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International Journal of Trend in Scientific Research and Development (IJTSRD)
Volume 5 Issue 2, January-February 2021 Available Online: www.ijtsrd.com e-ISSN: 2456 – 6470
@ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 13
Transgenic Animals: A Better
Approach towards Experimentation
Swarnima Negi1, Dr. Sachdev Yadav2
1Scholar, 2Associate Professor,
1,2Department of Pharmacology Banasthali Vidyapith, Radha Kishnpura, Rajasthan, India
ABSTRACT
Animals play a crucial role in the development of medical products from
medicines to various implants and major surgical procedures. They are not
approved for human use until they qualify the safety parameters in animals.
The animals play a pivotal role in drug discovery and development. Oneofthe
most challenging aspects of targeting drugs for any pathological condition is
the development of animal models. Animal models are nothing but an
approach to replicate the general symptoms of the diseased condition which
occur in humans. The whole pathophysiology cannot be replicated but, the
symptoms which are known and precipitate the most in any pathological
condition are positively reproduced within the animal. With the increasing
need in the medical field, the paradigm is now slowly shifting towards
transgenic animals as they have given a new dimension to medical sciencesto
study the pathophysiology of the disease rather than focusing on the
symptom-based analysis of the diseasedcondition. Thesegeneticallymodified
organisms have shown groundbreaking results not onlyindevelopingmodels
for various diseases but also in developing biopharmaceuticals, receptor-
selective drugs, and have a huge contribution to xenotransplantation and the
agriculture sector. This review article vividly describesthenewerapproaches
that are adopted to develop transgenic animal models and also highlights
certain limitations to the older approach of developing the models.
KEYWORDS: Transgenic animals, in vivo models, ex vivo models, transgenesis,
xenotransplantation, disease resistant animals
How to cite this paper: Swarnima Negi |
Dr. Sachdev Yadav"TransgenicAnimals:A
Better Approach towards
Experimentation"
Published in
International Journal
of Trend in Scientific
Research and
Development(ijtsrd),
ISSN: 2456-6470,
Volume-5 | Issue-2,
February 2021, pp.13-17, URL:
www.ijtsrd.com/papers/ijtsrd38268.pdf
Copyright © 2021 by author(s) and
International Journal ofTrendinScientific
Research and Development Journal. This
is an Open Access article distributed
under the terms of
the Creative
CommonsAttribution
License (CC BY 4.0)
(http://creativecommons.org/licenses/by/4.0)
INTRODUCTION
Animal models are nothing but an approach to replicate the
general symptoms of the diseased condition in animals
which occur in humans. Over the decades with the
refinement in technology, the animal models can be are
prepared by using different methods that involve some
genetic and non-genetic approaches of model development.
The animals which are involved in the research are of two
types:
1. Non-genetically modified animal model of human
disease
The models developed can be in vivo, in vitro, or ex vivo.
Usually, the study begins with the in vitro models later the
data is extrapolated to in vivo and finally to humans.
In vitro models – These are developed by analyzing the
action of the drug either on the tissue of the organ from the
animal itself or on the tissue homogenate. These models
usually opted for the screening of any new chemical entity.
For example, the hepatoprotective screening studies are
done on primary hepatocytes or fresh hepatocytesextracted
from the animal. In some studies, direct human cells can be
taken for analyzing the action of drugs.
Ex-vivo models- These models involve the organs extracted
from the animal body and kept alive by giving almost same
environment like inside the human body. For example heart
is isolated from the animal bodyandactionofdifferentdrugs
are analysed. Similarly the liver or part of liver is also
isolated to study the hepatoprotective actions of different
drugs.
In-vivo models – In these models, there istheinvolvementof
intact animals, which are produced by different methods.
Physical models – The induction of symptoms in these is
done by physical factors such as electric shock to induce
convulsions. Similarly, the pain is induced by radiant heat or
cold treatment to study the analgesic effect of the drugs.
Chemical models – The symptoms are induced by exposing
the animal to certain drugs, which alters the ongoing
physiology of the animal and thus producesthesymptoms of
the disease. For example to study the hepatoprotective
action of any chemical entity the animals are exposed to
hepatotoxic agents such as carbon tetrachloride, ethanol,
acetaminophen, thioacetamide, etc. Similarly, todevelopthe
model for antipyretic agents the lipopolysaccharides and
yeast are injected into the animal. Streptozotocin and
alloxan, synergistically destroy the pancreatic beta cells and
produce the hyperglycemic condition within the animal.
Surgical models – To develop certain symptoms the surgical
interventions are adopted, one of the most common
examples is pancreatectomy to induce diabetes-like
condition in animals. Similarly to develop a model of
IJTSRD38268
International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470
@ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 14
myocardial infraction either the coronary artery ligation is
one of the methods which is opted and others may include
thoracotomy. To produce renovascular hypertension the
either one or both the kidneysaretied,toproducesecondary
hypertension within the rats.
