Invasive Group a Streptococcal Diseases in Taiwan Is Not Associated with the Presence of Streptococcal Pyogenic Exotoxin Genes
Resource
CLINICAL INFECTIOUS DISEASES v.26 n.3 pp.584-589
Journal
CLINICAL INFECTIOUS DISEASES
Journal Volume
v.26
Journal Issue
n.3
Pages
584-589
Date Issued
1998
Date
1998
Author(s)
HSUEH, PO-REN
WU, JIUNN-JONG
TSAI, PEI-JANE
LIU, JIEN-WEI
CHUANG, YIN-CHING
LUH, KWEN-TAY
Abstract
We reviewed the clinical features of 44 patients with invasive group A streptococcal (GAS) disease who were treated at two teaching hospitals in southern Taiwan from 1991 to 1994. Genes encoding streptococcal pyrogenic exotoxin types A (speA), B (speB), C (speC), and F (speF) and serotypes of M1, M6, and M12 were determined by polymerase chain reaction to target specific sequences in the 44 isolates recovered from these patients and in 28 isolates recovered from upper respiratory sites in 28 additional patients during the study period. The protease activity of these isolates was tested by using the casein plate method. Of the 44 patients with invasive diseases, 25( 57%) had no obvious underlying diseases, and 14 (32 %) had preexisting neoplastic diseases or had previously used steroids. Twenty-five patients (57%) presented with cellulitis or necrotizing fasciitis, 24 (55%) had bacteremia , and eight (18%) had streptococcal toxic shock syndrome ( STSS). Eight patients (18%) died of invasive GAS disease; seven had STSS, and seven had underlying diseases. All eight patients died within 48 hours after hospitalization. The presence of speA, speC, or speF was not implicated in any particular clinical syndrome in patients with invasive GAS disease. High-level protease activity and the M 1 serotype of the isolates were significantly associated with the clinical signs of STSS and with mortality. M1 serotype and protease activity, as well as host immune status, might play significant roles in the pathogenesis of invasive GAS disease in Taiwan.