Drug Delivery: Plant Lectins as Bioadhesive Drug Delivery Systems

doi:10.4236/jbnb.2011.225073

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Journal of Biomaterials and Nanobiotechnology, 2011, 2, 614-621

doi:10.4236/jbnb.2011.225073 Published Online December 2011 (http://www.scirp.org/journal/jbnb)

Drug Delivery: Plant Lectins as Bioadhesive Drug

Delivery Systems

Marija Gavrovic-Jankulovic, Radivoje Prodanovic

Department of Biochemistry, Faculty of Chemistry, University of Belgrade, Belgarde, Serbia.

E-mail: mgavrov@chem.bg.ac.rs

Received September 17th, 2011; revised October 9th, 2011; accepted November 11th, 2011.

ABSTRACT

Selective targeting of drugs to the proposed site of action provides therapeutic advantages such as reduced toxicity and

smaller dose levels. Despite a huge progress made in drug design and delivery systems, many challen g es still ha ve to b e

solved. Small therapeutic drugs always have the potential to pass into the kidneys and be excreted from the body. The

use of macromolecular constructs (carriers) that allow longer circulation times, contribute to improved chemical func-

tionality and more precise drug delivery is an attractive alternative option. Bioadhesive systems which will utilize in-

tense contact to increase the drug concentration gradient could be an attractive approach. Because of their specific

carbohydrate-binding, lectins can in teract with g lycoco n jugates presen t o n the ep ith elial cells th a t line all o f th e organs

exposed to the external environm ent. The unique carboh ydrate specificitie s of plant lectins can facilitate mucoadh esion

and cytoadhesion of drugs. As immunostimulatory molecules with an adjuvant effect plant lectins can also be employed

in vaccine development.

Keywords: Drug Delivery, Epithelium, Plant Lectin, Polymers, Vaccine

1. Introduction

The traditional routes of drug administration are nasal,

oral, subcutaneous, intramuscular, intravenous, topical,

ophthalmic and rectal. A wide variety of polymeric bio-

materials are compounds of various formulations and

devices which are routinely used for delivering drug to

the body. However, these medication delivery systems

may not always achieve optimal drug concentration at

the appropriate site, nor do they necessarily minimize

local or systemic toxicity [1]. Therefore, there has been

enormous interest in developing controlled-release for-

mulations and devices that can maintain a desired blood

plasma level of the drug for longer periods of time with-

out reaching a toxic level or dropping below the mini-

mum effective level [2].

This paper will give an overview of the systems that

have been used for drug delivery via mucosal surfaces

and will showcase recent employment of plant-derived

lectins in creation of drug delivery vehicles, but also their

immunomodulatory p ot ential.

2. Mucoadhesive Polymer Drug Delivery

Systems

Mucoadhesive drug delivery systems are vehicles which

utilize the property of bioadhesion of certain polymers

that become adhesive on hydration [3] and can be used

for targeting a drug to the particular region of the body

for an extended period of time [4]. In the case of a

polymer attached to the mucin layer of a mucosal tissue

the term “mucoadhesion” is employed [5].

The polymeric properties which are relevant for high

retention via mucoadhesive interactions at particular

targeted sites include hydrophobicity, negative charge

potential and the presence of hydrogen bond forming

groups [6]. In add ition, the polymer should p ossess suffi-

cient flexibility to penetrate the mucus network and be

biocompatible, non-toxic and economically favorable [7].

According to Park and Robinson, [8] polymers com-

monly employed in the manufacturing of mucoadhesive

drug delivery platforms that adhere to mucinepithelial

surfaces are categorized as follows:

 Polymers that are bioadhesive due to their stickiness,

 Polymers that adhere through nonspecific, noncovalent,

primarily electrostatic interactions,

 Polymers that bind to a specific receptor on the cell

surface.