2. Genetically modified animal model of human
disease. (Transgenic models)
Transgenic animals are the ones whose genome has been
modified deliberately to achieve the desiredgenotype which
resembles the diseased condition in human beings.
Transgenic animals are considered the best models to work
with because the researcher does not have to prepare the
animal for a certain study which is usually donewithnormal
animals a month or two months early before starting any
drug therapy. Based on the increasing need for animals in
medical sciences it has become more important to have
animals that by birth show the characteristics of some ofthe
diseases and disorders similar to that of human beings. The
main advantage of this approach is it provides a method to
rapidly introduce new genes into animals without cross-
breeding.
Limitationof anon-geneticallymodified animal model of
human disease
One of the major limitations of normal animals istheydonot
provide a solid basis for the pathogenesis of a disease. Thus,
the research always revolves around the development of
symptomatic treatment of the disease.Thisfactisnothidden
that almost all the drugs which are available forthecommon
aliments are based on giving symptomatic relief be it
diabetes, Multiple sclerosis,Parkinson'sdisease,Alzheimer's
disease, etc. These models are produced by giving the
animals various environmental exposure, which is a tedious
and time-consuming task.Asanimalshavetobeprepared for
the induction of any drug therapy weeks and months prior.
For example for induction of hypertension, thedietofthe rat
is modified, it has to be provided with an increased salt diet
from a month earlier. Apart from this the methodswhich are
adapted to induce the symptoms of any pathological
condition are not always favorable. Sometimes because of
the exposure of chemicals and surgery-induced models, the
animals are known to produce symptoms other than the
ones which are required, thus hampering the outcomeofthe
final results. Although the researcherskeepshamcontrol for
such purposes but cannot confidentlyruleoutthe possibility
of surgery hampering the results.
Production of genetically modified animals or
transgenic animals
The production of transgenic animals is the targeted
mutation which is solely based on two approaches that are
gene knock-in (insertion of any gene to therecipientanimal)
and gene knock-out (deletion of a gene from the animal).
This addition and deletion are based on the altered genetic
makeup in humans during any pathological condition.
The procedure involves the manipulation of endogenous
genomic DNA by transfecting the desired set of genes from
the donor animal. The process deals with the introduction of
specific mRNA into the germ cells of the host by using
recombinant DNA technology, with the thought that if germ
cell lines are altered, the characters will be passed on to the
forthcoming generation in normal reproduction. This whole
process of transferring the manipulated gene or altering the
DNA sequence is called transgenesis. Transpharmers is the
name given to the transgenic animals which are involved in
the production of pharmaceutical products. Table 1 shows
the different methods for the production of transgenic
animals.
Table 1 Methods of producing transgenic animals
S/N Technique Procedure Limitations Examples
Gene knock-in
1. DNA
microinjection
(Pronucleus
microinjection)
The eggs are obtained from a donor female
and in vitro made to fuse with the sperms.
The transgene is microinjected to the male
pronucleus in the premature zygote. The
zygote is then transplanted to the uterus of
the pseudopregnant female.
The success rate of this
method is very less, few
offsprings produced are
transgenic.
The technique is not
popular as it is tedious
and very few cells can be
handled at a time.
Muta mouse, big
blue transgenic
rats.
2. Embryonic Stem
cell-mediated
gene transfer
The totipotent stem cells are isolated from
the donor pregnant female. They are
cultured invitro and later transfected with
the desired gene. The pure population of
transfected ES cells is microinjected to the
blastocyst. The blastocyst is finally
implanted into the uterus of the
pseudopregnant recipient animal.
The progeny produce by
this technique is chimeric
i.e. they contain both
normal cells and
genetically modified cells.
Mice, rats
3. Retrovirus
mediated gene
transfection
The vectors used for transfection is
retrovirus which include lentivirus and
adenovirus.These are modified by
incorporating the desired gene into its
genome. Later the recombinant virus is
microinjected into the embryo of the animal
and grown-up to blastocyst in invitro. Later
the a blastocyst is implanted in the
pseudopregnant female.
The progeny produced is
chimeric in the F1
generation. The
probability of offspring
with transgene is very
low.
Pigs,mice
(Smian virus
was introduced
in mice for the
first time)
International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470
@ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 15
4. Transposons
(Jumping gene)
These are the small DNA sequence that is
used as a vector, which can jump from one
place to another in a genome simply by cut
and paste mechanism. Thus, recombinant
transposons are microinjected into the
embryo of the animal to have the desired
character in the progeny.
-
Transgenic
insects, zebra
fishes, chicken
cattle.
5. Somatic cell
Nuclear Transfer
The oocytes are arrested in meiosis II of the
cell cycle, specifically at metaphase or
telophase. These are reprogramed with the
nucleus of the somatic cell (skin cell, liver,
fat, or any other organ of the body is
extracted). The cell is stimulated with an
electric shock to begin the cell cycle.
