![Figure 7. Hematopoietic activity in intra-BM islet-infused mice after infection with LCMV. (A) Mice receiving islets intra-BM were infected at approximately 1 year of age with 2 × 105 plaque-forming units of LCMV. Glycemia, platelet, and WBC counts were measured either daily or every other day. (B) Femurs collected from intra-BM islet-transplanted LCMV-treated mice and from controls (age-matched C57BL/6 mice either infected with LCMV or not) were harvested on day 8 postinfection and monitored for the relative content of BM precursors and the presence of insulin-producing β cells. (C) Viral titers in blood harvested at the indicated time points after infection were measured by a reverse transcription–polymerase chain reaction–based assay with a detection limit of 103 copies of LCMV RNA (genome equivalents [GE]) per mL of total blood. Results are expressed as means of triplicate measurements ± SD. Assessment by intracellular IFN-γ staining of the percentage of glycoprotein 33-specific CD8+ T cells recovered from spleens harvested at day 8 postinfection. Results are expressed as mean ± SD.](https://ash.silverchair-cdn.com/ash/content_public/journal/blood/114/20/10.1182_blood-2009-03-209973/4/zh89990944750007.jpeg?Expires=1722655622&Signature=ETuCsCDpWvc-PbzcAIL~dfkuP4qKl497Zz6mORI7z7dpOHVv~z9x0w8Mw5uLU36R1dH3XkOm0m9xTFwSi~-2DsAEl-BEL7Ej~3PSp8SZdXK4yVf-K8xndLkaWuWsNP88cBvPok-EGEeQ95iwaWm~Ri~LFAd~Fbn8rGxChEzdHHBUglapwRcvjfX6O0NeLmHyxDBxgsL9TwjFk--yk-wHhgqFowbtHtTHIjvipIzts1AyzgV7f76eDswglVIrd1IEKw2AWTs7zA4oaTU~i4bWpHjDi1pCJlNrJdm1cIj6KdVzsIVDDmde1Nyka7S~IZfLPzhAdzNr6I1xA1ufLqe9ug__&Key-Pair-Id=APKAIE5G5CRDK6RD3PGA)
Hematopoietic activity in intra-BM islet-infused mice after infection with LCMV. (A) Mice receiving islets intra-BM were infected at approximately 1 year of age with 2 × 105 plaque-forming units of LCMV. Glycemia, platelet, and WBC counts were measured either daily or every other day. (B) Femurs collected from intra-BM islet-transplanted LCMV-treated mice and from controls (age-matched C57BL/6 mice either infected with LCMV or not) were harvested on day 8 postinfection and monitored for the relative content of BM precursors and the presence of insulin-producing β cells. (C) Viral titers in blood harvested at the indicated time points after infection were measured by a reverse transcription–polymerase chain reaction–based assay with a detection limit of 103 copies of LCMV RNA (genome equivalents [GE]) per mL of total blood. Results are expressed as means of triplicate measurements ± SD. Assessment by intracellular IFN-γ staining of the percentage of glycoprotein 33-specific CD8+ T cells recovered from spleens harvested at day 8 postinfection. Results are expressed as mean ± SD.