2.1. First-Generation Mucoadhesive Polymers

According to the net overall charge, mucoadhesive poly-

Drug Delivery: Plant Lec ti ns a s B ioad hesi ve Drug Delivery Syste ms615

mers have been divided into three categories: anionic

polymers, cationic polymers, and non-ionic polymers,

with the first two groups exhibiting the highest mucoad-

hesive strength [9]. Due to their high mucoadhesive po-

tential and low toxicity anionic polymers are the most

widely employed mucoadhesive vehicles in pharmaceu-

tical formulations. Anionic polymers contain carboxyl

and sulphate functional groups that give rise to a net

overall negative charge. Examples include poly-acrylic

acid (PAA), its weakly cross-linked derivatives and so-

dium carboxymethylcellulose (NaCMC). Both polymers

possess excellent mucoadhesive characteristics because

of the formation of hydrogen bonding interactions with

mucin from porcine stomach [10].

Due to its good biocompatibility, biodegradability and

favorable toxicological properties [11] chitosan is among

the most extensively investigated cationic polysaccha-

rides, produced by the deacetylation of chitin [12]. Chi-

tosan binds to mucin via ionic interactions between pri-

mary amino functional groups and sialic and sulphonic

acid of mucins [13,14]. The hydroxyl and amino groups

may also interact with mucus via hydrogen bonding.

The major benefit of using chitosan within pharma-

ceutical applications has been its chemical reactivity and

the easiness of addition of various chemical groups, in

particular to the C-2 position, allowing the formation of

novel polymers with improved functionality. Using such

modifications, the properties of chitosan may be tailored

to the requirements of specific pharmaceutical-techno-

logical challenges [15].

2.2. Second-Generation Mucoadhesives

The major disadvantage in using traditional, non-specific

mucoadhesive systems is that adhesion may occur at sites

different than those intended, i.e. delivery of the drug

may occur nonspecifically to any region of the 10-meter

long gastrointestinal tract. Unlike first-generation non-

specific polymers, certain second-generation polymers

are less susceptible to mucus turnover rates, with a po-

tential to bind directly to mucosal surfaces via the proc-

ess of “cytoadhesion”. Taking into consideration differ-

ent surface topogr aphy of poten tial target sites, this could

be an advantage for the creation of more accurate drug

delivery ve hi cles.

3. Mucus Structure

In order to improve bioadhesive properties of drug deliv-

ery vehicles it is necessary to reveal structural features of

epithelial surfaces for which the drug is targeted to. Mu-

cus is a complex viscous secretion synthesized by spe-

cialized goblet cells in the columnar epithelium that lines

all of the organs exposed to the external environment.

This includes the respiratory tract, the gastrointestinal

tract, the reproductive tract, and the oculo-rhino-oto-

laryngeal tract [16]. Its physiological functions at these

locations include maintaining a hydrated layer over the

epithelium, shielding the epithelial surfaces against phy-

sical and chemical damage, posing a barrier to pathogens

and nontoxic substances and acting as a permeable gel

layer for the exchange of gases and nutrients with the

underlying epithelium [17,18]. Mucus is the first barrier

with which nutrients and enteric drugs must interact and

pass through, in order to be absorbed and to reach the

circulatory system and respective target organs. The

mucus blanket is highly hydrated (95% water), with the

main component of this extracellular epithelial layer re-

sponsible for its viscosity and gel-like properties being

the glycoprotein mucin.

Mucins are large (0.5 to 20 MDa) membrane bound

and extracellular glycoproteins. They are highly glycol-

sylated and consist of about 80% of carbohydrates, pri-

marily N-acetyl-D-galactosamine, N-acetyl-D-glucosa-

mine, fucose, galactose, and sialic acid (N-acetylneura-

minic acid), with traces of mannose and sulfate.

The oligosaccharide chains, consisting of 5 - 15 mono-

mers, exhibit moderate branching and are attached to the

protein core by O-glycoside bonds via the hydroxyl side

chains of serine and threonine and arranged in a “bottle

brush” configuration around the protein core. NMR

studies of MUC1 secondary structure revealed very little

alpha helixes, a small amount of beta sheets and mostly

random coil [19,20]. Currently, approximately 19 human

mucin (designated MUC) genes have been identified,

cloned and partially sequenced, and homologs of many

of these have been identified in mice and rats [21].

