Medicinal Plant PDF

1. Introduction to Medicinal plants.
1.1. Introduction
Plants have been used for medicinal purposes long before recorded history. Primitive
men observed and appreciated the great diversity of plants available to them. Plants provide
food, clothing, shelter, and medicine. Much of the medicinal use of plants seems to be
developed through observations of wild animals, and by trial and error. As time went on, each
tribe added the medicinal power of herbs in their area to its knowledge base. They
methodically collected
information
on herbs and developed well-defined herbal
pharmacopoeias.1-2
Many drugs listed as conventional medications were originally derived from plants.
Salicylic acid, a precursor of aspirin, was originally derived from white willow bark and the
meadowsweet plant. Cinchona bark is the source of malaria-fighting quinine. The opium
poppy yields morphine, codeine and paregoric, a remedy for diarrhoea. Laudanum, a tincture
of the opium poppy, was the favoured tranquilizer in Victorian times. Even today, morphine
the most important alkaloid of the opium poppy remains the standard against which new
synthetic pain relievers is measured.3 similarly, tetrahydrocannabinol (THC), the component
of Cannibas sativa responsible for the CNS effect, has also been found to reduce nausea
associated with cancer chemotherapy. Another therapeutic area where natural products have
had a major impact on longevity and quality of life is in the treatment of cancer. In fact, most
of the major anticancer drugs are natural products either from plants or micro-organisms.
Examples include important anticancer drugs such as Bleomycin, Doxorubicin, Vincristine,
Vinblastine, and now the recent addition of Paclitaxel (Taxol), Ironotecan (a camptothecin
derivative) and Etoposide and Tenoposide (Podophyllotoxin derivatives).
Some of the most exciting natural products discovered in the recent years are the
cholesterol-lowering agents derived from fungi.
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(These drugs act by inhibition of 3-hydroxy-3-methylglutaryl co-enzyme A reductase
(HMG-COA reductase), an enzyme in the biosynthesis of cholesterol).The first of the HMGCOA reductase inhibitors were isolated from Pencillium sp.4 Substances derived from the
plants remain the basis for a large proportion of the commercial medications used today for
the treatment of heart diseases, high blood pressure, pain, asthma, cancer and other problems.3
Plants contain a number of metabolites, as shown in the Table no-1.1.1 (a), only a small
percentage has been investigated phytochemically and some fractions of them have been
submitted for biological screening. The process of evaluation of plants for various
pharmacological activities is a much time consuming process. So also is the process of
isolation of active components present in the plants. Hence, it requires multi-disciplinary
collaboration.4-5 Natural products have proven to be the richest source of medicinal
compounds. Screening the marine flora and fauna, soil samples, fungi and microbes is
conducted either to discover a new drug or a lead structure. A lead is a prototype compound
for a given biological activity. For example for anti-tumour activity, a natural product lead
structure is subjected to chemical modification or scaffolds to arrive at the therapeutically
important molecular fragment, the pharmacophore. Only a few natural products are directly
used as drugs, but in many cases the chemical scaffolds of the lead structure give a more
potent synthetic or semi-synthetic analogs.6-7
Globally, there has been an unparalleled growth in the plant-derived medicinally
useful formulations, drugs and health-care products. It has a market covering more than 60%
products derived from plant origin. India exhibits remarkable outlook in modern medicines
that are based on natural products besides traditional system of Indian medicines. Almost,
70% of the modern medicines in India are derived from natural products.
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Table No-1.1.1(a) presents some of the clinically very important natural product drugs,
scaffolds structures, synthetic or semi-synthetic analogs.
Sl.No.
Drugs from
herbs and
plants
Source
Atropine
Atropa
belladonna
Antimuscarinics
Therapeutic
activity
Synthetic or semisynthetic analogs
Dicyclomine Hcl,
Hyoscinebutylbromide
Benzyl
penicillin
Penicillin
chrysogenum
Antibiotic
Ampicllin, amoxycillin.
Codeine
Papaver
somniferum
Analgesic
Nalarphine, meperidine.
10-hydroxy camptothecin,
aminocamptothecin,
topotecan, ironotecan.
Camptothecin
Camptotheca
accumnata
Anticancer
Digoxin
Digitalis
lantana
Cardiovascular
Ephedrine
Ephedra
vulgaris
Anti-asthma
Salbutamol, salmeterol.
Lovastatin
Aspergillus
terrus
Hypercholesterol
emia
Pravastatin.
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Sl.No.
Drugs from herbs

Source
and plants
Therapeutic
activity
Synthetic or semisynthetic analogs
Morphine
Papaver
somniferum
Analgesic
Heroine, naloxane,
phthadine
Podophyllotoxin
Podophillum
pettatum
Anticancer
Etopside, toniposide.
10
Quinine
Cinchona
succirubra
Anti-malarial
Chloroquine,
meploquinine,
pamaquine, premaquine.
11
Reserpine
Rawolfia
serpentina
Hypotension and
Anticholinergic
12
Tubacurarine
Tube curare
Neuro-muscular
blocking agent
Decamethoxium,
soxamethorium.
13
Taxol
Taxus baccata
Anticancer
14
Teprotide
Bathrops
javaraca
Antihypertensive
Captropril, enalapril,
lisinopril
15
Vinblastin,
Vincristine
Cathranthus
roseus
Anticancer
Vindesine.
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Medicinal plants play a central role not only as traditional medicines but also as trade
commodities, meeting the demand of distant markets. Ironically, India has a very small share
(1.6%) of this ever-growing global market.
To compete with the growing market, there is urgency to expeditiously utilize and
scientifically validate more medicinally useful plants while conserving these species, which
seems a difficult task ahead.8
1.1.1. Medicinal and Aromatic Plants

