9422/82/05095%20$10.00/0 @ 1982 Pergamon Press Ltd.

REVIEW
STEROID SAPONINS
S. B. MAHATO, A. N. GANGULY and N. P. SAHU Indian Institute of Experimental Medicine, Calcutta 700 032, India
(Revised received 18 August 1981) Key Word Index-Steroid saponins; sapogenins; isolation; structure elucidation; natural distribution.

Ah&a&-Steroid saponins isolated from various plants are reviewed. The newer techniques used in their isolation and strucure elucidation are discussed. A compilation of the saponins isolated up to 1980 along with their available physical data is included. The basic steroidal saponins isolated after 1972 are also compiled.
INTRODUCTION

The saponins are plant glycosides which have the property of forming a soapy lather when shaken with water. The cardiac glycosides also possess this property but these are classified separately because of their specific biological activity. The saponins are classified as steroid or triterpenoid saponins depending upon the nature of the aglycone. The aglycone of a steroid saponin is usually a spirostanol or its modification. A third group of saponins which are called basic steroid saponins contain nitrogen analogues of steroid sapogenins as aglycones. Some natural products may produce froth with water but only exhibit some of the properties of saponins. Excellent general reviews on saponins [l-7] have been published. Particular mention may be made of the comprehensive reviews on the triterpenoid saponins by Rastogi et al. [&lo]. Steroid saponins have been reviewed briefly by Elks [11,12] and Takeda [13]. The basic steroid saponins have been reviewed by Schreiber [14], Roddick [IS], Herbert [16] and Harrison [17]. This review deals with recent developments with regard to isolation and structure elucidation of steroid saponins including the configuration of the carbohydrate moieties.
ISOLATION

procedure involving for the separation

The methods of isolation of steroid saponins are essentially the same as those of triterpenoid saponins. The classical methods of isolation of triterpenoid saponins have been reviewed [8-101. The separation of a saponin mixture into individual components is a formidable task. The development of recent chromatographic techniques has provided valuable means for isolation of pure saponins and their derivatives. A convenient method of separation of steroidal glycosides has been described by Nohara et al. [18].
Sephadex LH-20 chromatography countercurrent chromatography @CC) and droplet

Si gel CC and Sephadex LH-20 of furostanol oligosides of Asparagus cochinchinensis has been described by Konishi and Shoji [19]. The technique of DCC [20,21] has been applied successfully for the separation of saponins. The technique is based on the difference of the partition coefficients of compounds in liquidliquid phases such as countercurrent distribution. Those solvent systems which form two immiscible layers are selected for the separation of the compounds by this method. In the case of Sephadex LH-20 chromatography, plant extracts are partially purified by the usual Si gel CC methods before subjecting them to DCC. This technique is useful for the small scale and semi-micro qualitative and quantitative determination of saponins. Nevertheless, it requires a longer time, viz., a period of four days to a week even for effective semi-micro separation. The molluscidal saponins from Comus florida have been separated by Hostettman et al. [22]. The methanol extract of the plant was first fractionated by Sephadex LH-20 CC followed by the separation of pure saponins by DCC. This method has also been applied for the separation of the dammarane-type saponins of Panax ginseng and P. japonicum by Tanaka et al. [23,24]. The separation of the major saponins of Bupleuri radix has been achieved using the DCC technique by Otsuka et al. [251.
High performance liquid chromatography (HPLC)

Sephadex LH-20 has successfully been used for the separation of steroidal saponins. A typical isolation
PHYTO Vol. 21. No. 5-A

The very efficient newer technique of HPLC is increasingly being used for the separation of various compounds including saponins. The technique has been described in a recent book by Simpson [26]. Rapid, selective, and highly sensitive separation of saponins can be effected by HPLC using a variety of stationary and mobile phases. Successful separation of the major saponin components in liquorice has been achieved using HPLC [27]. Tanaka et al. [28] have analysed the saponin constituents of Bupleuri radix on a column of octadecylsilylated (ODS) Si gel LS-410 with a mixture of methanol, water, acetic acid
959

960

S.B.MAHATO, A.N. GANGLJLYand N. P. SAW

and triethylamine as the mobile phase. Anthracene was used as an appropriate int. standard for quantitative analysis. The saponin mixture obtained from Tribulus terrestris (Mahato, S. B. et al., unpublished results) was separated on a column of p-Bondapak Cl8 using methanol as the mobile phase. The very complex mixtures of saponins which were not amenable to separation previously can now be effectively separated by a combination of silica gel CC, gel chromatography on Sephadex LH-20 and HPLC on a reversed phase column.
STRUCTUREELUCIDATION

The conventional method of structure elucidation of steroidal saponins starts with acid hydrolysis which yields the aglycone and the sugar moieties which are separately investigated. Extensive chemical studies on the aglycones revealed that they are almost exclusively spirostane derivatives. But furostanol glycosides, which according to Marker and Lopez [29] are precursors of spirostane glycosides, have also been isolated and characterized. A simple qualitative test for furostanol glycoside has been developed by Kawasaki et al. [30]. The furostanol glycosides with some exceptions [18], show a characteristic red colour on a TLC plate when sprayed with pdimethylaminobenzaldehyde and hydrochloric acid (Ehrlich reagent). Moreover, the furostane skeleton does not exhibit the characteristic IR absorptions of spirostane derivatives [6]. Confirmatory evidence for the furostane structure is obtained by examination of the products of Markers degradation or BaeyerVilliger oxidation followed by hydrolysis. The first isolation of a furostanol glucoside, jurubine (l), was announced by Schrieber and Ripperger [31] and later Tschesche et al. [32, 331 isolated and characterized a furostanol bisglycoside, sarsaparilloside (2), corresponding to the spirostanol glycoside, parillin. Moreover, some glycosides have been isolated whose aglycones are not spirostanol but a modification. In general, the sugar moieties of steroidal saponins are oligosaccharides which consist of 2-4 kinds of sugar units, e.g. D-glucose, u-galactose, u-xylose and Lrhamnose. DXylose and L-rhamnose generally occur at the terminal positions. Arabinose-containing steroidal saponins are also known. In a very few cases, quinovose occurs as the carbohydrate moiety. Trillenoside A, a novel ll-norspirostanol glycoside, contains xylose, rhamnose, arabinose and apiose as the sugar constituents [34-361. Another unusual

saponin consisting of kammogenin and five molecules of 2deoxyribose has been reported by Backer et al. [37]. The furostanol bisglycosides so far isolated contain a glucose unit attached to the C-26 hydroxyl. In the classical method, the structure of the sugar moieties of the saponins is determined by identification of the monosaccharides obtained on acid hydrolysis by PC and GLC, quantitative determination of monosaccharides by GLC, partial hydrolysis followed by isolation and characterization of prosapogenins and also, where possible, by characterization of oligosaccharides. The points of attachment of different sugar units are revealed by permethylation of the saponins followed by hydrolysis or methanolysis and identification of the methylated sugars by PC or GLC. The mode of sugar linkage in saponins is determined by enzymic hydrolysis with aand @glycosidases or by the application of Klynes rule [38] on molecular rotation difference. However, both of these methods are not always applicable, particularly in the case of complex glycosides.