The well-know tendency of other substances to adhere

to mucin, known as mucoadhesivity, is not surprising

given that this glycoprotein exhibits electrostatic, hydro-

phobic, and hydrogen bonding interactions [22]. Mucus

covers all the organs that are exposed to the external en-

vironment and therefore those locations are targets for

bioadhesi ve dr ug deli ve ry vehicles.

4. Mucosal Membrane Delivery

4.1. Intranasal Delivery

Intranasal formulation is regarded as a patient-friendly

route of drug administration. In terms of pharmacokinet-

ics, the absorption rate is rapid and followed by a faster

onset of action compared with oral and intramuscular

administration. Due to the high total area which is sur-

rounded by a dense vascular network the nasal mucosa is

regarded as an excellent absorptive surface [23]. In addi-

tion, the advantage of this route lies in the fact that the

hepatic first-pass metabolism is avoided, compared to

oral drug administration, in which a clinically significant

Drug Delivery: Plant Lectins as Bioadhesive Drug Deliv ery Systems

616

portion of the drug taken is degraded during first-pass

metabolism, requiring a higher oral dose for the given

effect. Intranasal drugs can be delivered in a variety of

formulations that include powders, drops, topical gels,

and sprays.

The most commonly employed intranasal pharmaceu-

ticals are solutions of sympathomimetic vasoconstrictors

as nasal decongestants. Apart from local effects, the in-

tranasal route of drug administration is often employed

for induction of systemic effects [24]. For example, the

synthetic hormone desmopressin exerts its action on the

kidneys by reducing urine production. It is formulated for

intranasal application, frequently prescribed for treatment

of Diabetes insipidus.

Another systemic effect achieved by intranasal drug

administration is used in the treatment of patients with

vitamin B12 deficiency. After normalization with intra-

muscular vitamin B12 therapy, maintenance of vitamin

B12 concentration is achievable with CaloMist (cyano-

cobalamin) nasal spray that is used on a daily base [25].

4.2. Gastrointestinal Tract Delivery

Despite the tremendous advances in drug delivery the

oral route still remains the preferred route for the ad-

ministration of therapeu tic agen ts due to low cost, ease of

administration and high levels of patient compliance

[26].

However, the delivery of therapeutic agents to, or via

the oral cavity is limited by the efficient removal mecha-

nisms that exist in this area. The oral cavity is employed

as a site for local and systemic drug delivery [27]. He-

patic first pass metabolism and drug degradation within

the gastrointestinal tract are additional obstacles in the

oral administration of certain classes of drugs, such as

peptides and proteins.

It is generally believed that mucoadhesive drug deliv-

ery systems have not reached their full potential within

oral drug delivery, since their lack of sufficient adhesion

onto the GI tract does not provide prolonged residence

time [28]. Targeted drug delivery systems have mainly

been focused on mucoadhesive patches and microparti-

cles using first-generation polymers [29]. The problem

with mucoadhesive solid formula tions, such as tablets, is

their poor adherence to mucosal surfaces, combined with

their vigorous movement to the GI tract [6]. However,

second-generation vehicles have attracted more attention

to drug delivery via the GI tract. In an animal model, a

thiolated chitosan tablet has been employed for the oral

delivery of insulin in rats [30]. In non-diabetic rats a

more decreased glucose level was achieved with thio-

lated chitosan insulin tablets than with unmodified poly-

mer insulin tablets. The explanation for this was that

chitosan and the thiol group s showed an inhib itory effect

on proteolytic enzymes, together with the penetration

enhancing effect of the polymer system, and its improved

mucoadhesi ve potential.

