| dc.description.abstract | Tsetse flies are haematophagous arthropods which feed on a diverse
range of vertebrates. The Glossina morsii ans group of tsetse flies are
among the important vectors of the African trypanosomes. The African
trypanosomes are the causative agent of the diseases, sleeping sickness in
man and nagana in livestock. The trypanosomes are protozoal parasites
with a complicated life cycle both within the vertebrate host and the tsetse
fly vector. These diseases, are generally fatal unless treated. Once a tsetse
fly ingests trypanosomes during feeding, the parasites pass through the
oesophagus to the midgut. Here, the parasites are exposed to a hostile
environment which consists of the digestive enzymes like trypsin, a
trypsin-like enzyme, chymotrypsin, carboxypeptidase A and B, and an
aminopeptidase. Out of the six digestive enzymes, trypsin is the most
abundant involved in digestion. The tsetse fly midgut trypsin has been
implicated in the lysis of the trypanosomes as well as their transformation
into procyclic forms. Similarly, "lectins", a group of proteins that bind
carbohydrates specifically, ~aye been reported to be secreted by tsetse
midgut in response to a bloodmeal. These "lectins" which are specific for
glucosamine have been proposed to have two functions. Firstly, they
mediate lysis of the parasites that enter the fly midgut .
Secondly, they provide the signal for the surviving parasites to
differentiate to procyclic forms. Furthermore, in vivo studies have shown
that flies infected with parasites and maintained on a diet of blood
containing D-glucosamine develop elevated levels of midgut infections. It
might be argued that the reason for the increased infections is due to
inhibition of the "lectins" by D-glucosamine. Since the "lectins" and
trypsin appear to be induced by the same factors, and mediate similar
events, it was considered pertinent to explore the relationship between
"lectins" and trypsin in midgut of the tsetse fly, Glossina morsitans
morsitans.
In these studies, it was shown that the sugar D-glucosamine
specifically and reversibly inhibited trypsin and trypsin-like enzyme
activity. In contrast, galactosamine, mannose, glucose, fructose, galactose,
Inositol, glucosamine pentacetate. N-acetyl-glucosamine, methyl-a- Dglucopyranoside,
methyl-E-Dvglucopyranoside, a-D-mannosamine had no
inhibitory effect on tsetse fly trypsin activity even at concentrations as high
as 700 mM. The inhibition by glucosamine was determined to be partial,
as shown by non linear Dixon plots. The Lineweaver-Burk plots
intersected on the y axis, a pattern characteristic or competitive inhibition.
The Kjwas estimated to be 68 + 3 mM. Clucosarnine also had similar
inhibition effect on bovine pancreas trypsin. However, glucosamine did
not inhibit tsetse fly midgut aminopeptidase activity. Interestingly,
glucosamine at a concentration of 100 mM both in vivo and in vitro,
inhibited transformation of Trypanosoma brucei brucei bloodstream forms
to procyclic forms. The inhibition of transformation was fairly constant,
and 90% of the parasites were still in the bloodstream forms 8 hours after
feeding. On the other hand, transformation proceeded normally in the
absence of glucosamine with 80-90% of the parasites in the procyclic form 8
hours after feeding. The results suggest a close relationship exist between
tsetse fly midgut lectins which are specifically inhibited by glucosamine
and the enzymes, trypsin and trypsin-like.
In addition Glossina morsitans morsitans midgut proteases, trypsin
and trypsin like were purified and partially characterized. The purification
process involved anion exchange, gel filtration, affinity chromatography
and electroelution. The two enzymes, trypsin and trypsin-like enzyme
had the molecular weight of - 24 ;r<D. They differed in charge, trypsin
being positively charged at pH 8.0 and trypsin-like enzyme had a net
negative charge at the same pH. Soybean trypsin inhibitor (STI) and N-p-
Tosyl-lysine chloromethyl ketone .(TLCK) had similar inhibitory effect on
the trypsin and trypsin-like enzyme. The Kjs' for trypsin and trypsin-like
enzyme were determined to be 0.295, 0.24 ~g/ml for STI and 0.12, 0.15
mg/ml for TLCK respectively. The tsetse fly midgut trypsin was 2-3 times
more active than the trypsin-like enzyme. | en |
