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This work is licensed under a Creative Commons Attribution ... · PowerPoint Presentation Author: Marcelo Jacobs-Lorena Created Date: 9/22/2006 3:50:17 PM

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Page 1: This work is licensed under a Creative Commons Attribution ... · PowerPoint Presentation Author: Marcelo Jacobs-Lorena Created Date: 9/22/2006 3:50:17 PM

This work is licensed under a Creative Commons Attribution-NonCommercial-ShareAlike License. Your use of this material constitutes acceptance of that license and the conditions of use of materials on this site.

Copyright 2006, The Johns Hopkins University and Marcelo Jacobs-Lorena. All rights reserved. Use of these materials permitted only in accordance with license rights granted. Materials provided “AS IS”; no representations or warranties provided. User assumes all responsibility for use, and all liability related thereto, and must independently review all materials for accuracy and efficacy. May contain materials owned by others. User is responsible for obtaining permissions for use from third parties as needed.

Page 2: This work is licensed under a Creative Commons Attribution ... · PowerPoint Presentation Author: Marcelo Jacobs-Lorena Created Date: 9/22/2006 3:50:17 PM

Genetic Approaches forMalaria Control

Marcelo Jacobs-Lorena, PhD

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The Malaria Problem

At risk: >2,000,000,000 in 102 countries

Infected: >270,000,000

Clinically ill: >110,000,000 cases each year

Deaths: >2,000,000 each year• 90% in Africa• Mainly children 5-yr-old or younger

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From CDC web site

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Possible Weapons to Fight Malaria

1. Drugs that kill the parasite in humans

2. Insecticides that kill the mosquito vector

3. 3. Vaccines

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1. Drugs

Plasmodium falciparum is now largely resistant to chloroquine, which used to be the most effective drug.

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2. Insecticides: Mosquitoes Quickly Acquire Resistance

AfterBefore During

Biologic niche intact Mosquitoes return

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Mosquito Breeding

Photo: Marcelo Jacobs-Lorena

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Mosquito Breeding

Photo: Marcelo Jacobs-Lorena

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Mosquito Breeding

Photo: Marcelo Jacobs-Lorena

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3. Vaccine3. Vaccine……

… does not exist (yet).

It does not exist (yet)…

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The mosquito is an obligatory vectorThe mosquito is an obligatory vector(transmission by transfusion has no epidemiological significance)

Interference with parasite development Interference with parasite development will result in decreased transmissionwill result in decreased transmission

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Anopheles gambiae

CDC

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NEW APPROACH:NEW APPROACH:GENETIC MODIFICATION OF MOSQUITOESGENETIC MODIFICATION OF MOSQUITOES

1) GENETICALLY ENGINEER MOSQUITOESTO MAKE THEM RESISTANT TO PLASMODIUM

2) INTRODUCE THE REFRACTORY GENE(S)INTO MOSQUITO POPULATIONS

LESS TRANSMISSION LESS MALARIA

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Plasmodium development in the mosquito

Ghosh et al. (2003) Trends in Parasitology 19:94-101. Used with Permission.

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The use of a

PHAGE DISPLAY LIBRARY

to search for peptides with affinity to mosquito salivary gland and midgut epithelia

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Repeat selection 3 times

Enriched phage population

Dissect gut, open into a sheet, wash

Elute

Feeder

Midgut lumen

Elute

Repeat selection 3 times

Enriched phage population

Inject

Dissect, wash

Salivary gland

From Ghosh et al. Proc Nat Acad Sci USA 2001;98:13278-1328. Copyright 2001 National Academy of Sciences, USA. Used with permission.

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SM1 PEPTIDE

C C

Q

IA

FQ

SI

NP

R

BIOTIN

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SALIVARY GLANDS INCUBATED WITH BIOTINYLATED PEPTIDES

pSM1

FITC DAPI

unrelatedpeptide

From Ghosh et al. Proc Nat Acad Sci USA 2001;98:13278-1328. Copyright 2001 National Academy of Sciences, USA. Used with permission.

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THE SM1 PEPTIDE BINDS TO THE MIDGUT LUMENBUT NOT TO THE OUTSIDE

Open midgutsheet

FITC DIC optics

Closed (intact)midgut

From Ghosh et al. Proc Nat Acad Sci USA 2001;98:13278-1328. Copyright 2001 National Academy of Sciences, USA. Used with permission.

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SM1 Constructfor Mosquito Germ Line Transformation

Gut-specific & blood-induciblecarboxypeptidase promoter

Secretionsignal

[SM1]4

HA1epitope

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An. stephensi - piggyBac (3xP3-eGFP)eye-specific

promoter

WT

WT

TransgenicTransgenic

Transgenic

Larvae Adults

Images courtesy of Jacobs-Lorena

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Inhibition of oocyst formationin CP-[SM1]4 transgenic mosquitoes

Average of 9 experiments:

Oocysts/ Inhibitiongut

Non-trangenic 9382%

CP-[SM1]4 18(range: 69% - 95%)

Ito et al. (2002) Nature 417:452-455.

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Challenge: Driving Genes into Mosquito Populations

What drive mechanisms are being considered?

1. Transposable elements

2. Wolbachia

3. Meiotic drive

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An Alternative

Introduce genes into bacteriagenes into bacteria of the mosquito

midgut, instead of into the mosquito itself

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0

50

100

150

200

250

300

Mea

n oo

cyst

s/m

idgu

t

**

* p < 0.001

OmpA SM1-1 SM1-2

E. coliE. coliOmpAOmpA SM1

-- Feed Feed E.coliE.coli ( , or ) to ( , or ) to An. stephensiAn. stephensi mosquitoesmosquitoes-- After 24 h feed a After 24 h feed a P. bergheiP. berghei--infected blood mealinfected blood meal-- After 15 d count oocysts per gut (n > 100 mosquitoes) After 15 d count oocysts per gut (n > 100 mosquitoes)