Mass spectrometry
Until very recently MW determination of saponins was a difficult task. But newer developments in mass spectrometry have almost solved this problem. Electron impact mass spectrometry (EIMS) has been shown to be a very useful method [39-42] for identification, determination of purity and structural elucidation of saponins, although volatile derivatives have to be produced. Moreover, saponins containing more than four sugars do not give molecular ions, even when derivatized. Field ionization mass spectrometry (FIMS) has been applied to the structural analysis of permethylated oligosaccharides underivatized r43,441, nucleosides [451, naturally occurring glycosides, e.g. somalin [46] and cardiac glycosides [47,48]. However, mass spectrometry has had limited application in the field of underivatized oligosaccharides because it requires volatilization and ionization of the sample. Ionization and volatilization are coupled in one process in field desorption mass spectrometry (FDMS) [49,50]. Very little of the energy goes into internal excitation and the degree of fragmentation is relatively small. FDMS of underivatized steroid and triterpenoid saponins have been reported 151-551. The spectra show the intense ions formed by attachment of alkali cations to the neutral molecule. The FDMS of the saponins not only gives the MW but also clear

Jurubine

Sarsaparil loside

Steroid saponins information with regard to the sequence of the sugar units in the molecule and their individual chemical structures by the fragment ions formed by the direct bond cleavages in the oligosaccharide moiety of the saponins. The formation of the fragment ions in FDMS has been discussed in relation to the well established mechanisms of glycosidic bond cleavage by the acidic hydrolysis. The new technique of plasma desorption mass spectrometry (PDMS) [56,57] has also been successfully employed for MW determination of underivatized steroidal saponins [22]. This technique utilizes energetic fission fragments from the decay of *Cf to volatilize and ionize a solid sample. The rapid sample heating (flash desorption) technique has been used for the structural analysis of o-hederin, a triterpenoid saponin [58]. H NMR spectroscopy peracetate or permethylate sometimes helpful in determining the mode of sugar When the spectrum shows an anomeric proton signal as a doublet with J - 7 Hz which is assignable
27

961

2 3

Wsitogenin, 25R, 2a, 36, ls~-cxr I3 Nectigogenin, 255, 36-0~ I4 Keochlorcgcnin, 25s. 39, 6a-aE I5 P~iculwenin, I6 Aeoegigenin, I7 Neo~lNwnin, Solagenin, Siealegenin, 25% 25S, 255, 25S, 3P, 2a, 6cr, 23p-OII 3p,
50, @-m

3 4 5 6 7 8 9 IO II 12

Pigwenin, Gitogenin, Ka~tawwnin,


Alliogenin.

25R, Jp-OB 25R, 2q 25R. 2a, 25R, 2a, rp-OH 36,


5a, @-OH

25R, 2a-OBe, 38, 3a, 25R, 38-OH, 3B,

66-0~

Heowen%
Wgenin,

12-130

6p-OH

Digalogenin, F.cckogenin,

25R. 3@, 156-0~ 25R, Ji3, 128-0~ 25R, 3p, Q-m

a-OhlorogenIn,

formation

(a- and C, in L-arabinose)

2a,

313, q-m 6a-oxi

residues. However, when several anomeric proton signals appear and when J is small (1-3 Hz), suggesting

I6 I9

~-CO,

25.S, 3f~-OH. 12-co

Moreover, it is observed that the anomeric proton signal of (Y-Dglucosides, a-D-mannosides, generally at lower field (8 5.0-6.0) than those of the corresponding 4.5-5.0). This difference structure. C NMR spectroscopy very useful tool for the elucidation developed and of the structures 20 2: 23 24 25 26 27 26 29 30 31
Yonogenin, Tokorogenin, Epimetagenin, 25 R, 28, 3a-OH 3a-OH I la-OH 25 R, 18, 28, 25 R, 28,3a,

aglycones and sugar moieties are available. shifts available [59-64] and the of a number of

carbon chemical sapogenins

Metagenin, 25R, 28, 38, I la-OH Protometagenin, 25 R,2/3, 38, I la-OH, 4-ene Nagiragenin, 25R, 38, Ila-OH Isorhodeasapogenin, 25 R, Ip, 3/3-OH Sarsasapogenenin, 25 S, 38 -OH Rhodeasapagenin, Conval lagenin A, Convol lagenin 6, Neotokorogenin ,

25S,
25 S,

I/?, 3/3-OH IB, 38, 5fl-OH OH

25 s, 11% 3&4&5fl25 S, 18, 2p, 3a-OH

@anomeric ranosides

pairs

of u-glucopythe direct bonded C-H coupling constant of the C-l signal (.L.w_J of hexapyranoses and pentopyranoses are characteristic of the anomeric configuration. Jc.r.w.l - 155 Hz when H-l is axial whereas it is cu 165 Hz when H-l is equatorial [76]. Thus it is evident that C NMR spectroscopy is of immense help in the elucidation of the structure of saponins.

steroid-, and triterpenoidoligoglycosides have been reported [63,72-751. The anomeric configuration different sugar moieties in a saponin can also be determined difference in chemical shifts of a- and carbons,

S. B. MAHATO, N. GANGULY A. and N. P. Sanu

32 33 34 35 36 37 36 39 40

Diosgenin, Ruscogenin, Yuccagen in, Kammogenin, Pennogenin, Prazerigenin Epidiosgenin, Epiruscogenin, Yamogenin,

25 R,

3f3-OH 3fi-OH 3/3-OH 3/3-OH, 17a-OH 14a-OH 12-w

25 R, I/3, 25177, 2a, 25R, 20, 2!iR, 38, A, 25 R, 38,

25R, 3a-OH 25 R, Ig, 3a-OH 25 S, 38-OH

OH

*--

HO-

HO@ OH

41 42

Cryptogenin 17 (201Dehydrocryptogenin

43

Hispigenin

HO H
44 Trillenqenin 45 46 Convallaaarogenin A5- Convallamarogeain

HO 47 Episceptrumgenin 46 Nuatigenin 49 Solanidine

..

HO 50 Solasodine

Steroid saponins
Table 1. Steroidal saponins whose genins and sugars have been fully characterized

963

Wonins (mp, MD)


Agave saponin C Agave saponin D

Source
Agaoc americana
Agaue americana

structure
Hecogenin 0, xyl-2gic-4glc-gla_(3B_OH) Hecogenin (7), rha )&Ic-glc-gal_(3kWH)

Reference
77-79 77-79

Agave saponin E, 304-3W, - 130 (MeOH)

Agave americana

xyl Hecogenin rha-rha

(7)

77.78.

80

)$glc-glc-gal-(3g-oH) Agave saponin H


Agave americana

xyl Hecogenin rha-rha

(7).

77,80

)Lc-glc-ga1~3a-0H,: XYl dc-W-OW

Agavoside Agavoside

A B

Agave americana
Agave americana Agaue americana Agave americana

Agavoside C 275, - 55 (DMP) Agavoside G

Hecogenin (7). gal-Q&OH) Hecogenin (7). glc-gal-(3g-OH) Hecogenin (7). glc-glc-gal-(3&OH) Hecogenin (7). rha )&-glc-gal-(36 xyl glc-(26-OH) Agigenin (8).
XYl

77,83 77, 83 77,a4 78.81 - OH);

Aginoside

All&m gigantenin

a2

)&lc-gal_(3g-OH) Allionin Alliumoside B


Allium karataviense Album narcissiflorum

Alliumoside

Allium narcissiflorum

Alliumoside

Allium narcissiflorum

glc Alliogenin (0, gW3@-OH) Diosgenin (32). glc-glc-3glc-(3&OH); glc-@-OH) Diosgenin (32). rha-4rha-4rha-6gal-6Blc-(3B-OH); glc-(26-OH) Diosgenin (32), rha-rha-$&z >&lc<3&OH); gl~_(26Xr:)~ Diosgenin (32). glc-rha-rha-6glc -

85 a6

86

86

Alliumoside

Allium narcissifloncm

86 )&tlc_(3&OH);

ASP-IV, 165-167 - 23 (MeOH) ASP-V, 150-156 (dec), - 45.5 (MeOH)

Asparagus cochinchinensis Asparagus cochinchinensis

glc glc-(26-OH) Sarsasapogenin (27) xyl-glc-Q/&OH); glc_(26-OH); (22-OMe) Sarsasapogenin (27). rha-6glc-(3&OH); glc_(26_OH); (22-OMe)

I9 19

964
Table l-continued Saponins ASP-VI, (mp, [&)

S. B. MAHATO,A. N. GANGULY and N. P. SAHU

Source
Asparagus cochinchinensis

Structure Srasasapogenin &-(3g-OH); (27), glc-(26-OH); (27). glc-f26-OH); (22-OMe) (22-OMe)

Reference 19

165-168 (dec),

- 50 (MeOH) ASP-VII, 179-181 (dec), - 27 (MeOH)


Asparagus cochinchbwnsis

>

XYl Sarsasapogenin rha


xylf 44

19

glcO@OH);

Asparagoside Asparagoside Asparagoside

A B D

Asparagus

0fEcinalis
Asparagus oficinalis Asparagus

dc Sarsasapogenin gw38-OH) Sarsasapogenin dc-wOH) Sarsasapogenin glc >kdc-c3/3-oH)

(27). (27). (87).