4.3. Ocular Drug Delivery

The delivery of aqueous ophthalmic drug solutions shows

limitations due to the efficient removal mechanisms that

exist within the precorneal area. Ocular drug absorption

requires good corneal penetration, along with a pro-

longed contact ti me with the corneal tissue [31]. Various

approaches have been considered to extend the residen ce

time of topically applied medications in the precorneal

region and various formulations such as suspensions,

inserts, and aqueous gels have been investigated [32]. It

is estimated that almost 95% of medication delivered by

eye drops is lost as the medication mixes with tears and

drains into the nasal canal [33]. The first report on the

use of soft contact lenses in drug deliv er y was reported in

1965 for effective treatment of ocular conditions [34]. A

drug delivery smart lens has been an ticipated to be useful

in the control of infection during wound healing follow-

ing trauma and surgery. Several research groups have

been working on strategies for smart lenses that will

release medications more evenly over extended periods

[35]. One approach in the smart lens technology is based

on the suspension of the pharmaceutical in a layer of

biodegradable polymer (poly-lactic-co-glycolic acid,

PLGA). The relative amount of PLGA to the pharma-

ceutical will regulate the amount that passes through the

lens over time. The more PLGA, the slower the drug is

released. In lab tests, these multilayer lenses demon-

strated ability to release ciprofloxacin for up to 100 days

[36].

4.4. Buccal Drug Delivery

The buccal cavity is an attractive target for drug delivery

formulations as it is easily accessible. Delivery systems

used include mouthwashes, aerosol sprays, chewing

gums, bioadhesive tablets, gels and patches [37]. The

obstacles associated with drug therapy within the oral

cavity are the rapid elimination of drugs due to the

flushing effect of saliva, the non-uniform distribution of

drug release from a solid or semisolid delivery system

within saliva, and the taste and “mouth discomfort” [38-

41]. In case of side reactions and toxicity buccal drug

delivery can be promptly terminated, and therefore this

route is considered safe and easy for drug utilization [42].

Due to its unique structural and physiological properties

the oral mucosa offers several opportunities for drug de-

livery. As the mucosa is highly vascularised, any drug

diffusing across the oral mucosa membranes has direct

access to the systemic circulation and will bypass hepatic

circulation. The rate of blood flow through the oral mu-

Drug Delivery: Plant Lec ti ns a s B ioad hesi ve Drug Delivery Syste ms617

cosa is substantial, and is not considered to be the rate-

limiting factor in the drug absorption [43]. In addition,

saliva a relatively mobile fluid with less mucin and lim-

ited enzymatic activity [44], is favorable for protein and

peptide delivery.

The first-generation mucoadhesives, such as carboxy-

methylcellulose [45] have been extensively evaluated

mostly for the treatment of periodontal disease [46], and

resent research has been mainly focused on the con-

trolled delivery of therapeutic reagents such as peptides,

and proteins [47].

4.5. Vaginal Drug Delivery Systems

Drug delivery via the vaginal rout is an attractive option

due to the avoidance of hepatic first-pass metabolism and

a reduction in the incidence of gastrointestinal side ef-

fects. The advantages for systemic drug delivery are the

large surface area, rich blood supply and high permeabil-

ity, while low retention time is a disadvantage because of

the self-cleansing effect of the vaginal tract [48]. Data

from literature demonstrated the superiority of vaginal

placement over the oral route regarding minimization of

general and gastrointestinal side effects [49]. A very at-

tractive issue concern ing the vaginal drug delivery refers

to prevention and treatment of sexually transmitted dis-

eases. Some of these approaches will be discussed later.

5. Lectins as Specific Site Directed

Bioadhesives

Due to the lack of specificity, the first generation of mu-

coadhesive polymers provides nonspecific binding to

mucosal surfaces in the body. Therefore, their employ-

ment in the creation of mucoadhesive drug delivery sys-

tems for a particular tissue is limited. Creation of poly-

mers and microspheres with attached mucus or cell-spe-

cific ligands have increased therapeutic benefits and

made site-specific drug delivery possible. In contrast to

classical mucoadhesion, which relies on nonspecific in-

teractions of polymer chains and mucins, the lectin in-

teractions with mucins are very specific.