-
Dolly sheep
(mammary cell
somatic cell was
incorporated)
6. Sperm Mediated
Gene Transfer
(SMGT)
Mature spermatozoa are allowed to bind to
the exogenous transfected DNA which is
then injected through ICSI (Intracytoplasmic
Sperm Injection) to the cytoplasm of the
oocyte.
The whole procedure is
dependent upon the
binding of the sperms to
the DNA without losing its
activity.
Cattle, Pigs
7. Testis cell
implantation
The testis is removed from the donor male
and transfected with the desirable gene, the
cells are then cultured and microinjected to
the lumen of seminiferous tubules of the
recipient animal. Later the recipient was
followed to mate.
- -
Gene knock-out
8. RNA
Interference
(RNAi)
The siRNA has the complementary sequence
which attaches covalently with the specific
sequence on the principle mRNA strand. The
powerful digesting enzyme argonaut
destroys the complementary sequence on
the principle mRNA strand and silences the
particular gene.
-
Salt sensitive
rats used in the
antihypertensive
study.
The superiority of transgenic models to the non-genetic
animal model of human disease
The transgenic models are superior in every respect as
compared to the other non genetically modified models of
human disease. The transgenic animals have shown
pioneering results in various fields. It has not only pavedthe
path to developing new frontiersinmedical sciencesbutalso
various other fields including agriculture. The scope of
transgenic animals is not only limited to serve humanity in
the medical area but also in various other sectors which is
not seen with non genetically modified animals. The below
mentioned are the areas where transgenic have showntheir
contribution more as compared to the non-genetic models
which are restricted to only animal models of human
disease.
Human disease models
The transgenic models are by far the best models to study
the pathogenesis of the diseases. This technology has
enabled the researcher to look beyond just symptoms and
have focused the studies towards the curative aspect of
treating the disease. Thepreferencehasnowshiftedtowards
the transgenic models in almost every research. This
approach can decrease the number of higher animals to be
used in the experimentation likes canines, nonhuman
primates. A successful model can be produced by modifying
the genomic sequence. This approach has very well defined
the pathogenesis of human diseases and has leadtothebirth
of gene therapy. The advantagewhichcomeswithtransgenic
models is we are able to produce models for conditions like
those whose models have not developed yet in normal
animals. The transgenic animals are easy to work with
because they do not require induction therapy.
For example, to study the basis of essential hypertension, no
such model has been developed which could give an insight
over the pathogenesis of the same. But transgenic animals
have been produced known as Spontaneous Hypertensive
Rats (SHR) and SHR-SP stroke-pronehypertensiverats,Dahl
and Sabra rats which are salt-sensitive rats, and rats which
already have highly activated RAAS. Thusthestudybecomes
easy with the genetic models.
Production of Biopharmaceuticals
The transgenic animals are known as bioreactors when it
comes to the production of biopharmaceuticals. The
biopharmaceutical contains vaccines, blood products, gene
therapies, etc. Several proteins like AT-III(antithrombinIII),
TPA (tissue plasminogen factor) are produced in the
mammary glands of goats and sheep which are later
extracted from them. Another blood product is produced in
transgenic swine is hemoglobin that has the same oxygen-
carrying capacity as that of human hemoglobin.
Certain enzymes are also produced by the use of transgenic
animals, like the enzyme α-glucosidase which is required in
International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470
@ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 16
patients with Pompe disease thus the enzyme isproduced in
the milk of transgenic rabbits and later extracted and
purified to be given to the patients. Similarly, the enzyme
butyrylcholinesterase has been developed in the milk of
goats and sheep which can reverse the poisoning of
organophosphates.
The goat’s mammary glands are transfected by the spider
gene through which they produce milk which constant of
strong strands known as Bio-Steel. The polymer is extracted
from the milk and the threads are weaved and used in the
preparation ofmilitaryuniforms,medical sutures,andracket
strings.
Organ transplantation (Xenotransplantation)
Transgenic animals have shown the best results when it
comes to humanizing the animal organs which are
successfully used for organ transplantation. The biggest
challenge is to establish the compatibility between animal
donors and human physiology, secondly, the aim isreducing
the transmission of pathogens from donor to human. The
two main approaches which are adopted to increase the
compatibility are, the transgenic animals have been
produced with human proteins on their surface, which has
drasticallyreducedtheincompatibility.Thesecondapproach
is to knock out the genes which are responsible for the
production of antigenic structures on the surface of the
animal’s organ. It was observed that the organ’s survival
time has increased to several months when the 1,3-
αgalactosyltransferase gene was knocked out. The RNAi-
mediated gene knockout is a successful tool to splice out the
PERV (Porcine Endogenous Retrovirus) gene which has
shown many complications in the human recipient for heart
or valve transplantation. Thus, technology has made safe
xenotransplantation from animals to humans. The animal
which is widely used for this purpose is the transgenicpig as
it shows a high level of anatomical and physiological
similarities with humans. The transgenic animals are being
used to transplant hearts, heart valves, skin (for burnt
cases), kidneys. The xenotransplantationis notpossible with
normal animals as there is a risk of hyperacute and vascular
rejection of animal organs in the human body.