India has 2.4% of worlds area with 8% of global bio-diversity. It is one of the 12
mega-diversity hot-spot regions of the world. Other countries being Brazil, Colombia, China,
South Africa, Mexico, Venezuela, Indonesia, Ecuador, Peru, USA and Bolivia. Across the
country, the forests of India are estimated to harbour 90% of Indias medicinal plants
diversity. Only about 10% of the known medicinal plants of India are restricted to non-forest
habitats. The estimated numbers of plant species and those used for medicinal purpose vary.
According to (Schippmann, 2002), 10 one fifth of all the plants found in India are used for
medicinal purpose. The world average stands at 12.5% while India has 20% plant species of
medicinal value.9
But according to Hamilton (2003)10, India has about 44% of flora, which is used
medicinally. Although it is difficult to estimate the number of medicinal and aromatic plants
present worldwide, the fact remains true that India with its rich biodiversity ranks first in its
The existence of traditional medicine, depends on plant species diversity and the related
knowledge of their use as herbal medicine. Both plant species and traditional knowledge are
important to the herbal medicine trade and the pharmaceutical industry where plants provide
raw materials and the traditional prerequisite information.11
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India has one of the richest plant medical traditions in the world. It is the tradition that
is of remarkable contemporary relevance for ensuring health security to the teeming millions.
There are estimated to be around 25,000 effective plant-based formulations, are used in folk
medicine and are known to rural communities in India. There are over 1.5 million
practitioners of traditional medicinal system using medicinal plants in preventive, promotional
and curative applications. It is estimated that there are over 7800 medicinal drugmanufacturing units in India, which consume about 2000 tonnes of herbs annually.12 two of
the largest users of medicinal plants are China and India.13-15
1.1.2. Herbal medicine.

Herb has various meanings, but in simplest form, it refers to crude drugs of vegetable
origin utilized for the treatment of diseases , often of a chronic nature, or to attain or maintain
a condition of improved health. Herbal medicine, sometimes referred to as Herbalism or
Botonical Medicine, is the use of herbs for their therapeutic or medicinal value. A herb is a
plant or plant part valued for its medicinal, aromatic or savory qualities. Herbs plants produce
and contain a variety of chemical substances that act upon the body. Herbal preparations
called phytopharmaceuticals, phytomedicinal or phytomedicine, are preparations made
from different parts of herbs or plants. They come in different formulations and dosage forms
including tablets, capsules, elixir, powder, extract, tincture, cream and parenteral preparations.
A single isolate or active principle derived from plants such as digoxin or reserpine tablet is
not considered herbal medicine.16-17
Herbal Remedies
The effectiveness of herbal remedies, their easy availability, low cost and
comparatively being devoid of serum toxic effects popularized them.
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Table No -1.1.2. (a). Number of Plant species used medicinally worldwide.10
Country
Plants species
Medicinal plant
species
Percentage
China
26,092
4,941
18.9
India
15,000
3,000
20.0
Indonesia
Malaysia
22,500
15,500
1000
1,200
4.4
7.7
Nepal
6,973
700
10.0
Pakistan
4,950
300
6.1
Phillippines
Sri Lanka
8,931
3,314
850
550
9.5
16.6
Thailand
11,625
1,800
15.5
USA
Vietnam
21,641
10,500
2,564
1,800
11.8
17.1
Average
13,366
1,700
12.5
world
422,000
52,885
Table No-1.1.2. (b). Numbers and percentage of medicinal plant species recorded from
different countries and regions (Hamilton, 2003).11
Country or
region
Total no. of native

species of flora
No. of species of
medicinal plants
% of flora which is
medicinal
China
27,100
11,146
41
India
17,000
7,555
44
Mexico
30,000
2,237
North America
20,000
2,572
13
World
297,000,-510,000
52,896
10-18
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1.1.3. Popularity of herbal medicine
The herbal medicines are largely gaining popularity over allopathic medicine because of the
following reasons favourable reasons:
Rising costs of medicinal care.
As these are from natural origin, so free from side effects in several cases.
Goes to the root cause and removes it, so that the disease does not occur again.
Freedom from approaching various specialists.
Cure for many obstinate diseases.
Easy availability of drugs from natural sources.
1.1.4. Need and Scope of herbal therapy

The treatment of diseases with pure pharmaceutical agents is a relatively modern
phenomenon. However, as European explorers and merchants spread out to the Western and
Eastern parts of the world, some of the benefits they would bring back were newly discovered
pharmaceutical preparation of natural origin. One of the earliest success stories in developing
a drug from a natural product was aspirin. Today we are more concerned with the life-style
disease like depression, cancer and heart troubles caused by faulty nutrition and stress. The
need of alternative therapy is to cover good health for all. Herbal therapy is one of the best
practices to overcome illness. Traditional Indian practice held that certain drugs should be
formulated through the addition of chosen substance that enhances bioavailability of the drug.
Pepper has confirmed bioavailability enhancer property and point to the active component as
the molecule piperine. An anti-TB drug Rifampicin has to be given at a higher dosage than
required in order to compensate for losses on the way to the target site. Formulation of
Piperine with Rifampicin will have counter effects.18-19
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Hence one needs to be cautions while administrating herbal medicine with any other
formulations.
1.1.5. Herbal medicine drug-interactions

