The sequencing race has ended and the functional race has already begun. Microarray technology enables
simultaneous gene expression analysis of thousands of genes, enabling a snapshot of an organisms’
transcriptome at an unprecedented resolution. The close correlation between gene transcription and
function, allow the inference of biological processes from the assessed transcriptome profile. Among the
sophisticated analytical problems in microarray technology at the front and back ends respectively, are the
selection of optimal DNA oligos and computational analysis of the genes expression. In this review paper,
we analyse important methods in use today in customized oligos design. In the course of executing this,
we discovered that the oligos designer algorithm hanged on gene PFA0135w of chromosome 1, while
designing oligos for the gene sequences of Plasmodium falciparum. We do not know the reason for this
yet, as the algorithm runs on other sequences like the yeast (Saccharomyces cervisiae) and Neurospora
crassa. We conclude the paper highlighting the procedures encompassing the back end phase and discuss
their application to the development of vaccines and drugs for malaria treatment. Note that, malaria is the
cause of significant global morbidity and mortality with 300-500 million cases annually. Our aims are not
ends, but a means to achieve the following: Iterate the need for experimental biologists to (i) know how to
design their customized oligos and (ii) have some idea about gene expression analysis and the need for
cooperation between experimental biologists and their counterpart, the computational biologists. These
will help experimental biologists to coordinate very well the front and the back ends of the system
biology analysis of the whole genome effectively