Production of antibodies
The genetically modifiedanimalsarealsousedextensivelyto
produce monoclonal antibodies. Usually, mammary glands
are targeted for the production of antibodies. Mostly goat
mammary glands are targeted for the production of the
antibodies. The anibodies produced by transgenic animals
give resistant against many disease as theyarerecombinant.
Bovine offspring produced through transchromosomal
techniques expressedhumanimmunoglobulinintheirblood.
Agriculture
Ranching is one of the fields in agriculture in which animals
are reared for milk and meat purposes. The pigs are made
transgenic to improve their fat-muscle ratioandgrowthrate
by incorporating the porcine growth hormone genewiththe
human metallothionein as the promoter sequence, which
enables the transcription. The sows are modified with the
bovine lactalbumin gene to produce milk that is rich in
lactose content and produces a higher yield as compared to
the normal sows. Similarly, the transgenic sheep have been
used for high-quality wool (clear fleece) production by
knocking in the keratin-IGF-I gene into the sheep’s genome.
The bovine mammaryglandsaretransfectedwiththehuman
lysozyme gene, as human milk contains a higher amount of
lysozyme and lactoferrin which are the potential
antimicrobial and main source of iron in the milk
respectively. Thus with this, the bovine milk quality is
increased to many folds and more amount of lactoferrin is
best suited for feeding infants. The transgenic cattle have
been developed to produce superior quality milk that
contains beta and kappa casein which in turn yield the high-
quality production of milk-based products. Another
modification that is done in a bovine genome isknockingout
the B-lactoglobulin gene to produce lactose-free milk for
lactose intolerant individuals. Thus, transgenic animals can
be modified according to the need.
Improving reproductive performance and fertility
Some genes are known to increase the reproductive
performance within the animals. Such as the gene ESR gene
introduction within the swine genome can increase in the
litter size. Similarly the another gene Booroola fecundity
gene (FECB) when transfected in the sheep genome
ovulation rate was increased.
Disease resistance
The animals which are either used for xenotransplantation
or edible purposes possess a great threat of transmittingthe
infection which is prevalent in animals. Some disease does
affect animals but shows detrimental effectswhenpassed on
to humans. Thus, transgenic animals have produced disease
resistance by knocking out some specific genes from their
genome. The prion protein is one of the biggest threats
which could transmit from animals to human found in
animals. In humans, it is knownforcausingfatal neurological
disorders. Thus, the gene which encodes for this protein is
knocked out from the transgenic animals. Thus these
animals are much safer to use in any form as compared to
normal animals. Similarly, pigs are prone to influenza
infection thus the expression of the Mx1 gene is amplified in
their genome as the gene is known to provide resistance
against influenza.
The sheep are made resistant against the Maedi-Visna virus
(MVV) as it can be fatal to human beings if the infected
product is consumed. The cows have been made resistant to
one of the common pathology that is mastitis by
incorporating lysostaphin gene in their mammary gland.
Development of receptor-selective drug
The gene from the animal’s genome is knocked out with
encodes for the specific type of receptor subtype. Then the
drug is given, to check if it is acting on other receptors other
than the knockout one. These animals have helped in
formulating the selective agonist and antagonist for
particular receptor subtypes. In comparison to normal
animals, these types of selective studies cannot be done
precisely.
Conclusion
With the increase in medical advancement globally, the
medical fraternity still lags to find the cure of very common
diseases with normal animal models. Thus transgenic
animals have now slowly taken over the animal model of
human disease. This approach will change the fate of the
medical sciences in near future.
International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470
@ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 17
REFRENCE
[1] Ravi Rajoriya, Sweta Rajoriya, Nitesh Kumar (2013).
Transgenic animals: prospects for improving
livestock productivity. J.Bio.Innov2 (5):240-259.
[2] Manmohan Singhal, Niraj Kansara (2010).Transgenic
animals: production and application. IJPSR1 (9): 12-
22.
[3] Amare Bihon Asfaw &Ayalew Assefa (2019). Animal
transgenesis technology: A review. Cogent Food &
Agriculture5 (1):1-9.
[4] Uzoeto Henrietta Onyinye, Eruka Nick-Jnr Cetal
(2019). The use of transgenic animals in clinical
research; the pros and cons (review). Pharmacology
online 5:177-189.
[5] Fahimi Mohammed, TilayeShibbiruetal (2016).
Transgenic animal technology: Technique and its
application to improve animal productivity. IISTE
48:35-44.
[6] RenaldBundell (2006), transgenic animals- review
paper. Journal of animal and veterinary advances
5(11):935-938.
[7] Katarzyna Razny, Marek Bednarskietal (2014).
Animal models for hypertension research. Acta
biologicacracoviensiaSeries Zoologia 55(56):124-129.
[8] C. Delgado-Montemayor,P.Cordero-Perezetal (2015).