The potential risk of herbal medicine interacting with the prescribed drug is also a
concern with the increased use of phytomedicine. Recently, several interactions have drawn
the attention of the medical community. Janetzky and Morrealc reported a probable
interaction between ginseng one of the most popular herbs with multiple health claims and
warfarin, drug with numerous well-recognized drug-drug interaction.20
1.1.6. Understanding Drug-Herb Interactions

Drug interactions occur by 4 major mechanisms.
Altered drug absorption
Altered renal (kidney) elimination of drugs
Additive effects or toxicities (pharmacodynamic interaction)
Altered hepatic (liver) metabolism of drugs
The first three account for a relatively small number of problems, while the fourth is the
major culprit in drug interactions. The potential seriousness of drug interaction depends part
by the drugs involved. Some drugs have what is called a "narrow therapeutic margin" which
means that there is relatively small difference between the amount of drug needed to achieve
its beneficial effect and to that of causing adverse or unwanted effects. Classic examples of
drugs falling in this category are anticoagulants (blood thinners like warfarin), which can
cause bleeding if relative amounts of the drug is increased.
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Absorption
When drugs are given orally they are usually absorbed into the bloodstream through
the stomach. Changes in drug absorption may be due to alterations in pH, or acidity of the
stomach, or by drugs binding together in the stomach to form complexes which cannot be
absorbed, For example, when the molecule is too large to pass through the intestinal wall.
Common examples include antacids, which increase stomach pH, and iron supplements,
which can bind to some antibiotics, such as ciprofloxacin or tetracycline.
Another issue for absorption is the "motility of the gastrointestinal tract", in other
words, how fast or slow your guts are moving. If you have diarrhea, the drugs or herbs are
moving through your system quickly and may have less time to be absorbed. Laxatives or
bulk-forming agents speed up intestinal transit, and might interfere with intestinally absorbed
drugs. Common stimulant laxative herbs are anthranoid-containing plants like senna, frangula,
yellow dock and Chinese rhubarb, as well as Cascara sagrada and Aloe-Vera leaf. Bulkforming agents include guar gum and psyllium. The clinical significance of these interactions
are not clear.
Elimination
Drug interactions due to alterations in elimination of drugs through the kidney can
only occur if a drug is primarily eliminated from the body through the kidney. If a drug or
herb causes decreased kidney function, levels of the drugs eliminated through the kidneys
may be increased as a result. Herbs containing diuretic properties, such as corn silk,
dandelion, and juniper can increase the toxicity of lithium, a drug used to treat bipolar
disorder.
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Pharmacodynamic Interactions
Some drugs (and herbs) that may be given together have similar beneficial effects, or
similar toxic effects- this is called a pharmacodynamic interaction. For example, two
antiretroviral drugs can cause the side effects of peripheral neuropathy, increasing the
likelihood of that side effect developing. Many drug-herb interactions fall in this category. For
example herbs that have sedative properties, such as kava, nettle and sage may increase the
sedative effects of some sleeping medications. Herbs that have antiplatelet activity, such as
ginkgo biloba, ginger, ginseng, and garlic may increase the risk of bleeding in patients taking
traditional drugs with antiplatelet activity or blood thinners. Herbs that can increase blood
pressure, such as blue cohosh, ginger, liquorice and bayberry can interfere with the
effectiveness of drugs used to treat high blood pressure.
Liver Metabolism
The most complicated drug interactions, and those with the greatest significance for
antiretroviral medications, are those resulting in altered liver metabolism of drugs. The
activity of liver enzymes which are responsible for breaking down drugs can be increased
(induced) or decreased (inhibited) by drugs or herbs. Many antiretroviral medications are
enzyme inducers, enzyme inhibitors, or even both, at the same time. The resulting drug
interactions are complex, and not always predictable. Ritonavir, a protease inhibitor, is a
powerful inhibitor of liver metabolizing enzymes, and can dramatically increase the blood
levels of other drugs metabolized by the same enzymes. This interaction can be used to our
benefit, so that lower doses of the drugs affected are required to achieve the same effect. If
dosage adjustments are not made however, toxic levels of the affected drug could result.
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Nevirapine, another antiretroviral is an enzyme inducer, and can decrease the blood
levels of other drugs metabolized by the same enzymes. If we know how each drug is
metabolized and how it affects metabolizing enzymes, we can predict the response and be
prepared.Many drugs in a wide variety of therapeutic categories are metabolized by liver
enzymes and subject to this type of interaction. These include drugs used to treat anxiety and
insomnia (diazepam and some of its relatives), drugs used to treat depression, some antiarrhythymics (used to treat abnormal heart rhythms), oral contraceptives, painkillers and
recreational drugs.
1.1.7. Common Medicinal Plants Reported To Interact With Pharmaceuticals

