TY - JOUR
T1 - Drug resistance in non-B subtype HIV-1
T2 - Impact of HIV-1 reverse transcriptase inhibitors
AU - Singh, Kamalendra
AU - Flores, Jacqueline A.
AU - Kirby, Karen A.
AU - Neogi, Ujjwal
AU - Sonnerborg, Anders
AU - Hachiya, Atsuko
AU - Das, Kalyan
AU - Arnold, Eddy
AU - McArthur, Carole
AU - Parniak, Michael
AU - Sarafianos, Stefan G.
N1 - Publisher Copyright:
© 2014 by the authors; licensee MDPI, Basel, Switzerland.
PY - 2014/9/24
Y1 - 2014/9/24
N2 - Human immunodeficiency virus (HIV) causes approximately 2.5 million new infections every year, and nearly 1.6 million patients succumb to HIV each year. Several factors, including cross-species transmission and error-prone replication have resulted in extraordinary genetic diversity of HIV groups. One of these groups, known as group M (main) contains nine subtypes (A-D, F-H and J-K) and causes ∼95% of all HIV infections. Most reported data on susceptibility and resistance to anti-HIV therapies are from subtype B HIV infections, which are prevalent in developed countries but account for only ∼12% of all global HIV infections, whereas non-B subtype HIV infections that account for ∼88% of all HIV infections are prevalent primarily in low and middle-income countries. Although the treatments for subtype B infections are generally effective against non-B subtype infections, there are differences in response to therapies. Here, we review how polymorphisms, transmission efficiency of drug-resistant strains, and differences in genetic barrier for drug resistance can differentially alter the response to reverse transcriptase-targeting therapies in various subtypes.
AB - Human immunodeficiency virus (HIV) causes approximately 2.5 million new infections every year, and nearly 1.6 million patients succumb to HIV each year. Several factors, including cross-species transmission and error-prone replication have resulted in extraordinary genetic diversity of HIV groups. One of these groups, known as group M (main) contains nine subtypes (A-D, F-H and J-K) and causes ∼95% of all HIV infections. Most reported data on susceptibility and resistance to anti-HIV therapies are from subtype B HIV infections, which are prevalent in developed countries but account for only ∼12% of all global HIV infections, whereas non-B subtype HIV infections that account for ∼88% of all HIV infections are prevalent primarily in low and middle-income countries. Although the treatments for subtype B infections are generally effective against non-B subtype infections, there are differences in response to therapies. Here, we review how polymorphisms, transmission efficiency of drug-resistant strains, and differences in genetic barrier for drug resistance can differentially alter the response to reverse transcriptase-targeting therapies in various subtypes.
KW - Drug resistance
KW - HIV subtypes
KW - HIV-1 reverse transcriptase
KW - Non-nucleoside RT inhibitors
KW - Nucleoside RT inhibitors
KW - Translocation defective RT inhibitors
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U2 - 10.3390/v6093535
DO - 10.3390/v6093535
M3 - Review article
C2 - 25254383
AN - SCOPUS:84907909666
SN - 1999-4915
VL - 6
SP - 3535
EP - 3562
JO - Viruses
JF - Viruses
IS - 9
ER -