Models of hepatoprotective activity assessment.
Medicina Universitaria.17 (69):222-228.
[9] Murray Moo-Youngetal. “Comprehensive
Biotechnology”,Elsevierpublication.2ndedition,2011,
pp 365-377.
[10] Laurence L. Bruntonetal “The pharmacological basis
of therapeutics”, Mc Graw Hill publication, 12th
edition, 2011.

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Transgenic Animals A Better Approach towards Experimentation

  • 1. International Journal of Trend in Scientific Research and Development (IJTSRD) Volume 5 Issue 2, January-February 2021 Available Online: www.ijtsrd.com e-ISSN: 2456 – 6470 @ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 13 Transgenic Animals: A Better Approach towards Experimentation Swarnima Negi1, Dr. Sachdev Yadav2 1Scholar, 2Associate Professor, 1,2Department of Pharmacology Banasthali Vidyapith, Radha Kishnpura, Rajasthan, India ABSTRACT Animals play a crucial role in the development of medical products from medicines to various implants and major surgical procedures. They are not approved for human use until they qualify the safety parameters in animals. The animals play a pivotal role in drug discovery and development. Oneofthe most challenging aspects of targeting drugs for any pathological condition is the development of animal models. Animal models are nothing but an approach to replicate the general symptoms of the diseased condition which occur in humans. The whole pathophysiology cannot be replicated but, the symptoms which are known and precipitate the most in any pathological condition are positively reproduced within the animal. With the increasing need in the medical field, the paradigm is now slowly shifting towards transgenic animals as they have given a new dimension to medical sciencesto study the pathophysiology of the disease rather than focusing on the symptom-based analysis of the diseasedcondition. Thesegeneticallymodified organisms have shown groundbreaking results not onlyindevelopingmodels for various diseases but also in developing biopharmaceuticals, receptor- selective drugs, and have a huge contribution to xenotransplantation and the agriculture sector. This review article vividly describesthenewerapproaches that are adopted to develop transgenic animal models and also highlights certain limitations to the older approach of developing the models. KEYWORDS: Transgenic animals, in vivo models, ex vivo models, transgenesis, xenotransplantation, disease resistant animals How to cite this paper: Swarnima Negi | Dr. Sachdev Yadav"TransgenicAnimals:A Better Approach towards Experimentation" Published in International Journal of Trend in Scientific Research and Development(ijtsrd), ISSN: 2456-6470, Volume-5 | Issue-2, February 2021, pp.13-17, URL: www.ijtsrd.com/papers/ijtsrd38268.pdf Copyright © 2021 by author(s) and International Journal ofTrendinScientific Research and Development Journal. This is an Open Access article distributed under the terms of the Creative CommonsAttribution License (CC BY 4.0) (http://creativecommons.org/licenses/by/4.0) INTRODUCTION Animal models are nothing but an approach to replicate the general symptoms of the diseased condition in animals which occur in humans. Over the decades with the refinement in technology, the animal models can be are prepared by using different methods that involve some genetic and non-genetic approaches of model development. The animals which are involved in the research are of two types: 1. Non-genetically modified animal model of human disease The models developed can be in vivo, in vitro, or ex vivo. Usually, the study begins with the in vitro models later the data is extrapolated to in vivo and finally to humans. In vitro models – These are developed by analyzing the action of the drug either on the tissue of the organ from the animal itself or on the tissue homogenate. These models usually opted for the screening of any new chemical entity. For example, the hepatoprotective screening studies are done on primary hepatocytes or fresh hepatocytesextracted from the animal. In some studies, direct human cells can be taken for analyzing the action of drugs. Ex-vivo models- These models involve the organs extracted from the animal body and kept alive by giving almost same environment like inside the human body. For example heart is isolated from the animal bodyandactionofdifferentdrugs are analysed. Similarly the liver or part of liver is also isolated to study the hepatoprotective actions of different drugs. In-vivo models – In these models, there istheinvolvementof intact animals, which are produced by different methods. Physical models – The induction of symptoms in these is done by physical factors such as electric shock to induce convulsions. Similarly, the pain is induced by radiant heat or cold treatment to study the analgesic effect of the drugs. Chemical models – The symptoms are induced by exposing the animal to certain drugs, which alters the ongoing physiology of the animal and thus producesthesymptoms of the disease. For example to study the hepatoprotective action of any chemical entity the animals are exposed to hepatotoxic agents such as carbon tetrachloride, ethanol, acetaminophen, thioacetamide, etc. Similarly, todevelopthe model for antipyretic agents the lipopolysaccharides and yeast are injected into the animal. Streptozotocin and alloxan, synergistically destroy the pancreatic beta cells and produce the hyperglycemic condition within the animal. Surgical models – To develop certain symptoms the surgical interventions are adopted, one of the most common examples is pancreatectomy to induce diabetes-like condition in animals. Similarly to develop a model of IJTSRD38268