87 87 88

oficinalis

Asparagoside

Asparagus

oflicinalis

glc Sarsasapogenin dc >!c_(38_OH);

(27).

88

glc-W-OH)
89

Asperin, 222-231. - loo (pyridine) Asperoside

Smilax opera

dc Yamogenin rha-rha

(48).

1. ,&_(38-OH) Smilax aspem rha Yamogenin rha-%a (48), gL(26-OH) 90


89

>kdc_(38_OH); Aspidistrin, 265-267, - 65


Aspidistra elatior

rha Diosgenin (32). ac >&logal-(3&OH)

Avenacoside

Avena sativa

XYl Nnatigenin rha

(48). glc-(26-OH)

91

)Wc-(3&OH): Avenacoside B
Avena sativa

glc Nuatigenin

(48), glc-(26_OH)

92

rha-$_(3&OH); Balanitiscin A, 274278, - 39


Balanites roxburghii

dc-*glc Diosgenin (32). rha ):glc-(38-OH)

93

Capsicoside,

295.

Capsicum

annum

glc Gitogenin glc

(4). glc-(26OH)

94

- 35 (CHClr + MeOH) Capsicosin


Capsicum

>&k-$aL3glc-(3~-OH); annum glc Gitogenin (4). glc >&c-4gal-3glc-(3g-OH)

94

Convallamaronin, 215-218. - 30 (MeOH)

Convallaria

majalis

glc Convallamarogenin (4fl). rha-(3g-OH); rha-qui-(l&OH)

95

Steroid sapottins Table l-continued

965

SaPonins (mp, MD)


Convallamaroside

!3OUrCC

Structure Convallamarogenin (4ft), gic-rha_(3/3_OH);rha-*qui-(l&OH): glc_(26-OH) Convallagenin A (29). ara-(3&OH) Convallagenin B (30). ara-(5@OH) Isorhodeasapogenin (20, rha-rha-*ara_(3&OH) Rhodeasapogemn (28). glc-(l@OH); rha-2xyl-3rha-(3g-OH) Diosgenin (32). ara-*am-*ara-(3&OH) Cryptogenin (41). gW3WH) Tigogenin (3),
XYl
13

Reference 95

Convallaria

majalis Convallasaponin A. 238-M. - 400 (CHCis) Convallasaponin B, 273-274, - 56 (CHC&+ MeOH) Convallasaponin C, 218-221. - 89.7 (CHCIa+ MeOH) Convallasaponin D, 264-265. - 66 (MeOH) Convallasaponin E, 213-217. - 149 Cryptogenin glycoside, 238-241 (dec), - 129(EtOH) Degalactotigonin, 284-286. - 64 (pyridiie)
Convallaria keisukei

% % 91 98.99 100 18 6, 101

Convallaris keisukei
Convallaria

keisukei
Convallaria keisukei Convallaria kcisukei Paris tetraphylla

Digitalis pwpuna

,2glc-gal_(3&OH)

BlC
Deglucoderhamnoruscin Deglucodigitonin
Ruscus aculteatus LXgitalis purpurea

A5-Convallamarogenin (40, ara-(l&OH) Digitogenin (12), xyt >&lc&al~3g-OH,

103 184

Deglucoruscin Deglucoruscoside Dehydrocryptogenindiglycoside, 265-268 (dec), - 80 (pyridine) Dehydrocryptogenintetraglycoside

Ruscus aculeatus Ruscus aculeatus Trillium

kamtschaticum

gal A-Convallamarogenin (46). rha-zara-(l&OH) As-Convallamarogenin (40, rha-*ara-(l&OH); glc-(26-OH) 17(20)-Dehydrocryptogenin (42), rha-*glc_(3S-OH); glc-@-OH) 17(20)-dehydrocryptogenin (42). rha-rha )&_(3g_OH); glc_(26-OH)

103 105 18

Paris tetraphyl~a

18, 106

Deltonin

Dtoscorca

deltoidea

rha Diosgenin (32). dc >&lc43&OH) rha Diosgenin (32). dc 14 ,&-(3g-OH);

107

Dioscorea ddtoidea

108 glc-(26-OH) 109 110

Desghtcodesrhamnoparillin. - 65.5 (CHCI, + MeOH) Desghrco-lanatigonin, 246-251, -47.6 (CHCl3+ MeOH)


250-265.

Smilax aristolochiaefolia Digtialis lanata

rha Sarsasapogenin (27) glc-glc-(3S-OH) Tigogenin (3), gal )$glc-gal~3S_OH)

Desglucoparillin,
250-265. - 67.5

(EtOH)

Smiiax aristolochiaefolia

xyl Sarsasapogenin (27). Blc ):glc_(3S-OH) rha Digalogenin (9) Blc-gal

109

Digalonin, 25tX295

LXgitalis purpurea

6, 104

S. B. MAHATO, A. N. GANGULY and N. P. SAHU Table l-continued Saponins (mp, [aln) Source
Digitalis purpurea

Structure Digitogenin
gk-pl

Reference 104

(12).

24j-285;

- 40 (pyridine)
Digitalis lanata

Dioscin, 2X-27?*, - 115 (EtOH)

Diosgenin-3-Orhamnoside Diosgenin trighrcoside, 290 (dec), - 77 (pyridine)

Costus speciosus, Dioscorea septemloba, Paris polyphylla, Solanum introsum, Tribulus term&s, Trigonella foenumgraecum, Trillium tschonoskii Smilax excelsa

Diosgenin (32). rha )&<3&OH) rha

111-119

Dioscorea
deltoidea

Diosgenin (32). rha-Q&OH) Diosgenin (32), gtc )$lc-O&OH) Blc

120 121

Epidiosgeninghrcoside, 2%221, - 122 Epimetageninglycoside, amorphous, - 154 (CHCI,) Epiruscogeninghrcoside Episceptrumgeninghrcoside, 236-238, - 109 Eruboside B

Gynura japonica Metanarthecium luteo- uiride

Senshokushichiken (Chinese name) Gynura japonica


Allium erubescens

Epidiosgenin (38). glc-(3n-OH) Epimetagenin (22). (tri-OAc)ara-(lla-OH), 2g-OAc Epiruscogenin (39), glc-(3a-OH) Episceptrumgenin (47). glc-(3a-OH) g-Chlorogenin (11), .& >~1c-ga1-(3@0H)

122 123 124 122 125

Filiferine A, 292. - 50.5 (DMSO) Filiferine B, 319-321, - 35 (DMSO) Floribundasaponin B, 251-253 (dec), - 86:5 (pyridine) Floribundasaponin C, 255-258. - 93.6 (pyridine) Floribundasaponin D, 232234, - 85 (pyridine) Floribundasaponin E, 226-229 (dec), - 66 (pyridine) Floribundasaponin F, 243-247 (dec), - 74.6 (pyridine) Funkioside B, 258-266. - 135 (MeOH) Funkioside C Funkioside Funkioside Funkioside D E F