A comprehensive search of interactions between commonly used medicinal plants and
pharmaceutical drugs recently published in clinical reports suggest that potential interactions
with the following herbals, betel nut, chilli pepper (capsicum), Danshen, Devils claw, dong
quai, eleuthero or siberian ginseng, garlic, gingko, ginseng, guar gum, karela or bitter melon,
liquorice, papaya, psyllium, St. Johns wort, Saiboku-to (Asian herbal mixture);
Shankhaspushpi (Ayurvedic mixed-herb syrup); Sho-saiko-to or xiao chai hu tang (Asian
herbal mixture), tamarind, valerian and yohimbine.
Some specific cautions are that people with clotting disorders, those awaiting surgery,
or those on anticoagulant therapy should be aware that ginkgo, danshen, dong quai, papaya,
garlic, feverfew, ephedra or ginseng may cause unexpected bleeding, increase bleeding times
or inhibit blood clotting for about two weeks after you stop taking the herb. People taking
protease inhibitors, serotonin re uptake inhibitors (newer antidepressants), cyclosporin,
digoxin, phenprocoumon need to consider potential interactions with St. Johns wort. Ginseng
may interact with phenelzine, another antidepressant.
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People taking tricyclic antidepressants should avoid yohimbine. Liquorice, which has
been shown to have antiviral properties and is a very common ingredient in Chinese herbal
remedies, can have an additive synergistic effect with corticosteroids. Corticosteroids, like
prednisone are commonly prescribed to ulcers in the throat and mouth that dont respond to
topical preparations, or to treat rashes associated with some antiretroviral. These are only
some of the herb-drug interactions for which clinical reports have been made. Many others are
possible, and indeed likely. The complexity and potential gravity of drug-herb interactions
makes exercising caution and consulting a pharmacist or physician important.21
1.1.8. Toxicology & Herbs

In recent years there have been reports of deaths and poisonings attributed to the use
of medicinal plants such as comfrey and chaparral. Herbalists have a responsibility to
determine the truth/accuracy in such reports. Literature concerning poisonous plants is replete
with misinformation and erroneous reporting.20 the same mistakes continue to plague the
reporting of poisoning by medicinal plants.21, 22
Toxicology
The word toxicology is derived from toxicon - a poisonous substance into which arrow
heads were dipped and toxikos - a bow. Toxicology is a relatively young biological science
that involves a complex interrelationship of dose, absorption, distribution, metabolism and
elimination.
A poison
A poison is any substance which has a harmful effect on a living system. Paracelsus
(1493-1541) was one of the first to distinguish between the therapeutic and toxic properties of
substances.
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He thought that the only difference between a medicine and a poison was the dose.
Very few substances are actually classed as a "poison". Harmful chemicals are not necessarily
poisons. We are exposed to potentially toxic substances every day without immediate harm.
Our bodies can usually safely metabolize toxins if we are exposed to them in small amounts.
It is only when we overwhelm our body and reach the toxic dose of a substance that lifethreatening results occur. That is, all substances have a potential toxicity. All herbs can
therefore be harmful, but most would have to be ingested in large amounts to cause harm.
Herbs which have a high toxicity, such as Gelsemium and Aconitum, can be used safely and
effectively if taken in small, therapeutic doses. Thus, the primary determinate of the safety of
a substance is the dose. It is the dose, not the herb, which makes the poison. A correct use of
semantics and a correct understanding of these terms are crucial to avoid confusion and
misinformation.
For example,
Vitamin D has a very high acute toxicity. It would have had to carry a poison label but
it has been exempted from the Federal Hazardous Substances Labeling Act because it
is classified as a food and a drug.
Salt is not toxic in small doses. But a single large dose can be lethal.
Just two tablespoons can kill a one-year-old child.
Caffeine, one of the many alkaloids found in coffee can kill - at a dose of 100 strong
cups of coffee.
A litre of scotch contains a lethal dose of ethanol.
Water can be lethal if you drink enough of it in a short period of time.
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These are substances that are foreign to the body or exogenous as compared to
substances produced by the body or endogenous. It is important to point out that endogenous
substances can also cause poisoning and death. Toxic substances fall into several classes in
relation to how people are exposed to them. They can be put under the class as food additives,
drugs, pesticides, industrial chemicals, environmental pollutants, household poisons and
natural toxins. Many natural products used in medicine are derived not only from plants, but
also from marine organisms like starfishes, sea urchins, sea cucumbers and fish.
Dose-response relationship
Toxicity depends not only on the dose of the substance but also on the toxic properties of
the substance. The relationship between these two factors is important in the assessment of
therapeutic dosage in pharmacology and herbalism.23
Plant substances can harm.
Toxicants can interrupt metabolism of carbohydrates, lipids and proteins and alter synthesis,
release and storage of hormones.
Here are some examples of how substances from plants can harm.24
Oxalate crystals from Halogeton glomeratus can damage the tubules in the kidney.
because they are insoluble, precipitate and collect in the kidney tubules to then
obstruct them.
The alkaloid, aconitine in aconite, affects the sodium channels on the cell membrane
which can lead to increased uptake in sodium and other ions. This can lead to cardiac
arrhythmias and depression of respiration.
The psychotropic plant alkaloids, harmine and harmaline resemble serotonin and are
thought to block the serotonin receptors in the brain.
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1.2. REVIEW OF LITERATURE ON SELECTED PLANTS.
1.2.1. REVIEW OF LITERATURE ON Annona squamosa. L25-40

Family
: Annonaceae
Genus
: Annona
Species
: squamosa
Common name
: Custard apple, Sitaphala
Duration
August-January
Voucher No
HGUG-19
Habitus. In gardens, all over India.