Lectins are a highly heterogeneous group of proteins

and glycoproteins of non-immune origin that bind to

carbohydrates specifically and noncovalentlly. The term

“lectin” derives from the Latin verb legere—to select or

choose. Lectins were first discovered in plants; however,

their presence was confirmed in most living organisms

(bacteria, animals and humans). Lectins are involved in

various biological processes: cell-to-cell recognition and

communication, particularly in the mammalian immune

system (transendothelial migration), adhesion and attack

of infectious agents on host cells, clearance of glycopro-

teins from the blood circulation, etc. [50,51]. The asso-

cia- tion constant Ka of lectins with monosaccharides is

usu- ally in the range of 103 - 104 [52]. As carbohydr ate-

binding proteins lectins can increase the adherence of

drug delivery vehicles to the mucose surfaces.

The utilization of lectin-mediated drug targeting is

based on the fact that most cell surface proteins, and

many lipids in the plasma membrane, are glycosylated,

and these glycans represent ligands for lectins. Different

cell types express various glycan patterns, particularly in

pathological states, such as transformed or cancerous

cells, where completely different glycans are expressed

compared with their healthy counterpar ts [53]. Th eref or e,

lectins are regarded as potential carrier molecules to tar-

get drugs specifically to various cells and tissues. Selec-

tion from natural biological material or creation by re-

combinant DNA technology of a specific lectin, and its

coupling to macromolecular drugs or particular drug car-

riers may lead to efficient cellular uptake and subsequent

intracellular routing of such delivery systems. Russel-

Jones and coworkers were able to demonstrate transloca-

tion of nanoparticles which had been conjugated to

lectins, such as wheat germ agglutinin (WGA), concana-

valin A (Con A) and LBT, the binding subunit of heat-

labile toxin from E. coli, [54] across the cell layer in an

in vitro model of intestinal epithelial cells, whereas A.

aurantia lectin, from the edible orange cup mushroom,

was able to mediate antigen delivery to M cells [55].

Jain and Jangdey [56] reported on the development of

a ConA conjugated gastroretentive multiparticulate de-

livery system of clarithromycin for the effective treat-

ment of colonization of Helicobacter pylori. Attachment

of Con A lectin to ethylcellulose microspheres signifi-

cantly increased the mucoadhesiveness and also con-

trolled the release of clarithromycin in simulated gastric

fluid. Prolonged gastric residence time of over 6 h was

achieved in rabbits for Con A-conjugated microspheres

of clarithromycin.

For the patient, the gastrointestinal route is the most

convenient and attractive method for systemic delivery of

drugs. However it is one of the most challenging routes

of administration. The acidity of the gastric juice, as well

as the gastric and intestinal enzymes and brush border

hydrolases can degrade the drug. Also the viscous mucus

blanket overlying the epithelium can limit the absorptive

capacity of the cell layer, therefore successful mucosal

absorption of drugs requires drug formulations which

prolong the residence time at the site of absorption and

provide an intimate contact to the absorptive tissue [49].

Among reagents available to direct drugs specifically to

the gut epithelium, plant lectins are prime candidates,

due to their stability in low pH conditions and their abil-

ity to bind specifically to epithelial cells [50,57]. It has

been shown that recombinant banana lectin (rBanLec),

preserved structural stability and its carbohydrate-bind-

Drug Delivery: Plant Lectins as Bioadhesive Drug Deliv ery Systems

618

ing potential under the conditions of simulated gastric

fluid and simulated intestinal fluid. In this regard it can

be considered as a candidate for the novel bioadhesive

lectin-based drug delivery systems to the gastrointestinal

tract [58].