Yucca jihfera Yucca filifera

Dioscorea
floribunda Dioscorea fionbunda Dioscorea floribunda Dioscorea floribunda Dioscorea jloribunda Funkia ovata Funkia ovata Funkia ovata Funkia ovata Funkia ovata

glc Sarsasapogenin (27). xyl-gal-(3p-OH) Sarsasapogenin (27), glc-*gaL(3/3-OH) Pennogenin (36). rha-glc-(3@-OH) Diosgenin (32), rha-rha-glc-(3@OH) Diosgenin (32). rha-3rha-3rha-3rha-glc-(3g-OH) Diosgenin (32). rha-3rha-3rha-3rha-glc-(3&OH); glc_(26-OH); (22a-OMe) Diosgenin (32). rha-%ha-3rha-3rha-4glc-(3/3-OH); glc-(ZCOH) Diosgenin (32), glc-(3g-OH); glc-(26-OH) Diosgenin (32), glc-gal-(38-OH) Diosgenin (32). glc-*glc-gal-(38-OH) Diosgenin (32), rha-glc-glc-gal-(3@-OH) Diosgenin (32), g)c )fglc-gal-(3g-OH) XYl

126 126 127 128 128

128

128

129 129-131 129-131 129, 130, 132 129, 130

Steroid

saponins

%7

Table l-continued Saponins Funkioside G (mp, [alo) Source Funkia ovata Structure Diosgenin (32). rha-glc Reference 129, 130, 132

Funkioside

Funkia ovata

Diosgenin (32), rha-rha xy,)~lc-zglc-4gal_(3~-OH); gic-(26OH) Diosgenin (32). rha >&lc-c3@OH); gIc_(26-OH)

129, 130

Furostanol 189-193

bisglycoside,

Tribulus terrestris, Trigonella coerulea

133-13s

Furostanol 242-246

glycoside,

Trigonella joenum-graecum

rha Neotigogenin rha )~c_c3s-

(13). OH); glc-(26-oH): (22-OMe)

tdc
Furostanol saponin, 217-220 (dec), - 24 (CHCls + MeOH) Furostanol saponin-1 Lycopersicon
esculentum Asparagus oficinalis

Neotigogenin (13). glc-*gl~-~gal-(3~-OH);

Furostanol

saponin-2

Asparagus oficinalis Digitalis purpurea

F-Citonin, 251-255 (dec), -66O (pyridine)

Gitonin, 276.5-282.5

Digitalis lanata

Glucoconvalla-saponin A, 213&O (MeOH) Glucoconvalla-saponin B, 221-222. - 35 (MeOH) Glycoside A (identical to Kallstroemin E) Glycoside B Glycoside B

Convallaria keisukei Convallaria keisukei Dioscorea prazeri Dioscorea prazeri Trigonella foenum-graecum

Glycoside

Allium

Glycoside C, 272-274, - 87 Glycoside D, 278-280. - 85 Glycoside I, 300-303 Glycoside 297-3W, II, - 84 (pyridine)

narcissif7orum Discorea prazeri


Dioscorea prazeri Methanarthecium luteo-viride Methanarthecium luteo-viride

968 Table l-continued Saponins Glycoside III (mp. [alo)

S. B. MAHATO, A. N. GANGIJLY and N. P. SAHU

Source
Methanarthecium lureo-viride Costus speciosus,

Structure Nogiragenin (25), gal-(lla-OH) Diosgenin (32), rha )!&_(3B_OH) plc

Reference 143 111-113 118. 134, 144

Gracillin, 29@293, - 88 (pyridine)

Dioscorea

seplemloba,

LXoscorea caucasica, Tribulus rewestris Solanum hispidum Solanum hispidum

Hispigenin Hispinin A, 220-224. Hispinin B, 258-260. Hispinin C, 2%288, Kallstroemin 235-238, Kallstroemin 232235, -

glycoside

44 (pyridine)
Solanum hispidum

68 (pyridine)
Solanum hispidum

SSP (pyridine) A, 82 (pyridine) B, 79.5 (pyridine)

Kallstmemia pubescens Kallstmemia pubescens Kallsfmemia pubescens Kallstmemia pubescens Allium karataviense Allium spp .

Kallstroemin D, 275-276. - 94.5 (pyridine) Kallstroemin E, 218-219, - 101 (pyridine) Karatavegenin B, glucoside. 294-298 Karatavioside A

Hispigenin (4% rha-rha_(3&OH) Solagenin (a), rha_(6a-OH) Solagenin (18). rha-%ha_(6a-OH) Neochlorogenin (II), rha-rha_(6a-OH) Diosgenin (32), rha-%ha-%a-glc-(3&OH); Diosgenin (32), rha-2rha-%ha-6glc-(3&OH); (22a-OMe) Diosgenin (32), rha-%ha-%ha-6glc_(3&OH) Diosgenin (32). rha-6glc-(3&OH) Karatavegenin (5). gIc-(36-OH); gIc_(26-OH) Yuccagenin (34), XYl )&&al-(3/3-OH)

145 146 146 146 147 gl~-(26-OH) 147 glc-(26_OH); 147 147 148 149

Karatavioside

ANium spp.

glc Yuccagenin XYl

(34). glc-(26-OH)

150

>&lc-gal_(SB-OH): Kikuba saponin, 249-251. - 77O (MeOH)


Dioscorea septemloba, Tnbulus rerresMs

glc Diosgenin (32), glc-*glc >jcsa-OH)

113. 134

Lanadigalonin

Bgitalis

lanata

rha Digalogenin glc-gal

(9),

151

)&@gal-(3~-OH) XYl Gitogenin (4), glc-gal )fgl&al_(3~-OH): Lanatigonin I, 275-285 (de@, + 42 (pyridine) Digitalis lanato XYl Tigogenin (3), glc-gal >&IoBalO@-OH) Lanatigoside
Digitalis lanata

Lanagitoside

Digitalis lanara

110 glc_(26-OH) 151

XYl Tigonenin (3). glc-gal >:glc-gal-(3fl-OH):


XYl

110 glc_(26-OH) 152

Metanartheticum prosapogenin

Metanatihecium luleo- viride

Z&acetyl metagenin (23), 2,3,4-tri-O-acetyl ara_(lla-OH)

Steroid saponins Table l-continued

%9

Sawnins(mp, [eld
Molluscicidal saponin-1,24&245 (dec), - 68.5 Mulluscicidal saponin-2,286-288O Molluscicidal saponin-3, 320-322 Neochlorogenin glycoside Neohecogenin glucoside 280-282(dec), - 41 (pyridine) Neotokoronin, 270-274(dec), - 11(pfidine) Ophiopogonin A, 183. - 98 (pyridine) Ophiopogonin B, 269-271. - 105 (pyridine) Ophiopogonin D, 263-265, - 108 (pyridine)

source
Comusjkwida Comus florid0
Comus firida Solanum Tribulus Dioscorea Ophiopogon Ophiopogon hispidum rcnwtris tenuipes

Structure Sarsasauogenin (27).


gaM3&OH)

Reference 22 22 22 145 153 154 155 155, 156 155, 157

japonicus japonicus
japonicus

Ophiopogon

Sarsasapogenin (27), xyl-*gal-(3~-oH) Sarsasapogenin (27). gic-*gaL(3/3-OH) Neochlorogenin (18, rha-rha-(3@OH) Sisalagenin (19), gW3bOH) Neotokorogenin (31). ara-(l&OH) Ruscogenin (33). (3-0-acetyl) rha-%co~lfi-OH) Ruscogenin (X3), rh&uco-(lfi-OH) Ruscogenin (33). rha >$fuco-(l&OH) xyl Diosgenin (32). (4-0-acetyl) rha >bW3a-oH)
XYl

Ophiopogonin B, 245-248(dec), - 86 (pyridine)