Geographical distribution: It grows wild in the central provinces, western peninsula, South
India & Ceylon.
Morphological Characters
Key characters: Annona squamosa. L is a small, semi deciduous, much branched shrub or
small tree irregularly spreading branches and a short trunk.
Leaves. Thin leaves occur singly, long and wide, Leaf stalks are long, green, and sparsely
pubescent
Flowers. Solitary or in short lateral clusters greenish-yellow flowers on a hairy, slender
long stalk. Green outer petals, purplish at the base, oblong, wide, inner petals.
Stems. Branches with light brown bark and visible leaf scars; inner bark light yellow and
slightly bitter; twigs become brown with light brown dots
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Fruits. The round or heart-shaped greenish yellow, ripened aggregate fruit is pendulous
on a thickened stalk; many round protuberances and covered with a powdery bloom.
Fruits are formed of loosely cohering or almost free carpels (the ripened pistels).
Seed each carpel containing an oblong, shiny and smooth, dark brown to black,
Medicinal uses of Annona squamosa. L

The treatment of epilepsy, dysentery, cardiac problem, worm infection, constipation,
hemorrhage, antibacterial infection, dysuria, fever, ulcer. Anti fertility, anti tumor and
abortifacient properties.
Biological uses reported in literature.

Leaves: The leaf extract being used for ameliorate hyper thyroidism. An insecticidal
agent. Free radical scavenging activity, Hypoglycemic anti diabetic effect and Hepato
protective activity.
Bark and root: Ethanolic extract of leaves and stem are reported to have an anti
cancerous activity.
Seeds: Antibacterial and antiovulatory have been studied with seed extract.
Chemical constituents
Leaves
: Aporphine alkaloids, flavonoids, glycoside,
Root
: Terpine derivatives and novel diazepine,
Seed
: squamoline
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1.2.2. REVIEW OF LITERATURE ON Argemone Mexicana. L41-47
Family
: Papveraceae
Genus
: Argemone
Species
Common name
: mexicana
: Prickly poppy
Duration
: August-January
Voucher No
HGUG-614

Geographical distribution: prickly herb naturalized throughout India up to 5000 feet in
wastelands and along roadsides.
Key characters: Argemone Mexicana. L is a small, semi deciduous, much branched shrub
irregularly spreading branches and a short trunk.
Leaves. Alternative or radical, with sessile, semi-amplxicaul, sinuate-pinnatified leaves,

variegated with white.
Flowers. Terminal, bright yellow colored, pis 1-3 cm.
Stems. Cylindrical, herbaceous (green), prickly and branching.
Seed. Seeds numerous.
Medicinal uses of Argemone mexicana L.

Whole plant bitter, diuretic, purgative, destroys worms, cures itching, leprosy, various
skin diseases, reduce inflammation and bilious fevers, useful instangury. An antidote to
various poisons, enriches the blood, a good expectorant and aphrodisiach.
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Root an antielmintic , stimulant and chronic cases of skin diseases. Leaves are used
for cough. Seeds are used purgative, sedative. Juice is useful in leprosy, cutaneous affections;
scabies oil is a better preparation than juice.

Seed. Toxicity, anti-HIV.
Chemical constituents.
Leaf. Berberine, protopine nitrate, phenolics,
Bark and Root. Fatty acids, alkaloids.
Seed.
Allocryptonine, sanguinarine, long chain alcohol,
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1.2.3. REVIEW OF LITERATURE ON Calotropis gigantia. Br48-51
Family
Asclepidaceae
Genus
Calotropis
Species
gigantia
Duration
: August-January
Voucher No
HGUG-47

Geographical distribution: distributed throughout India.
Key characters: Calotropis gigantia a tall shrub reaching 2-4 to 3 m length.
Leaves. Leaves sessile or nearly so, elliptic ablong, acute thick, glauccous.
Flowers. Flowers are purplish or white, buds ovoid, corolla 2cm long or more, follicles 910 cm long.
Stems. Branches with light brown bark and visible leaf scars; inner bark light yellow and
slightly bitter; twigs become brown with light brown dots.
Seed. green seeds numerous, 6 by 5 mm, ovate.
Medicinal uses of Calotropis gigantia .L.

Latex is applied externally to corns. Antipyretic activity, whole plant cures leprosy,
leucoderma, ulcers, tumors, piles, diseases of spleen.

Leaves. Are applied to paralysed parts, painful joints, swelling, heal wound.Useful in
leprosy, scabies. Applied to painful joints and swellings.
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Flowers. Are anthelmintic, analgesic, astringent, cures inflammations, tumours.
Bark and Root. Antimicrobial activity, cytotoxic activity.
Seed. Antimicrobial activity.
Leaves. Steroids, flavonoids.
Bark and Root. Alkaloids.
Seed. Oil.
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1.2.4. REVIEW OF LITERATURE ON Cassia auriculata L.52-67
Family
: Caesalpiniaceae
Genus
: Cassia
Species
: auriculata
Common name
Avaram, Tanners
Duration
August-January
Voucher No
HGUG 222
3.1.2. Geographical distribution: It grows wild in the central provinces, western peninsula,
South India & Ceylon.
3.1.3. Morphological Characters.

