A Hereditary Form of Small Intestinal Carcinoid Associated With a Germline Mutation in Inositol Polyphosphate Multikinase

Yoshitatsu Sei; Xilin Zhao; Joanne Forbes; Silke Szymczak; Qing Li; Apurva Trivedi; Mark Voellinger; Grishma Joy; Jianying Feng; Millie Whatley; Mary Pat Sussex Jones; Ursula L. Harper; Stephen J. Marx; Aradhana M. Venkatesan; Settara C. Chandrasekharappa; Mark Raffeld; Martha M. Quezado; Adeline Louie; Clara C. Chen; Ramona M. Lim; Richa Agarwala; Alejandro A. Schäffer; Marybeth S. Hughes; Joan E. Bailey-Wilson; Stephen A. Wank

doi:10.1053/j.gastro.2015.04.008

A Hereditary Form of Small Intestinal Carcinoid Associated With a Germline Mutation in Inositol Polyphosphate Multikinase

Yoshitatsu Sei, Xilin Zhao, Joanne Forbes, Silke Szymczak, Qing Li, Apurva Trivedi, Mark Voellinger, Grishma Joy, Jianying Feng, Millie Whatley, Mary Pat Sussex Jones, Ursula L. Harper, Stephen J. Marx, Aradhana M. Venkatesan, Settara C. Chandrasekharappa, Mark Raffeld, Martha M. Quezado, Adeline Louie, Clara C. Chen, Ramona M. LimRicha Agarwala, Alejandro A. Schäffer, Marybeth S. Hughes, Joan E. Bailey-Wilson, Stephen A. Wank

Research output: Contribution to journal › Article › peer-review

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Abstract

Background & Aims Small intestinal carcinoids are rare and difficult to diagnose and patients often present with advanced incurable disease. Although the disease occurs sporadically, there have been reports of family clusters. Hereditary small intestinal carcinoid has not been recognized and genetic factors have not been identified. We performed a genetic analysis of families with small intestinal carcinoids to establish a hereditary basis and find genes that might cause this cancer. Methods We performed a prospective study of 33 families with at least 2 cases of small intestinal carcinoids. Affected members were characterized clinically and asymptomatic relatives were screened and underwent exploratory laparotomy for suspected tumors. Disease-associated mutations were sought using linkage analysis, whole-exome sequencing, and copy number analyses of germline and tumor DNA collected from members of a single large family. We assessed expression of mutant protein, protein activity, and regulation of apoptosis and senescence in lymphoblasts derived from the cases. Results Familial and sporadic carcinoids are clinically indistinguishable except for the multiple synchronous primary tumors observed in most familial cases. Nearly 34% of asymptomatic relatives older than age 50 were found to have occult tumors; the tumors were cleared surgically from 87% of these individuals (20 of 23). Linkage analysis and whole-exome sequencing identified a germline 4-bp deletion in the gene inositol polyphosphate multikinase (IPMK), which truncates the protein. This mutation was detected in all 11 individuals with small intestinal carcinoids and in 17 of 35 family members whose carcinoid status was unknown. Mutant IPMK had reduced kinase activity and nuclear localization, compared with the full-length protein. This reduced activation of p53 and increased cell survival. Conclusions We found that small intestinal carcinoids can occur as an inherited autosomal-dominant disease. The familial form is characterized by multiple synchronous primary tumors, which might account for 22%-35% of cases previously considered sporadic. Relatives of patients with familial carcinoids should be screened to detect curable early stage disease. IPMK haploinsufficiency promotes carcinoid tumorigenesis.

Original language	English (US)
Article number	59715
Pages (from-to)	67-78
Number of pages	12
Journal	Gastroenterology
Volume	149
Issue number	1
DOIs	https://doi.org/10.1053/j.gastro.2015.04.008
State	Published - Jul 1 2015
Externally published	Yes

Keywords

Familial
Linkage
Screening
Tumor Suppressor Gene

ASJC Scopus subject areas

Hepatology
Gastroenterology

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10.1053/j.gastro.2015.04.008

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Sei, Y., Zhao, X., Forbes, J., Szymczak, S., Li, Q., Trivedi, A., Voellinger, M., Joy, G., Feng, J., Whatley, M., Jones, M. P. S., Harper, U. L., Marx, S. J., Venkatesan, A. M., Chandrasekharappa, S. C., Raffeld, M., Quezado, M. M., Louie, A., Chen, C. C., ... Wank, S. A. (2015). A Hereditary Form of Small Intestinal Carcinoid Associated With a Germline Mutation in Inositol Polyphosphate Multikinase. Gastroenterology, 149(1), 67-78. Article 59715. https://doi.org/10.1053/j.gastro.2015.04.008