Ophiopogon

japonicus

158

Ophiopogonin C, 238-W (dec), - 99 (pyridine) Ophiopogonin D, 255-25T, - 41 Wridine)

Ophiopogon

japonicus

Diosgenin (32). rha-*glc-(3p-OH) Diosgenin (32). xyl )&c-(3@-OH) rha Paniculogenin (15). xyCqui_(6u-OH) PanicLogenin (is, rha-qui-(6a-OH) Paniculogenin (15). xyl-rha-(6a-OH) Paniculogenin (U), rha-rha-(3&OH) glc rhh>:$dc-(3B-OH) Diosgenin (32), rha-ara-glc-(3p-OH) Diosgenin (32). glc-rha >&c-c3WH) rha Diosgenin (32). glc-rha >:glc-(3fl-OH) ara (fur) Diosgenin (32). rha-glc-(3p-OH) Pennogenin (jr), rha ):&_(3&OH) rha

158

Ophiopogon

japonicus

158

Paniculonin A, 262-264. - 61 (pyridine) Paniculonin B, 237-238. - 79 (pyridine) Paniculogenin glycoside, 262-264. - 61 (pyridine) Paniculogenin glycoside Parillin, 22&223, - 64 (EtOH) Paryphyllin, 294-298. - 104(pyridine) Paryphyllin A, 212-214. -85 (pyridine) Paryphyllin B, 168-17Oe,-97.5 (pyridine)

Solanum Solanum Solanum Solomon

paniculatum panicularum paniculatum hispidum

159 160 160


145

109

Smilax aristolochiaefolia Paris polyphylla Paris polyphylla

161 162

Paris polyphylla

162

Paryphyllin C, 262266, - 97 (pyridine) Pennogenin chacotrioside, 297-299(dec), - 127 (pyridine)

Paris polyphylla Ttillium kamrscharicum

163 18

970 Table I-continued Saponins (mp, [alo)

S. B. MAHATO,A. N. GANOULY and N. P. SAHU

Source TMium kamtschoticum Heloniposis orientalis

Structure Pennogenin (jr), rha-*glc(3&OH) Pennogenin (jr), rha-rha >&-(3fl-OH)

Reference 18 -

Pennogenin diglycoside, 273-276 (dec), - 118 (pyridine) Pennogenin tetraglycoside, 224-228 (dec), - 136 (pyridine)

18, 106, 117

Polygonatoside

Prazerigenin glucoside, 260. - 79 (pyridine) Protodioscin, 1904% (dec), - 57.8 (pyridine)

Polygonatum latijolium Dioscorea prazeri

rha Diosgenin (32), glc-3glc-4gal-3glc43~-OH) Prazerigenin A (37). glc-(3&OH) Diosgenin (32), rha > &lc-(3/3-OH); gb(26-OH)

164 121

LXoscorea gracillima

165

Protogracillin, 235-238 (dec), - 57.8 (pyridine)

Doscorea septemloba

rha Diosgenin glc

(32), glc-(ZCOH)

165

)&(3p_OH); Metanatihecium luteo-viride Polygonatum latifolium Dioscorea tokoro Yucca filamentosa Yucca filamentosa

Protometeogenin glycoside, 265-270 Protopolygonatoside

Prototokorin, W-178, - 3.8 (MeOH) Protoyuccoside C, 182WV, - 30 (MeOH) Protoyuccoside E

rha Protometagenin (24), ara-(1 la-OH) Diosgenin (32), glc-3glc-4gal-3glc-(3fl-OH); glc-(26-OH) Tokorogenin (21). glc-(l~3-OH); glc-(26-OH) Sarsasapogenin (27), gal-2glc-4glc-(3~-OH); glc-(26-OH) Sarsasapogenin (27), gal >&lc-&-(Jg-OH); glc_(26-OH)

166 164 167 168 169

Rockoside Rockoside Rockoside Ruscin Ruscoside

A B C

Agave americana Agave ameticana Agave americana Ruscus aculeatus Ruscus aculeatus Paris polyphylla

Saponin P-a, 276-278 - 133

gal Rockogenin (lo), gal-(3&OH) Rockogenin (lo), glc-gal-(3&OH) Rockogenin (lo), xyl-*glc-glc-gal_(3@OH) A-Convallamarogenin (40, glo3rha-*ara-(l@OH) A-Convallamarogenin (46), glc-rha-*ara-(l/3-OH); glc (26-OH) Diosgenin (32), rha >&Jc-(3p-OH)

170 170 170 103 105 116, 161

Saponin P-d, 203-206, 153

Paris polyphylla

(fur)ara Diosgenin (32), rha-rha

116

Sarsaparilloside, amorphous, - 44 (HzO)

Smilax aristolochiaefolia

Sarsasapogenin glc rha>&lc-(3&OH); glc

(27). gk-(26-OH)

32,33

Taccaoside

Taccacheancer

Diosgenin (32), rha , /* rha lc43&OH)

171

Steroid saponins Table l-continued Saponins (mp. [aln) Source


Lycoperscicum

971

structure Neotigogenin (U), dc-*gic-gaM3WH); Tiigenin (3),

Reference 172 Blc-WOH) 6. 104

TFT, 217-220, - 24 (MeOH + CHCl,) Tiionin

esculmtum Digitalis lanata


Digitalis purpureo

lwm
>W-gaW3g-OH) xyl Sarsasapogenin gal-(3j?-OH) (27). 173

Timosaponin A-I, 240-245 (dec), - 68 (dioxan) Timosaponin A-III, 320-322 Tokorogenin glucoside, 275-284, - 43 (CHCI,) Tokoronin, 27%277, - 13 (pyridine) Tribulosin, > 300. - 61 (pyridine) Trigonelloside C

Anemarrhenoe asphodeloides Anemarrhenae asphodeloides Dioscorea tokoro Dioscorea tokoro Tribulus terrestris

Sarsasapogenin 07). glc-$gal_(3g-OH) Tokorogenin (21). gh=US-OH) Tokorogenin (21). ara-(lg-OH) Neotigogenin (13). xyl >fglc-+36-OH) /ha xyl Yamogenin 40). rha )jglc_(3&OH); gM26-OH)

173 174 175 153

Trigonella joenum-graecum

176

Trillenoside A, 269-220 (dec), - 142

Trillium kamtschaticum, Trillium small, Trillium eschonoskii

rha Trillenogenin apio(fu+rha

(44). )$ua-(lg-OH)

34-36

Trillin, 260, - 89 (dioxan) Trillioside A Trillioside B

saliva, Polygonotum lotijolium Trillium kamtschotscense Trillium komtschatscense

Dioscorea

xyl Diosgenin (32). glc_(3g-OH) Diosgenin (32), glc-rha-*glc-(3~-OH) Diosgenin (32). glc >&lcd3&OH,

177, 178 179 180

Turoside

Allium turcomanicum

glc Neoagigenin xyl

(16).

181

)&zlc-gal_(3g-OH) Turoside bcnzoate A-6-0Allium turcomonicum

glc Neoagigenin (16). xyl 13 ,,&-gal-(3g-OH); glc Neoagigenin glc-*glc

182 6-0-benxoate

Turoside

Allium turcomanicum

(16). glc-(26_OH)

183

):glc&l_(3g-OH): Yononin,
238-240. - 14

Dioscorea glycoside B C,
- 41

tokoro

Yuccagenin Yuccoside Yuccoside


282-284.