Key characters: A tall much branched shrub, bark with smooth reddish brown branch lets
finely pubescent.
Leaves: long, rhachis densely fulvous-pubescent with an erect linear gland between each
pair of leaflets, stipules foliaceous, reflexed, very large, rotundate-reniform, produced at
the base on the side next the petiole into a long subulate point, persistent. Leaflets 8-12
pairs, overlapping, oblong-obovate, and obtuse or emarginated, mucronate, glabrous or
finely downy, dull green above, base usually rounded, petioles long.
Flowers: Flowers large, reaching 5cm across, in terminal and axillary corymbose racemes
pedicels long, bracts ovate, acuminate, caduceus, calyx glabrous, segments leathery,
concave. Petals with long claws crisped on the margin, bright yellow, veined with orange.
Stamens 10, of which the 3 upper are reduced to staminodes, the remaining 7 perfect, of
which the 3 lower are larger than the 4 lateral ones. Flowers from October-May.
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Pods: flat, thin, papery, oblong, obtuse, mucronate, pale brown, deeply depressed between
the seeds, having a crupled apprearance, transversely veined, pubescent, fruits mature
from January-June depending on locality.
Seeds: 10-20 per pod, obovate, dark brown with hard shiny seed coat.
3.1.4. Medicinal uses of Cassia auriculata L.

Plant: The whole plant is used in diuresis and diabetes mellitus.
Bark and root: Astringent.
Roots: Cooling, alterative, depurative and alexeteric, and are useful in skin diseases,
leprosy, tumors, asthma and urethrorrhoea.
Bark: Astringent and alterative and a decoction of this is used as enemas and gargles, and
in the treatment of rheumatism and eye diseases.
Leaves: Leaves are depurative and anthelmintic and are recommended for leprosy, skin
diseases, ulcers and hepatoprotectivity.
Flowers: The flowers are used in urinary discharges, nocturnal emissions, and diabetes,
throat troubles.
Fruits: Anthelmintic, useful in vomiting, thirst and urinary discharge.
Seeds: Opthalmia and conjuctivities in diabetes and chylons urine, and also used as
astringent, sour, cooling, constipating, depurative, aphrodisiac, anthelmintic, stomachic,
dysentery, diarrhoea, swellings, abdominal disorders, leprosy, skin diseases and worm
infestations.
Twings: The twings are used as tooth brushes.
Parts used: Bark, root leaves, flowers, fruits, seeds.
Page 23

3.1.5. Biological uses reported in literature
Dried flowers and leaves of the plant are being used for medicinal treatment. Extract
made from the flowers and seeds have been shown to antidiabetes activity ethno medically.
Plant has been shown to antiviral and anti spasmodic activity. Flower and leaf extract shown
to antipyretic activity. Leaf extract also shows emollient effect.
Antihyperglycemic activity was inactive in rabbit and does in doses up to 50mg/kg
body weight. An aqueous leaf extract was found to lower the serum glucose level at body
weight. Effect of flowers on blood sugar levels, serum and tissue lipids in streptozotocin
diabetes rats. Antiperoxidative effect of flowers in streptozocin diabeteiic rats. Leaf extract in
rats with alcoholic liver injury. Effect of Cassia auriculata L. Root extract on cisplatin and
gentamicin-induced renal injury. Antioxidant activity of Cassia auriculata L. flowers.
3.1.6 Chemical constituents

Flowers: -sitosterol and kaempferol, proanthocyandin dimmer.
Leaves: -sistosterol and emodin, and 4, 5, 7. trihydroxyflavan-3, 4-diol also known as
leucoanthocyaningoratesidine, flavonoids and anthracene derivatives,
-sistosterol -D-
glucoside, quercetin 3-O-glucoside, rutin.

Seeds: Polysaccharide, Oligosaccharide, amino acids.
Bark: Tannins
Stem bark: Catechin, fisetinidol-(4->8) epicatechin, fisetinidol- (4->8) - gallocatechin,
and fisetinidol-(-(4>8) epigallocatechin.
Root: Flavone glycoside 7, 4,-dihydroxy flavone-5-O--D-galactopyranoside.
Pod husk: Chrysophenol, emodin, rubiadin and -sitosterol.
Whole plant: Protein, free amino acids, tannins and nonacosan-6-one.
Page 24

1.2.5. REVIEW OF LITERATURE ON Ficus religiosa L. 68-70
Family
: Moraceae
Genus
: Ficus
Species
: religiosa
Common name
: Ravi
Duration
: August-January
Voucher No
: HGUG 587

Geographical distribution: It distributed in sub- Himalayan forests, Bengal, central India.
Key characters: Ficus religiosa L. is a large tree, much branched, irregularly spreading
branches.
Leaves. Coriaceous, ovate-rotund, narrowed, upwards, base broadly ovate, stamen1,
anthers single, ovate-round, filament short, lanceolate, style short, lateral, stigma rounded.
Stems. Branches with light bark and visible leaf scars; inner bark light yellow and
slightly bitter; twigs become brown with light brown dots
Fruits. The round or heart-shaped greenish , ripened aggregate fruit is pendulous on a
thickened stalk;
Seed. Each carpel containing an oblong, shiny and smooth, brown to black,
Medicinal uses of Ficus religiosa L.