  • 2. International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470 @ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 14 myocardial infraction either the coronary artery ligation is one of the methods which is opted and others may include thoracotomy. To produce renovascular hypertension the either one or both the kidneysaretied,toproducesecondary hypertension within the rats. 2. Genetically modified animal model of human disease. (Transgenic models) Transgenic animals are the ones whose genome has been modified deliberately to achieve the desiredgenotype which resembles the diseased condition in human beings. Transgenic animals are considered the best models to work with because the researcher does not have to prepare the animal for a certain study which is usually donewithnormal animals a month or two months early before starting any drug therapy. Based on the increasing need for animals in medical sciences it has become more important to have animals that by birth show the characteristics of some ofthe diseases and disorders similar to that of human beings. The main advantage of this approach is it provides a method to rapidly introduce new genes into animals without cross- breeding. Limitationof anon-geneticallymodified animal model of human disease One of the major limitations of normal animals istheydonot provide a solid basis for the pathogenesis of a disease. Thus, the research always revolves around the development of symptomatic treatment of the disease.Thisfactisnothidden that almost all the drugs which are available forthecommon aliments are based on giving symptomatic relief be it diabetes, Multiple sclerosis,Parkinson'sdisease,Alzheimer's disease, etc. These models are produced by giving the animals various environmental exposure, which is a tedious and time-consuming task.Asanimalshavetobeprepared for the induction of any drug therapy weeks and months prior. For example for induction of hypertension, thedietofthe rat is modified, it has to be provided with an increased salt diet from a month earlier. Apart from this the methodswhich are adapted to induce the symptoms of any pathological condition are not always favorable. Sometimes because of the exposure of chemicals and surgery-induced models, the animals are known to produce symptoms other than the ones which are required, thus hampering the outcomeofthe final results. Although the researcherskeepshamcontrol for such purposes but cannot confidentlyruleoutthe possibility of surgery hampering the results. Production of genetically modified animals or transgenic animals The production of transgenic animals is the targeted mutation which is solely based on two approaches that are gene knock-in (insertion of any gene to therecipientanimal) and gene knock-out (deletion of a gene from the animal). This addition and deletion are based on the altered genetic makeup in humans during any pathological condition. The procedure involves the manipulation of endogenous genomic DNA by transfecting the desired set of genes from the donor animal. The process deals with the introduction of specific mRNA into the germ cells of the host by using recombinant DNA technology, with the thought that if germ cell lines are altered, the characters will be passed on to the forthcoming generation in normal reproduction. This whole process of transferring the manipulated gene or altering the DNA sequence is called transgenesis. Transpharmers is the name given to the transgenic animals which are involved in the production of pharmaceutical products. Table 1 shows the different methods for the production of transgenic animals. Table 1 Methods of producing transgenic animals S/N Technique Procedure Limitations Examples Gene knock-in 1. DNA microinjection (Pronucleus microinjection) The eggs are obtained from a donor female and in vitro made to fuse with the sperms. The transgene is microinjected to the male pronucleus in the premature zygote. The zygote is then transplanted to the uterus of the pseudopregnant female. The success rate of this method is very less, few offsprings produced are transgenic. The technique is not popular as it is tedious and very few cells can be handled at a time. Muta mouse, big blue transgenic rats. 2. Embryonic Stem cell-mediated gene transfer The totipotent stem cells are isolated from the donor pregnant female. They are cultured invitro and later transfected with the desired gene. The pure population of transfected ES cells is microinjected to the blastocyst. The blastocyst is finally implanted into the uterus of the pseudopregnant recipient animal. The progeny produce by this technique is chimeric i.e. they contain both normal cells and genetically modified cells. Mice, rats 3. Retrovirus mediated gene transfection The vectors used for transfection is retrovirus which include lentivirus and adenovirus.These are modified by incorporating the desired gene into its genome. Later the recombinant virus is microinjected into the embryo of the animal and grown-up to blastocyst in invitro. Later the a blastocyst is implanted in the pseudopregnant female. The progeny produced is chimeric in the F1 generation. The probability of offspring with transgene is very low. Pigs,mice (Smian virus was introduced in mice for the first time)