Yucca schottii Yucca jilamentoso Yucca filamentosa Yucca jilamentosa

Yuccoside

xyl Yonogenin (28). ara-(Zg-OH) Yuccagenin (jr), gal_(38-OH) Tigogenin (3) gal-glc-(3g-OH) Sarsasapogenin (27). gal-*glc-glc-(3&OH) Sarsasapogenin (87). gal\ ,$glc-&_0,9_OH) gal

184, 185 37 186 168. 187-189 188,190

Abbreviations galactopyranosyl; apiofuranosyl.

used: glc, g - D - glucopyranosyl; rha, a - L - rhamnopyranosyl; ara, (I - L - arabinopyranosyl; gal, g - n xyl, g - D - xylopyranosyl; ara -fur, n - L - arabinofuranosyl; qui, B - D - quinovopyranosyl; api -fur, g - o -

972

S. B. MAHATO,A. N. GANGULY and N. P. SAHU Table 2. Steroidal saponins whose genins and sugars have been identified Saponins (mp, [alo) Amolonin Asparagoside C, 287-2W, - 130 (MeOH) Balanitscin B Balanitscin C Balanitscin D Balanitscin E Caucasosaponin, 218-220 (dec) - 62.5 (pyridine) Dioscinin, 202-203, - 70 (MeOH) Diosgenin glycoside Diosgenin glycoside Diosgenin rhamnoghlcosyl Fenugrin B Graecunin B, 15b156, - 47 (MeOH) Graecunin C Ophiopogonin C, 238-240, - 93 (pyridine) Polygonatoside C Polygonatoside Polygonatoside Ruscoside A Ruscoside B Saponin C, 187 Saponin D,, 272 Saponin of kammogenin Sarsasapogenin glycoside, 285, - 35 (EtOH) Sarsasaponin, 245 Tigogenin glycoside, 260 (dec) Tigogenin glycoside Terrestroside F, 238-240 Triharin, 21 l, - 116 (EtOH) T. T. Saponin E G Source Chlorogalum pomeridianum Asparagus oficinalis Balanites roxburghii Balanites roxburghii Balanites roxburghii Balanites roxburghii Dioscorea caucasica Genins and sugars Tigogenin (3), glc (3) + gal (1) + rha (2) Sarsasapogenin (27), Blc Diosgenin (32), gic + rha Diosgenin (32), glc + rha (1: 3) Diosgenin (32), glc + rha Diosgenin (32), gk+ara+xyl+rha Diosgenin (32), rha (1) + glc (3) Diosgenin (32), glc (2) + rha (2) Diosgenin (32), glc+glc Diosgenin (32), glc+gat+xyl Diosgenin (32), glc + rha Diosgenin (32), glc + ara + rha Diosgenin (32), glc + xyl + rha Diosgenin (32), glc + rha Ruscogenin (33), fuc + xyl+ rha Diosgenin (32), glc + gal Diosgenin (32). glc + gal + xyl Diosgenin (32). glc + gal + xyl + ara Ruscogenin (33), gal + glc + rha (2) Ruscogenin (33), gal + glc + ara + rha (2) Ruscogenin (33), rha + glc + ara Diosgenin (32), rha + glc Kammogenin (35). 5 units of deoxyribose Sarsasapogenin (27), ara+glc+gal+xyl Sarsasapogenin (37), glc (2) + rha (1) Tigogenin (3), xyl + glc + gal Tigogenin (3), glc+gai+xyl+rha Tigogenin (3), gk + rha Diosgenin (32), glc (2) Diosgenin (32), glc + ara + rha Reference 11 191 192 192 192 192 144

Dioscorea polystachya Tribulus terrestris Polygonatum multifiorum Tribulus terrestris Trigonella foenum graecum Trigonella foenumgraecum Trigonella foenumgraecum Ophiopogon japonicus Polygonatum latifolium Polygonatum latifolium Polygonatum latifolium RUSCUS hyrcanus Ruscus hyrcanus Tribulus terrestris Tribulus terrestris Yucca schotti Narthecium essifragum Smilax aristolochiaefolia, Yucca schottii Cestrum diumum Yucca glorisa Tribulus terrestris Trillium erectum Tribulus terrestris

193 134 194 195 1% 197 198 158 178 178 178 199 199 200 200 37 201 11 202 203 204 11 205

Steroid saponins Table 3. Basic steroid saponins (characterized and uncharacterized) isolated after 1972 Saponin (mp,
b]D)

973

Source

Genins and sugars Solanidine (49),

Reference 206

Dehydrocommersonine

Solanum chacoense

fk
Khasianine, 226-228, - 95 (MeOH) Solapersine, 282-2&W, - 46 (MeOH) Solaplumbin, lNL181, -90 Solaplumbinin, 184-185, - 39.5 Solasodine glycoside Solasodine glycoalkaloid Solatifoline, 292293, - 119

Solanum khasianum Solanum persicum Nicotiana plumbaginijolie Nicotiana plumbaginijolie


Unidentified solanum species (Spanish name: noranjilla de Jibaro)

Solasodine (SO), rha-glc-(3p-OH) Solasodine (50). gal+glc+xy1 Solasodine (SO), glc-rha-(3B-OH) Solasodine (SO), rha-(3B-OH) Solasodine (50), glc+gal+rha Solasodine (50), glc + rha Solasodine (SO), glc+rha+gal

63 207 208 208 209

Solanum schimperianum Solanum platanijolium

210 211

The steroidal saponins isolated and characterized up to 1980 are listed in Table 1 along with the mps and specific rotations and Table 2 shows the steroidal saponins which have not been fully characterized. As comprehensive reviews [M-171 of basic steroidal saponins are available, the characterized and uncharacterized basic steroidal saponins isolated after 1972 are compiled in Table 3.
BIOLOGICAL ACTIVITY

An extensive study of the physical, chemical and physiological properties of saponins has been conducted owing to their wide occurrence in nature. There are several excellent reviews on the properties of saponins [6-l 1, 141 and on tomatine [15]. Saponins, in general, are very powerful emulsifiers, toxic, haemolytic and able to form complexes with cholesterol. Here information on the biological activities of various saponins, particularly the steroidal saponins, reported durjng the period 1972 to 1979 is given. Action on metabolism Saponins (1%) in the diet of rats decreased the plasma cholesterol level and increased bile acid production [212]. The depression of growth in vitro caused by complex formation of saponin with fatsoluble vitamins has been studied [213]. A change in the thyroid gland in experimental haemolytic anaemia has been observed [214] when subcutaneous injection of saponin at doses of 1, 4 and 8 mg/kg once every third day is given to rabbits. The development of proteins, carbohydrate and lipid dystrophy in the liver of rabbits is prevented by the oral administration of Tribulus terrestris saponin at 10-15 mglkglday for 90 days with the simultaneous administration of cholesterol (200 mg/kg/day) [2151. Certain steroidal saponins isolated from egg-plant, which contain mainly tigogenin and neotigogenin as aglycones, partially normalize lipase activity in the mitochondria

and increase cholinesterase activity in the cytoplasm [216]. The Na+ or K activated ATPase in rabbit red blood cell membranes is inhibited by low concentrations of saponin but activated by high concentrations while ouabain, a cardiac glycoside, inhibits the activating effect [217]. The effect of digitonin on glucose uptake by isolated fat cells in the presence or absence of insulin was studied by Akhtar and Perry [218] who observed that low concentrations of saponin inhibited the stimulation of glucose uptake by insulin without causing severe cell damage suggesting digitonin-cholesterol complex formation in the fat cell plasma membrane. Action on the cardio-vascular system The cardiotonic actions of g-strophanthin (0.15a-solanine (2.5-5 mg/kg) and T.T. 3.25 mg/kg), saponin were studied on a comparative basis. gStrophanthin and T.T. saponin decreased the frequency of cardiac contraction whereas a-solanine had no effect 12191. Cardiotonic activity of some glycoalkaloids, when compared with K-strophanthoside by the use of isolated frog heart, is found to be directly related to the nature of the aglycone and the number of sugar units [220]. Saponin isolated from the seeds of Achyranthes aspera is found to increase the force of contraction of isolated frog heart, guinea-pig heart and rabbit heart [221]. Two new steroidal saponins ruscoside A (ruscogenin + 1 glc + 1 gal + 2 rha) and ruscoside B (ruscogenin + 1 gal+ 1 glc +2 rha+ 1 ara) isolated from Ruscus hyrcanus [ 1991 exhibit various biological activities. They decrease the cholesterol content of the blood, lipid deposition in the aorta and liver arterial tension. They also slow down the cardiac rhythm and respiration of humans and rabbits suffering from arteriosclerosis. Ruscoponin and ruscogiponin from R. penticus and R. hypophyllum exhibit fibrinolytic activity in oitro at 0.1 and 0.25% concentration, respectively. Ruscoponin