Sei, Y, Zhao, X, Forbes, J, Szymczak, S, Li, Q, Trivedi, A, Voellinger, M, Joy, G, Feng, J, Whatley, M, Jones, MPS, Harper, UL, Marx, SJ, Venkatesan, AM, Chandrasekharappa, SC, Raffeld, M, Quezado, MM, Louie, A, Chen, CC, Lim, RM, Agarwala, R, Schäffer, AA, Hughes, MS, Bailey-Wilson, JE & Wank, SA 2015, 'A Hereditary Form of Small Intestinal Carcinoid Associated With a Germline Mutation in Inositol Polyphosphate Multikinase', Gastroenterology, vol. 149, no. 1, 59715, pp. 67-78. https://doi.org/10.1053/j.gastro.2015.04.008

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title = "A Hereditary Form of Small Intestinal Carcinoid Associated With a Germline Mutation in Inositol Polyphosphate Multikinase",

abstract = "Background & Aims Small intestinal carcinoids are rare and difficult to diagnose and patients often present with advanced incurable disease. Although the disease occurs sporadically, there have been reports of family clusters. Hereditary small intestinal carcinoid has not been recognized and genetic factors have not been identified. We performed a genetic analysis of families with small intestinal carcinoids to establish a hereditary basis and find genes that might cause this cancer. Methods We performed a prospective study of 33 families with at least 2 cases of small intestinal carcinoids. Affected members were characterized clinically and asymptomatic relatives were screened and underwent exploratory laparotomy for suspected tumors. Disease-associated mutations were sought using linkage analysis, whole-exome sequencing, and copy number analyses of germline and tumor DNA collected from members of a single large family. We assessed expression of mutant protein, protein activity, and regulation of apoptosis and senescence in lymphoblasts derived from the cases. Results Familial and sporadic carcinoids are clinically indistinguishable except for the multiple synchronous primary tumors observed in most familial cases. Nearly 34% of asymptomatic relatives older than age 50 were found to have occult tumors; the tumors were cleared surgically from 87% of these individuals (20 of 23). Linkage analysis and whole-exome sequencing identified a germline 4-bp deletion in the gene inositol polyphosphate multikinase (IPMK), which truncates the protein. This mutation was detected in all 11 individuals with small intestinal carcinoids and in 17 of 35 family members whose carcinoid status was unknown. Mutant IPMK had reduced kinase activity and nuclear localization, compared with the full-length protein. This reduced activation of p53 and increased cell survival. Conclusions We found that small intestinal carcinoids can occur as an inherited autosomal-dominant disease. The familial form is characterized by multiple synchronous primary tumors, which might account for 22%-35% of cases previously considered sporadic. Relatives of patients with familial carcinoids should be screened to detect curable early stage disease. IPMK haploinsufficiency promotes carcinoid tumorigenesis.",

keywords = "Familial, Linkage, Screening, Tumor Suppressor Gene",

author = "Yoshitatsu Sei and Xilin Zhao and Joanne Forbes and Silke Szymczak and Qing Li and Apurva Trivedi and Mark Voellinger and Grishma Joy and Jianying Feng and Millie Whatley and Jones, {Mary Pat Sussex} and Harper, {Ursula L.} and Marx, {Stephen J.} and Venkatesan, {Aradhana M.} and Chandrasekharappa, {Settara C.} and Mark Raffeld and Quezado, {Martha M.} and Adeline Louie and Chen, {Clara C.} and Lim, {Ramona M.} and Richa Agarwala and Sch{\"a}ffer, {Alejandro A.} and Hughes, {Marybeth S.} and Bailey-Wilson, {Joan E.} and Wank, {Stephen A.}",

note = "Publisher Copyright: {\textcopyright} 2015 AGA Institute.",

year = "2015",

month = jul,

day = "1",

doi = "10.1053/j.gastro.2015.04.008",

language = "English (US)",

volume = "149",

pages = "67--78",

journal = "Gastroenterology",

issn = "0016-5085",

publisher = "W.B. Saunders Ltd",

number = "1",

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TY - JOUR

T1 - A Hereditary Form of Small Intestinal Carcinoid Associated With a Germline Mutation in Inositol Polyphosphate Multikinase

AU - Sei, Yoshitatsu

AU - Zhao, Xilin

AU - Forbes, Joanne

AU - Szymczak, Silke

AU - Li, Qing

AU - Trivedi, Apurva

AU - Voellinger, Mark

AU - Joy, Grishma

AU - Feng, Jianying

AU - Whatley, Millie

AU - Jones, Mary Pat Sussex

AU - Harper, Ursula L.