Plant parts are bitter, sweetish, acrid, cooling, and useful in diseases of the blood,
vagina, uterus, leucorrhoea, burning sensation.
Page 25

Ripe fruit is cooling, alexipharmic; good for burning sensation, foul taste, and fruit is laxative
and helps in digestion, purgative, aphrodisiac, checks vomiting. Infusion of bark given
internally in scabies. A paste of powdered bark is used as absorbent in inflammontory
swellings. Hypolipidemic.
Leaves. Flavonoids, triterpenes.
Bark and Root. Tannins.
Page 26

1.2.6. REVIEW OF LITERATURE ON Jatropha curcas L. 71-75
Family
: Euphorbiaceae
Genus
: Jatropha
Species
: curcas
Duration
August-January
Voucher No
HGUG 1295

Geographical distribution: It is distributed throughout India, common hedge plant along
roadsides and outskirts of villages.
Key characters: Jatropha curcas L. Shrub or small tree. Up to 5 m tall.
Leaves. The leaves have significant variability in their morphology. In general, the leaves
are green to pale green, alternate to sub opposite, and three- to five-lobed with a spiral
phyllotaxis.
Flowers. Male and female flowers are produced on the same inflorescence, the petiole
length ranges from 0.24 to 0.90 inches (6.123.1 mm). The inflorescence can be formed in
the leaf axil. Plants are monoecious and also present hermaphroditic flowers occasionally.
Unisexual, monoecious, yellowish green in loose panicle of cymes.
Fruits. Fruits are produced in winter, or there may be several crops during the year if
soil moisture is good and temperatures are sufficiently high. Most fruit production is
concentrated from midsummer to late fall with variations in production peaks where some
plants have two or three harvests and some produce continuously through the season.
Page 27

Seed. The seeds are mature when the capsule changes from green to yellow. The seeds
contain around 20% saturated fatty acids and 80% unsaturated fatty acids, and they yield
25%40% oil by weight.
Medicinal uses of Jatropha curcas L

Drug obtained from Jatropha curcas is termed as Dravanthi it is bitter, pungent and
astringent in taste. It has anthelmintic; it is beneficial in chronic dysentery, thirst, urinary
discharges, anaemia, fistula, ulcer and diseases of heart and skin.The young leaves may be
safely eaten, steamed or stewed.
Cooked with goat meat, they are said to advantageously counteract its smell. Pounded
leaves are applied near horses' eyes to repel flies in India. The extracts of the plants are
dangerous to use but water can easily release it over if not too much extract is applied. Oil of
seeds used externally for rheumatism and paralytic. Milky say is used for the treatment of
different dermatomucosal diseases such as gingivitis, wounds, haemorrhoids, herpes, sores,
burns, ulcers, and warts.
Page 28

1.2.7. Within the frame work of thesis.
Natural product once served as the only source of medicines for mankind. Screening
of natural products, especially those having medicinal use, structure determination and
biological activity has been an important aspect in chemistry. A good number of bioactive
compounds isolated from medicinal plants and their semi synthetic and synthetic analogs have
found to have wide application in chemotherapy. Some of the synthetic derivatives have by
far surpassed the naturally occurring moieties due to their applicability in various fields. In
recent years, the chemistry of natural products have been extended to enormous length and as
a result large number of bioactive natural products, their lead and synthetic derivatives have
been synthesized.
The present investigation mainly describes the antioxidant screening of different plant
extracts; resulting in bioactivity guided selection of Annona squamosa. L an effort in isolation
of active constituent(s) from active extract from Annona squamosa. L has been made. Further
various biological screening of the active extracts as well as isolated active compound has
been undertaken. Their efforts have been discussed in the present thesis.
The thesis divided into seven chapters

Chapter I
This chapter divided into two parts, first part deals with general introduction to
medicinal plants. The second part deals with review of selected medicinal plants-work within
the frame of this thesis.
Chapter II
This chapter divided into to three parts, first part deals with general introduction to
antioxidant, second part deals with identification of six plants, collection, extraction and
Page 29

phytochemical screening of selected plants, third part deals with method adapted by us for
evaluating antioxidant potential and results and discussion of antioxidant screening of various
plant extracts and conclusion.
Chapter III
This chapter divided into to three parts, first part deals with review of Annona
squamosa. L Second part deals with collection, extraction and phytochemical screening of
different part (leaf, root, and seed) of Annona squamosa. L plant, third part deals with
evaluating antioxidant potential and, results and discussion of antioxidant.
Chapter IV
This chapter divided into to three parts, first part deals with introduction of Annona
squamosa. L Second part deals with collection, extraction and phytochemical screening of
different extracts of leaf part of Annona squamosa. L plant, third part deals with evaluating
antioxidant potential and, results and discussion, of antioxidant.
Chapter V
This chapter divided into to two parts, first part deals with collection, extraction of leaf
part of Annona squamosa. L Second part deals with the isolation of chemical constituents
from ethanol extract and structural elucidation physical data interpretation.
Chapter VI
The part deals with evaluating antioxidant potential of isolated compound(s) and,
results and discussion of antioxidant.
Page 30

