Novel NK cell activation/maturation defect in a patient with melanoma and opportunistic fungal infection

CAROLINA INÉS DOMAICA; IGNACIO URIARTE; MARÍA VICTORIA GIRART; JESSICA SARDANOUS; DORINA ILEANA COMAS; DANIELA DI GIOVANNI; MARÍA ISABEL GAILLARD; NORBERTO WALTER ZWIRNER; LILIANA BEZRODNIK

Ciudad Autonoma de Buenos Aires, Argentina

Congreso; 1º Congreso Franco-Argentino de Inmunología, LVIII Reunión Anual de la Sociedad Argentina de Inmunología, XIII Jornada Científica del Grupo Rioplatense de Citometría de Flujo y 3º Jornadas Argentinas de Inmunodeficiencias Primarias; 2010

Sociedad Argentina de Inmunología y Sociedad Francesa de Inmunología

<!-- /* Font Definitions */ @font-face {font-family:"Cambria Math"; panose-1:2 4 5 3 5 4 6 3 2 4; mso-font-charset:0; mso-generic-font-family:roman; mso-font-pitch:variable; mso-font-signature:-1610611985 1107304683 0 0 159 0;} /* Style Definitions */ p.MsoNormal, li.MsoNormal, div.MsoNormal {mso-style-unhide:no; mso-style-qformat:yes; mso-style-parent:""; margin:0cm; margin-bottom:.0001pt; mso-pagination:widow-orphan; font-size:12.0pt; font-family:"Times New Roman","serif"; mso-fareast-font-family:"Times New Roman"; mso-ansi-language:ES; mso-fareast-language:ES;} .MsoChpDefault {mso-style-type:export-only; mso-default-props:yes; font-size:10.0pt; mso-ansi-font-size:10.0pt; mso-bidi-font-size:10.0pt;} @page WordSection1 {size:595.3pt 841.9pt; margin:70.9pt 3.0cm 70.9pt 3.0cm; mso-header-margin:35.45pt; mso-footer-margin:35.45pt; mso-paper-source:0;} div.WordSection1 {page:WordSection1;} --> Melanoma and severe opportunistic infections, mainly fungal infections, are rare in healthy pediatric individuals. Here, we present a case of a 13 year old male, second son from non-consanguineous parents with clinical background of atopy and upper airway infections. At the age of 12, the patient presented a melanoma in the right ear, which was successfully treated by surgery. One year later he developed a lobar pneumonia due to Cryptococcus neoformans detected in a lung biopsy, accompanied by stools with blood. Thus, the patient was subjected to additional immunological studies, which ruled out the occurrence of classical cellular and humoral primary and secondary immunodeficiencies. A surprising finding was a persistently high percentage of CD56bright NK cells in PBMCs. Thus, the NK cell compartment was further investigated, assuming that an impaired NK cell function could lead to a weakened immune surveillance and the development of the observed clinical symptoms. NK cells of this patient, although normal in number, contain an unexpectedly high percentage of CD56bright cells (22.8±1.5% vs 5.8±1.4% for normal individuals, p<0.0001). Also, CD56dim NK cells of this patient expressed less perforin than CD56dim NK cells from normal donors (7% vs 20-50% of pfp+ CD56dim NK cells). Stimulation of PBMCs with PHA+IL-2 for 3 days did not restore normal perforin expression (upon stimulation, 11% of CD56dim NK cells were pfp+ in this patient vs 38% of CD56dim NK cells were pfp+ in the normal donors, while 5% of CD56bright NK cells were pfp+ cells in this patient vs 51% of CD56bright NK cells were pfp+ cells in the normal donors). Moreover, stimulation of PBMCs with PHA+IL-2 or PHA+IL-15 for 3-5 days did not trigger activation-induced down-regulation of CD62L in CD56bright NK cells in this patient. These studies indicate that this patient may curse with an underlying defect in NK cell activation/maturation that may preclude development of full NK cell effector functions.