AU - Marx, Stephen J.

AU - Venkatesan, Aradhana M.

AU - Chandrasekharappa, Settara C.

AU - Raffeld, Mark

AU - Quezado, Martha M.

AU - Louie, Adeline

AU - Chen, Clara C.

AU - Lim, Ramona M.

AU - Agarwala, Richa

AU - Schäffer, Alejandro A.

AU - Hughes, Marybeth S.

AU - Bailey-Wilson, Joan E.

AU - Wank, Stephen A.

PY - 2015/7/1

Y1 - 2015/7/1

N2 - Background & Aims Small intestinal carcinoids are rare and difficult to diagnose and patients often present with advanced incurable disease. Although the disease occurs sporadically, there have been reports of family clusters. Hereditary small intestinal carcinoid has not been recognized and genetic factors have not been identified. We performed a genetic analysis of families with small intestinal carcinoids to establish a hereditary basis and find genes that might cause this cancer. Methods We performed a prospective study of 33 families with at least 2 cases of small intestinal carcinoids. Affected members were characterized clinically and asymptomatic relatives were screened and underwent exploratory laparotomy for suspected tumors. Disease-associated mutations were sought using linkage analysis, whole-exome sequencing, and copy number analyses of germline and tumor DNA collected from members of a single large family. We assessed expression of mutant protein, protein activity, and regulation of apoptosis and senescence in lymphoblasts derived from the cases. Results Familial and sporadic carcinoids are clinically indistinguishable except for the multiple synchronous primary tumors observed in most familial cases. Nearly 34% of asymptomatic relatives older than age 50 were found to have occult tumors; the tumors were cleared surgically from 87% of these individuals (20 of 23). Linkage analysis and whole-exome sequencing identified a germline 4-bp deletion in the gene inositol polyphosphate multikinase (IPMK), which truncates the protein. This mutation was detected in all 11 individuals with small intestinal carcinoids and in 17 of 35 family members whose carcinoid status was unknown. Mutant IPMK had reduced kinase activity and nuclear localization, compared with the full-length protein. This reduced activation of p53 and increased cell survival. Conclusions We found that small intestinal carcinoids can occur as an inherited autosomal-dominant disease. The familial form is characterized by multiple synchronous primary tumors, which might account for 22%-35% of cases previously considered sporadic. Relatives of patients with familial carcinoids should be screened to detect curable early stage disease. IPMK haploinsufficiency promotes carcinoid tumorigenesis.

AB - Background & Aims Small intestinal carcinoids are rare and difficult to diagnose and patients often present with advanced incurable disease. Although the disease occurs sporadically, there have been reports of family clusters. Hereditary small intestinal carcinoid has not been recognized and genetic factors have not been identified. We performed a genetic analysis of families with small intestinal carcinoids to establish a hereditary basis and find genes that might cause this cancer. Methods We performed a prospective study of 33 families with at least 2 cases of small intestinal carcinoids. Affected members were characterized clinically and asymptomatic relatives were screened and underwent exploratory laparotomy for suspected tumors. Disease-associated mutations were sought using linkage analysis, whole-exome sequencing, and copy number analyses of germline and tumor DNA collected from members of a single large family. We assessed expression of mutant protein, protein activity, and regulation of apoptosis and senescence in lymphoblasts derived from the cases. Results Familial and sporadic carcinoids are clinically indistinguishable except for the multiple synchronous primary tumors observed in most familial cases. Nearly 34% of asymptomatic relatives older than age 50 were found to have occult tumors; the tumors were cleared surgically from 87% of these individuals (20 of 23). Linkage analysis and whole-exome sequencing identified a germline 4-bp deletion in the gene inositol polyphosphate multikinase (IPMK), which truncates the protein. This mutation was detected in all 11 individuals with small intestinal carcinoids and in 17 of 35 family members whose carcinoid status was unknown. Mutant IPMK had reduced kinase activity and nuclear localization, compared with the full-length protein. This reduced activation of p53 and increased cell survival. Conclusions We found that small intestinal carcinoids can occur as an inherited autosomal-dominant disease. The familial form is characterized by multiple synchronous primary tumors, which might account for 22%-35% of cases previously considered sporadic. Relatives of patients with familial carcinoids should be screened to detect curable early stage disease. IPMK haploinsufficiency promotes carcinoid tumorigenesis.

KW - Familial

KW - Linkage

KW - Screening

KW - Tumor Suppressor Gene

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A Hereditary Form of Small Intestinal Carcinoid Associated With a Germline Mutation in Inositol Polyphosphate Multikinase

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