974

S. B. MAHATO,A. N.

GAN~ULY N. P. SAHU and


REFERENCES 1. Vogel, G. (1%3) Planta Med. 11,362.

has a thrombolytic effect in dogs when given intravenously but no effect when given intramuscularly
[222]. Antimicrobial activity

2. Tschesche, 3.
272. Kochetkov,

R. and Wulff, G. (1964) PIuntu Med. 12, N. K. and Khorlin, A. J. (1966) Anneim.

Saponins are generally good antifungal and antibacterial agents. The antifungal activity is found to be more effective with saponins than the sapogenins and the acetylated saponins, the activity being highly influenced by the number of component monosaccharides and their sequence. Digitonin has a considerable fungistatic activity [223]. Strong fungistatic action was observed with saponins when added to the culture medium at 31.242.5 pg/ml [224]. Digitonin and tomatin caused considerable leakage of free amino acids from the mycelium of Botrytis cinerea and Rhizoctonia solani [225]. Deltonin and deltoside isolated from Dioscorea deltoidea have a fungitoxic effect on the growth of Fusarium solani conidia and Phytophthora infestans [226]. Saponins from common ivy [227] are more active against Gram positive bacteria than gram negative ones with a minimum inhibitory concentration of 0.312-1.25 mglml. The growth of Bacillus mycoides was inhibited by the saponins extracted from Allium atroyiolaceum, Saponaria viscosa, Caltha palustris and Verbascum
aureum [228]. Action on the reproductive system Saponins from Costus speciosus

4. Kawasaki, 5. Tschesche, 6. Kawasaki, I. Tschesche,

8.

T. (1967) Sogo Rinsyo 16, 1053. R. (1971) KagakunoRyoiki26,571. T. (1978) Method Chim. 11.87. R. and Wulff, G. (1973) in Portschritteder Chemie Organischer Naturstofe (Herz, W., Grisebach, H. and Kirby, G. W. eds.) Vol. 30, p. 461. Springer, Berlin. Basu, N. and Rastogi, R. P. (1%7) Phytochemistry 6,

Porsch. 16, 101.

9. Agarwal, S. K. and Rastogi, R. P. (1974) Phytochemis10. Chandel, R. S. and Rastogi, R. P. (1980) Phytochemistry 19, 1889. 11. Elks, J. (1971) Rodds Chemistry of Carbon Compounds (Coffey, S. ed.) 2nd edn, Vol. IIE, p. 1. Elsevier, Amsterdam. 12. Elks, J. (1974) in Rodds Chemistry of Carbon Compounds (Ansell, M. F. ed.) Supplement to the 2nd Edition, Vol. 2D, p. 205. Elsevier, Amsterdam. 13. Takeda, K. (1972) in Progress in Phytochemistry (Reinhold, L. and Liwschitz, Y. eds.) Vol. 3, p. 287. Interscience, New York. 14. Schreiber, K. (1%8) Alkaloids(London) lo, 1. IS. Roddick, J. G. (1974) Phytochemistry 13, 9. 16. Herbert, R. B. (1975) in Alkaloids. Specialist periodical reports (Sazton, J. E. ed.) Vol. 5, p. 256. The Chemical Society, London. 17. Harrison, D. M. (1976) in Afkoloids. Specialist periodical reports (Grundon, M. F. ed.) Vol. 6, p. 285. The Chemical Society, London. 18. Nohara, T., Miyahara, K. and Kawasaki, T. (1975) Chem. Pharm. Bull. 23,872. 19. Konishi, T. and Shoji, J. (1979) Chem. Pharm. Bull. 27, 3086. 20. Ogihara, Y., Inoue, O., Otsuka, H., Kawai, K. I., Tanimura, T. and Shibata, S. (1976) J. Chromatogr. 128, 218. 21. Tanimura, T., Pisano, J. J., Ito, Y. and Bowmann, R. L. (1970) Science 16954. 22. Hostettmann, K., Hostettmann-Kaldas, M. and Nakanishi, K. (1978) Helu. Chim. Acta 61, 1990. 23. Yahara, S., Kaji, K. and Tanaka, 0. (1979) Chem. Pharm. Bull. 27, 88. 24. Yahara, S., Tanaka, 0. and Nishioka, I. (1978) Chem. Pharm. Bull. M,3010. 25. Otsuka, H., Kobayashi, S. and Shibata, S. (1978) Planta Med. 33, 152. 26. Simpson, C. F. (1978) Practical High Performance Liquid Chromatography. Heyden, London. 27. Beasley, T. H. (Sr)., Ziegler, H. W. and Bell, A. D. (1979) J. Chromatogr. 175, 350. 28. Kimata, H., Hiyama, C., Yahara, S., Tanaka, O., Ishikawa, 0. and Aiura, M. (1979) Chem. Pharm. Bull. 27, 1836. 29. Marker, R. E. and Lopez, J. (1947) J. Am. Chem. Sot. 69, 2389. 30. Kiyosawa, S., Hutch, M., Komori, T., Nohara, T., Hosokawa, I. and Kawasaki, T. (1%8) Chem. Pharm. Bull. 16, 1162.

1249.

try 13,2623.

have shown varied and interesting biological activities. They have a stimulating effect [229] and anti-inflammatory activity on uterus and they produced proliferative changes in both vagina and uterus showing a similar effect to that produced by stilbesterol [230,231]. Prevention of pregnancy in rats when fed saponin at 5-500 &lOO g body wt for 15 days has been reported [232]. An abortifacient effect has been shown by saponins from C. speciosus when given to pregnant goats, rats and cows [232]. A similar antifertility effect has also been reported in the case of the triterpenoid saponin isolated from Gieditschia horrida
[233].

Miscellaneous The haemolytic action of digitonin on human, pig

and bovine erythrocytes is found to be higher than tomatine while human erythrocytes are very resistant to parillin[234]. Saponins from rhizomes of wolfberry inhibit the medicinally induced sleep in mice [235].Two new steroidal saponins ruscoside A and ruscoside B isolated from Ruscus hyrcanus have antisclerotic and hypotensive activity [WI]. The anti-inflammatory activity on rat paw edema is displayed by saponins from Ruscus aculeatus [236]. There are reported adjuvant effects of saponins on vaccine against Foot and Mouth Disease [237,238]. Two sarsasapogenin glycosides isolated from Cornus florida 1221 were found to exhibit strong molluscicidal activity. Biomphalaria gfabaratus were killed within 24 hr by a 6 ppm solution of one glycoside and by a 12ppm solution of the other. A saponin isolated from Tribulus terrestris has been found to be useful as an antisclerotic agent [239].