A recently published paper on the antiviral activity of

BanLec attracted lots of attention even beyon d the scien-

tific community, as it has been shown that BanLec has

the potential to inhibit genome integration of human

immunodeficiency virus (HIV) in the target cell, and

hence viral replication [59]. Viruses containing high-

mannose glycosylated envelopes, such as human immu-

nodeficiency virus type-1 (HIV-1), are potential targets

for BanLec binding. The entry of human immunodefi-

ciency virus into cells requires th e sequential interaction s

of the viral exterior envelope glycoprotein, gp120, with

the CD4 glycoprotein and a chemokine receptor on the

host cell surface. It has been found that BanLec inhibited

HIV-1 infection by binding to the glycosylated viral en-

velope in a way that blocks cellular entry of the virus.

The relative anti-HIV activity of BanLec compared fa-

vorably to other anti-HIV lectins, such as the snowdrop

lectin and griffithisin, and to T-20 and maraviroc, two

anti-HIV drugs currently in clinical use. Based on these

results, BanLec is a potential component for an anti-viral

microbicide that could be used to prevent the sexual

transmission of HIV-1. Although concerns have been

raised about the potential toxicity of lectins, creation of

recombinant therapeutic protein which can be attached to

polyethylene glycol (PEG) polymer chains to change

bioavailability and reduce toxicity [59].

As ocular drug delivery is limited both by patients’

acceptability and by the limited time that the dosage form

is retained within the precorneal region, Nicholls et al.

[60] tried to identify lectin receptors within the precor-

neal region as potential targets for a lectin containing

ocular dosage form, and thus facilitate prolonged drug

delivery. In an ex-vivo experiment conducted on rat cor-

neal and conjunctival intact (unfixed) epithelia, the

lectins from Solanum tuberosum (potato) and Helix po-

matia (edible snail), with specificity for N-acetyl-D-glu-

cosamine and N-acetyl-D-galactosamine respectively,

were the most promising lectins with binding to ocular

tissues in terms of a 10 s contact [60]. Following this, a

study which explored the potential of these lectins to

cause inflammation and tissue necrosis was performed

with New Zealand white rabbits. The authors concluded

that Solanum tuberosum and Helix pomatia lectins dem-

onstrated minimal acute irritancy, and would be suitable

for formulations and in vivo studies [61].

Beside specific mucoadhesion and cytoadhesion, it has

been shown that certain plant lectins are prone to induc-

tion of immune response upon oral feeding [62]. In this

regard, utilization of novel immunostimulatory mole-

cules having an adjuvant effect to enhance or redirect an

immune response against target immunogens has been an

important issue in vaccine development. Based on its

IgG4-inducing potential, BanLec is regarded as a poten-

tially useful protein carrier for oral antihapten immuniza-

tion in humans suffering from IgE mediated allergic dis-

orders [63]. Resistance to the proteolytic enzymes of the

gastrointestinal tract [64] enables BanLec to pass the

mucosal barrier and interact with the immune system,

inducing a strong IgG4 immune response.

6. Conclusions

In the recent past, new technologies have established

DNA arrays that distinguish different cell types through

the profiling of gene expression. However, cell surface

phenotypes are not only determined by gene expression.

Posttranslational modifications by glycosylation and re-

gulation of protein localization are believed to be essen-

tial in determining the identity of a particular cell type at

a given stage of differentiation. Therefore, it should be

possible to distinguish different cell phenotypes through

the profiling of cell-surface glycans. In this regard, it

seems feasible to design drug delivery vehicles with im-

proved bioadhesive features, and particularly with spe-

cific cytoadhesive properties. A very promising concept,

which can greatly expand the utility of lectins and afford

more accurate and reliable cellular identification and

targeting, is the development of novel lectin libraries

with diverse specificities [65]. Such an approach offers

the possibility of more specific targeting, attachment and

controlled release of no vel lectin-based vehicles. Despite

the promise still lot of investigation has to be conducted

in order to produce improved lectin-based therapeutic

reagents.

7. Acknowledgements

This work is supported by Grant No. 172049, sponsored

by the Ministry of Education and Science, Republic of

Serbia.

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