  • 3. International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470 @ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 15 4. Transposons (Jumping gene) These are the small DNA sequence that is used as a vector, which can jump from one place to another in a genome simply by cut and paste mechanism. Thus, recombinant transposons are microinjected into the embryo of the animal to have the desired character in the progeny. - Transgenic insects, zebra fishes, chicken cattle. 5. Somatic cell Nuclear Transfer The oocytes are arrested in meiosis II of the cell cycle, specifically at metaphase or telophase. These are reprogramed with the nucleus of the somatic cell (skin cell, liver, fat, or any other organ of the body is extracted). The cell is stimulated with an electric shock to begin the cell cycle. - Dolly sheep (mammary cell somatic cell was incorporated) 6. Sperm Mediated Gene Transfer (SMGT) Mature spermatozoa are allowed to bind to the exogenous transfected DNA which is then injected through ICSI (Intracytoplasmic Sperm Injection) to the cytoplasm of the oocyte. The whole procedure is dependent upon the binding of the sperms to the DNA without losing its activity. Cattle, Pigs 7. Testis cell implantation The testis is removed from the donor male and transfected with the desirable gene, the cells are then cultured and microinjected to the lumen of seminiferous tubules of the recipient animal. Later the recipient was followed to mate. - - Gene knock-out 8. RNA Interference (RNAi) The siRNA has the complementary sequence which attaches covalently with the specific sequence on the principle mRNA strand. The powerful digesting enzyme argonaut destroys the complementary sequence on the principle mRNA strand and silences the particular gene. - Salt sensitive rats used in the antihypertensive study. The superiority of transgenic models to the non-genetic animal model of human disease The transgenic models are superior in every respect as compared to the other non genetically modified models of human disease. The transgenic animals have shown pioneering results in various fields. It has not only pavedthe path to developing new frontiersinmedical sciencesbutalso various other fields including agriculture. The scope of transgenic animals is not only limited to serve humanity in the medical area but also in various other sectors which is not seen with non genetically modified animals. The below mentioned are the areas where transgenic have showntheir contribution more as compared to the non-genetic models which are restricted to only animal models of human disease. Human disease models The transgenic models are by far the best models to study the pathogenesis of the diseases. This technology has enabled the researcher to look beyond just symptoms and have focused the studies towards the curative aspect of treating the disease. Thepreferencehasnowshiftedtowards the transgenic models in almost every research. This approach can decrease the number of higher animals to be used in the experimentation likes canines, nonhuman primates. A successful model can be produced by modifying the genomic sequence. This approach has very well defined the pathogenesis of human diseases and has leadtothebirth of gene therapy. The advantagewhichcomeswithtransgenic models is we are able to produce models for conditions like those whose models have not developed yet in normal animals. The transgenic animals are easy to work with because they do not require induction therapy. For example, to study the basis of essential hypertension, no such model has been developed which could give an insight over the pathogenesis of the same. But transgenic animals have been produced known as Spontaneous Hypertensive Rats (SHR) and SHR-SP stroke-pronehypertensiverats,Dahl and Sabra rats which are salt-sensitive rats, and rats which already have highly activated RAAS. Thusthestudybecomes easy with the genetic models. Production of Biopharmaceuticals The transgenic animals are known as bioreactors when it comes to the production of biopharmaceuticals. The biopharmaceutical contains vaccines, blood products, gene therapies, etc. Several proteins like AT-III(antithrombinIII), TPA (tissue plasminogen factor) are produced in the mammary glands of goats and sheep which are later extracted from them. Another blood product is produced in transgenic swine is hemoglobin that has the same oxygen- carrying capacity as that of human hemoglobin. Certain enzymes are also produced by the use of transgenic animals, like the enzyme α-glucosidase which is required in
  • 4. International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470 @ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 16 patients with Pompe disease thus the enzyme isproduced in the milk of transgenic rabbits and later extracted and purified to be given to the patients. Similarly, the enzyme butyrylcholinesterase has been developed in the milk of goats and sheep which can reverse the poisoning of organophosphates. The goat’s mammary glands are transfected by the spider gene through which they produce milk which constant of strong strands known as Bio-Steel. The polymer is extracted from the milk and the threads are weaved and used in the preparation ofmilitaryuniforms,medical sutures,andracket strings. Organ transplantation (Xenotransplantation) Transgenic animals have shown the best results when it comes to humanizing the animal organs which are successfully used for organ transplantation. The biggest challenge is to establish the compatibility between animal donors and human physiology, secondly, the aim isreducing the transmission of pathogens from donor to human. The two main approaches which are adopted to increase the compatibility are, the transgenic animals have been produced with human proteins on their surface, which has drasticallyreducedtheincompatibility.Thesecondapproach is to knock out the genes which are responsible for the production of antigenic structures on the surface of the animal’s organ. It was observed that the organ’s survival time has increased to several months when the 1,3- αgalactosyltransferase gene was knocked out. The RNAi- mediated gene knockout is a successful tool to splice out the PERV (Porcine Endogenous Retrovirus) gene which has shown many complications in the human recipient for heart or valve transplantation. Thus, technology has made safe xenotransplantation from animals to humans. The animal which is widely used for this purpose is the transgenicpig as it shows a high level of anatomical and physiological similarities with humans. The transgenic animals are being used to transplant hearts, heart valves, skin (for burnt