Steroid saponins 31. Schreiber, K. and Ripperger, H. (1966) Tetrahedron Letters 5997. 32. Tschesche, R., Ludke, G. and Wulff, G. (1967) Tetrahedron Letters 2785. 33. Tschesche, R., Ludke, G. and Wulff, G. (1%9) Chem. Ber. 102, 1253. 34. Nohara, T., Nakano, A., Miyahara, K., Komori, T. and Kawasaki, T. (1975) Tetrahedron Letters 4381. 35. Kawasaki, T. Japan Kokai 77,51,011 (Co A 61 K 31/58) 23 April 1977. [Chem. Abstr. (1977) 87,65 4941. 36. Nohara, T., Komori, T. and Kawasaki, T. (1980) Chem. Pharm. Bull. 28, 1437. 37. Backer, R. C., Bianchi, E. and Cole, J. R. (1972) J. Pharm. Sci. 61, 1665. 38. Klyne, W. (1950) B&hem. J. 47, XLI. 39. Komori, T., Ida, Y., Mutou, Y., Miyahara, K., Nohara, T. and Kawasaki, T. (1975) Biomed. Muss Spectrom. 2, 65. 40. Komori, T., Tanaka, 0. and Nagai, Y. (1974) Org. Mass Spectrom. 9,744. 41. Higuchi, R., Komori, T. and Kawasaki, T. (1976) Chem. Pharm. Bull. 24, 2610. 42. Kasai, R., Matsuura, K., Tanaka, O., Sonada, S. and Shoji, J. (1977) Chem. Pharm. Bull. 25, 3277. 43. Krone, H. and Beckey, H. D. (1%9) Org. Mass Spectrom. 2,427. 44. Krone, H. and Beckey, H. D. (1971) Org. Mass Spectrom. 5, 983. 45. Brown, P., Pettit, G. R. and Robins, R. K. (1%9) Org. Mass Spectrom. 2,521. 46. Brunnee, Z. (1967) Z. Noturforsch. Teil B 22. 121. 47. Brown, P., Bruschweiler, F. R., Pettit, G. R. and Reichstein, T. (1970) J. Am. Chem. Sot. 92.4470. 48. Brown, P., Bruschweiler, F. R. and Pettit, G. R. (1972) Helv. Chim. Acta 55, 531. 49. Beckey, H. D. and Schulten, H. R. (1975) Angew. Chem. 14,403. 50. Beckey, H. D. (1977) Principles of Field-Zonization and Field-Resorption Mass Spectrometry. Pergamon Press, Oxford. 51. Schulten, H. R., Komori, T. and Kawasaki, T. (1977) Tetrahedron 33,2595. 52. Schulten, H. R., Komori, T., Nohara, T., Higuchi, R. and Kawasaki, T. (1978) Tetrahedron 34, 1003. 53. Schiebel, H. M. and Schulten, H. R. (1979) Tetrahedron 35, 1191. 54. Hinze, R. P., Schiebel, H. M., Lass, H., Heise, K. P., Gossauer, A., Inhoffen, H. H., Ernst, L. and Schulten, H. R. (1979) Justus Liebigs Ann. Chem. 811. 55. Komori, T., Kawamura, M., Miyahara, K., Kawasaki, T., Tanaka, O., Yahara, S. and Schulten, H. R. (1979) 2. Naturforsch. Teil C 314, 1094. 56. Macfarlane, R. D. and Torgerson, D. F. (1976) Science 191,920. 57. Kasai, H., Nakanishi, K., Macfarlane, R. D., Torgerson, D. F., Ohashi, Z., McCloskey, 3. A., Gross, H. J. and Nishimura, S. (1976) 1 Am. Chem. Sot. 98, 5044. 58. Anderson, W. R. Jr., Frick, W. and Daves, G. D. Jr. (1978) J. Am. Gem. Sot. 100, 1974. 59. Gorin, P. A. J. and Mazurek, M. (1975) Can. J. Chem. 53, 1212. 60. Yahara, S., Kasai, R. and Tanaka, 0. (1977) Chem. Pharm. Bull. 25, 2041. 61. Stothers, J. B. (1972) CurbonNMR Spectroscopy p. 461. Academic Press, New York. 62. Walker, T. E., London, R. E., Whaby, T. W., Baker, R.
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S. B. MAHATO, N. GANOULY A. and N. P. SAHU de Vivar, A. and Castillo, M. (1977) Carbohydr. Res. 55,113. 127. Mahato, S. B., Sahu, N. P. and Ganguly, A. N. (1981) Phytochemistry 28, 1943. 128. Mahato, S. B., Sahu, N. P. and Pal, B. C. (1978) Indian J. Chem. 16,350. 129. Kintya, P. K., Mashchenko, N. E., Kononova, N. I. and Lazurevskii, G. V. (1976) Khim. Prir. Soedin. 267. 130. Lazurevskii, G. V., Kintya, P. K. and Mashchenko, N. E. (1976) Dokl. Akud. Nauk. SSSR 230.476. 131. Mashchenko, N. E., Lazurevskii, G. V. and Kintya, P. K. (1977) Khim. Prir. Soedin. 123. 132. Kintya, P. K., Mashchenko, N. E. and Lazurevskii, G. V. (1977) Khim. Prir. Soedin. 69. 133. Bogacheva, N. G., Gorokhova, M. M. and Kogan, L. M. (1977) Khim. Prir. Soedin. 421. 134. Perepelitsa, E. D. and Kintya, P. K. (1975) Khim. Prir. Soedin. 11, 260. 135. Tomowa, M. and Gjulemotowa, R. (1978) Planta Med, 34, 188. 136. Hardman, R., Kosugi, J. and Per&t, R. R. (1980) Phytochemistry 19,698. 137. Sato, H. and Sakamura, S. (1973) Agric. Biol. Chem. 37, 225. 138. Kawano, K., Sato, H. and Sakamura, S. (1977) Agric. Biol. Chem. 41, 1. 139. Meena, W., Rajaraman, K. and Rangaswami, S. (1977) Indian J. Chem. 15,451. 140. Bogacheva, N. G., Sheichenko, V. I. and Kogan, L. M. (1977) Khim. From-Zh. 11,65 [Chem. Absrr. (1977) 87. 1806851. 141. Krohmalyuk, V. V. and Kintya, P. K. (1976) Khim. Prir. Soedin. 55. 142. Kitagawa, I., Imkwang, S. and Morii, Y. (1976) Chem. Pharm. Bull. 243114. 143. Yosioka, I., Morii, Y. and Kitagawa, I. (1973) Chem. Pharm. Bull. 21,2092. 144. Madaeva, 0. S., Ryzhkova, V. K. and Panina, V. V. (1%7) Khim. Prir. Soedin. 3, 237. 145. Chakravorty, A. K., Dhar, T. K. and Pakrashi, S. C. (1978) Tetrahedron Letters 3875. 146. Chakravorty, A. K., Saha, C. R. and Pakrashi, S. C. (1979) Phytochemistry 18,902. 147. Mahato, S. B., Sahu, N. P., Pal. B. C. and Chakravarty. R. N. (1977) Indian J. Chem. 15.445. 148. Khristulas, F. S., Gorovits, M. B. and Abubakirov, N. K. (1974) Khim. Prir. Soedin. 4, 530. 149. Vollermer, Yu. S., Gorovits, M. B., Gorovits, T. T. and Abubakirov, N. K. (1978) Khim. Prir. Soedin. 740. 150. Vollermer, Yu. S., Gorovits, M. B., Gorovits, T. T. and Abubakirov, N. K. (1980) Khim. Prir. Soedin. 355. 151. Tschesche, R. and Balle, G. (1963) Tetrahedron 19. 2323. 152. Yosioka, I., Imai, K. and Kitagawa, I. (1971) Tetrahedron Letters 1177. 153. Mahato, S. B., Sahu, N. P., Ganguly, A. N., Miyahara, K. and Kawasaki, T. (1981) Z, Chem. Sot. Perkin Trans. 1, 2405. 154. Akahori, A., Yasuda, F., Kagawa, K. and Iwao, T. (1973) Chem. Phann. Bull. 21, 1799. 155. Kato, H., Sakuma, S., Tada, A., Kawanishi, S. and Shoji, J. (1968) Yokugaku Zasshi 88,710. 156. Tada, A. and Shoji, J. (1972) Chem. Pharm. Bull. 26, 1729. 157. Tada, A., Kobayashi, M. and Shoji, J. (1973) Chem. Pharm. Bull. 21,308.

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