Chapter VII
This chapter divided into to three parts, first part deals with general introduction to
microbial, second part deals with method adapted by us for evaluating anti microbial potential
and, results and discussion of antimicrobial screening of Annona squamosa. L plant extracts.
Appendix.
1) Computer aided Drug design related to Rutin.
2) Application of Briggs Rauscher reaction for measurement of antioxidant capacity.
Page 31

1.3. References.
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7. Ram Gopal M.D. Medicinal plants: Screening for various biological activities, isolation
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13. Masood, E. Medicinal plants threatened by over-use. Nature (1997), 570.
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No. 25, (1991).
22. Ibid. The Good, The Bad and The Worst, Herbal Gram No. 25; (1991).
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27. Asholkar LV, Kakkar KK, Chakre OJ. Glossary of Indian Medicinal plants with active
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Ovulatory studies on Annona squamosa. L Planta medica. (1975), 28, 97-100.
30. Sunanda P, Anand K, Possible amelioration of hyper thyroidism by the leaf extract of
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34. Gupta RK, Kesari AN, Murthy PS, Chandra R, Tandon V, Watal G. Hypoglycemic and
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37. Bhakuni DS, Tewari S, Dhar MM. Aporphine alkaloids of Annona squamosa. L
Phytochemistry. (1972), 11, 1819-1822.
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Annona squamosa. L Phytochemistry. (1979), 18, 1584-1586.
39. Seetharaman TR. Flavonoids from the leaves of Annona squamosa. L and Polyathia
longifolia L.Fitoterapia. (1986), 57, 189-198.
40. Forgas P, Desconclois JF, Provost R, Tiberghien et touch A.UnNovel Heteroside nitre
extrait D. Annona squamosa. L Phytochemistry. (1980), 19, 1251-1252.
41. Bohlmann F, and Nagabhushan R. Naturally occurring terpene derivatives; XXI, on the
constituents of Annona squamosa. L Chem. Ber. (1973), 106, 841-844.
42.Yang T H and Chi-Ming C. Structure of Squamoline, a novel diazepine from Annona

squamosa .L J.Chi.Chem.Soc.(Taipei) (1972), 19, 149-151.
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44. Kaushal, K., Preti, U., Mukul Das., Subhash K. Toxicology. (1988), 42, 301-308.
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53. Cappasso, A., et al. Planta Medica. (1997), 63, 326-28;
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Page 37

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1. Introduction to Medicinal plants.

on herbs and developed well-defined herbal

1. Introduction to Medicinal plants.

1. Introduction to Medicinal plants.

Synthetic or semisynthetic analogs

1. Introduction to Medicinal plants.

Drugs from herbs

Synthetic or semisynthetic analogs

1. Introduction to Medicinal plants.

1.1.1. Medicinal and Aromatic Plants

1. Introduction to Medicinal plants.

1.1.2. Herbal medicine.

1. Introduction to Medicinal plants.

Total no. of native

1. Introduction to Medicinal plants.

Rising costs of medicinal care.

Freedom from approaching various specialists.

Cure for many obstinate diseases.

Easy availability of drugs from natural sources.

1.1.4. Need and Scope of herbal therapy

1. Introduction to Medicinal plants.

1.1.5. Herbal medicine drug-interactions

1.1.6. Understanding Drug-Herb Interactions

Altered drug absorption

Altered renal (kidney) elimination of drugs

Additive effects or toxicities (pharmacodynamic interaction)

Altered hepatic (liver) metabolism of drugs

1. Introduction to Medicinal plants.

1. Introduction to Medicinal plants.

1. Introduction to Medicinal plants.

1.1.7. Common Medicinal Plants Reported To Interact With Pharmaceuticals

1. Introduction to Medicinal plants.

1.1.8. Toxicology & Herbs

1. Introduction to Medicinal plants.

A litre of scotch contains a lethal dose of ethanol.

Water can be lethal if you drink enough of it in a short period of time.

1. Introduction to Medicinal plants.

Plant substances can harm.

1. Introduction to Medicinal plants.

1.2.1. REVIEW OF LITERATURE ON Annona squamosa. L25-40

: Custard apple, Sitaphala

Habitus. In gardens, all over India.

1. Introduction to Medicinal plants.

Medicinal uses of Annona squamosa. L

Biological uses reported in literature.

: Aporphine alkaloids, flavonoids, glycoside,

: Terpine derivatives and novel diazepine,

1. Introduction to Medicinal plants.

Habitus. In gardens, all over India.

Leaves. Alternative or radical, with sessile, semi-amplxicaul, sinuate-pinnatified leaves,

Medicinal uses of Argemone mexicana L.

1. Introduction to Medicinal plants.

Biological uses reported in literature.

Allocryptonine, sanguinarine, long chain alcohol,

1. Introduction to Medicinal plants.

Habitus. In gardens, all over India.

Medicinal uses of Calotropis gigantia .L.

Biological uses reported in literature.

1. Introduction to Medicinal plants.

1. Introduction to Medicinal plants.

3.1.3. Morphological Characters.

1. Introduction to Medicinal plants.