cases), kidneys. The xenotransplantationis notpossible with normal animals as there is a risk of hyperacute and vascular rejection of animal organs in the human body. Production of antibodies The genetically modifiedanimalsarealsousedextensivelyto produce monoclonal antibodies. Usually, mammary glands are targeted for the production of antibodies. Mostly goat mammary glands are targeted for the production of the antibodies. The anibodies produced by transgenic animals give resistant against many disease as theyarerecombinant. Bovine offspring produced through transchromosomal techniques expressedhumanimmunoglobulinintheirblood. Agriculture Ranching is one of the fields in agriculture in which animals are reared for milk and meat purposes. The pigs are made transgenic to improve their fat-muscle ratioandgrowthrate by incorporating the porcine growth hormone genewiththe human metallothionein as the promoter sequence, which enables the transcription. The sows are modified with the bovine lactalbumin gene to produce milk that is rich in lactose content and produces a higher yield as compared to the normal sows. Similarly, the transgenic sheep have been used for high-quality wool (clear fleece) production by knocking in the keratin-IGF-I gene into the sheep’s genome. The bovine mammaryglandsaretransfectedwiththehuman lysozyme gene, as human milk contains a higher amount of lysozyme and lactoferrin which are the potential antimicrobial and main source of iron in the milk respectively. Thus with this, the bovine milk quality is increased to many folds and more amount of lactoferrin is best suited for feeding infants. The transgenic cattle have been developed to produce superior quality milk that contains beta and kappa casein which in turn yield the high- quality production of milk-based products. Another modification that is done in a bovine genome isknockingout the B-lactoglobulin gene to produce lactose-free milk for lactose intolerant individuals. Thus, transgenic animals can be modified according to the need. Improving reproductive performance and fertility Some genes are known to increase the reproductive performance within the animals. Such as the gene ESR gene introduction within the swine genome can increase in the litter size. Similarly the another gene Booroola fecundity gene (FECB) when transfected in the sheep genome ovulation rate was increased. Disease resistance The animals which are either used for xenotransplantation or edible purposes possess a great threat of transmittingthe infection which is prevalent in animals. Some disease does affect animals but shows detrimental effectswhenpassed on to humans. Thus, transgenic animals have produced disease resistance by knocking out some specific genes from their genome. The prion protein is one of the biggest threats which could transmit from animals to human found in animals. In humans, it is knownforcausingfatal neurological disorders. Thus, the gene which encodes for this protein is knocked out from the transgenic animals. Thus these animals are much safer to use in any form as compared to normal animals. Similarly, pigs are prone to influenza infection thus the expression of the Mx1 gene is amplified in their genome as the gene is known to provide resistance against influenza. The sheep are made resistant against the Maedi-Visna virus (MVV) as it can be fatal to human beings if the infected product is consumed. The cows have been made resistant to one of the common pathology that is mastitis by incorporating lysostaphin gene in their mammary gland. Development of receptor-selective drug The gene from the animal’s genome is knocked out with encodes for the specific type of receptor subtype. Then the drug is given, to check if it is acting on other receptors other than the knockout one. These animals have helped in formulating the selective agonist and antagonist for particular receptor subtypes. In comparison to normal animals, these types of selective studies cannot be done precisely. Conclusion With the increase in medical advancement globally, the medical fraternity still lags to find the cure of very common diseases with normal animal models. Thus transgenic animals have now slowly taken over the animal model of human disease. This approach will change the fate of the medical sciences in near future.
  • 5. International Journal of Trend in Scientific Research and Development (IJTSRD) @ www.ijtsrd.com eISSN: 2456-6470 @ IJTSRD | Unique Paper ID – IJTSRD38268 | Volume – 5 | Issue – 2 | January-February 2021 Page 17 REFRENCE [1] Ravi Rajoriya, Sweta Rajoriya, Nitesh Kumar (2013). Transgenic animals: prospects for improving livestock productivity. J.Bio.Innov2 (5):240-259. [2] Manmohan Singhal, Niraj Kansara (2010).Transgenic animals: production and application. IJPSR1 (9): 12- 22. [3] Amare Bihon Asfaw &Ayalew Assefa (2019). Animal transgenesis technology: A review. Cogent Food & Agriculture5 (1):1-9. [4] Uzoeto Henrietta Onyinye, Eruka Nick-Jnr Cetal (2019). The use of transgenic animals in clinical research; the pros and cons (review). Pharmacology online 5:177-189. [5] Fahimi Mohammed, TilayeShibbiruetal (2016). Transgenic animal technology: Technique and its application to improve animal productivity. IISTE 48:35-44. [6] RenaldBundell (2006), transgenic animals- review paper. Journal of animal and veterinary advances 5(11):935-938. [7] Katarzyna Razny, Marek Bednarskietal (2014). Animal models for hypertension research. Acta biologicacracoviensiaSeries Zoologia 55(56):124-129. [8] C. Delgado-Montemayor,P.Cordero-Perezetal (2015). Models of hepatoprotective activity assessment. Medicina Universitaria.17 (69):222-228. [9] Murray Moo-Youngetal. “Comprehensive Biotechnology”,Elsevierpublication.2ndedition,2011, pp 365-377. [10] Laurence L. Bruntonetal “The pharmacological basis of therapeutics”, Mc Graw Hill publication, 12th edition, 2011.