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HER2 deficiency causes a developmental disorder with growth retardation and craniofacial malformations
Huaxiang Zhao, Pan Wang, Yuhua Jiao, Huimei Huang, Min Yu, Qing He, Chengkai Pan, Shuang Guo, Wenbin Huang, Yunfei Jia, Qianying Kong, Huifang Peng, Yandong Han, Yuxia Hou, Zhanping Ren, Yongwei Tao, Fei Huang, Hongwei Jiang, Shan Sun, Yanying Dong, Jiuxiang Lin, Chunyan Yin, Xuechen Zhu, Feng Chen, Yi Ding
Huaxiang Zhao, Pan Wang, Yuhua Jiao, Huimei Huang, Min Yu, Qing He, Chengkai Pan, Shuang Guo, Wenbin Huang, Yunfei Jia, Qianying Kong, Huifang Peng, Yandong Han, Yuxia Hou, Zhanping Ren, Yongwei Tao, Fei Huang, Hongwei Jiang, Shan Sun, Yanying Dong, Jiuxiang Lin, Chunyan Yin, Xuechen Zhu, Feng Chen, Yi Ding
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Research Article Development Genetics

HER2 deficiency causes a developmental disorder with growth retardation and craniofacial malformations

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Abstract

The human epidermal growth factor receptor 2 (HER2) is a major therapeutic target in cancer. While the oncogenic effects of HER2 hyperactivation are well characterized, the biological consequences of its deficiency remain poorly defined. Here, through exome sequencing analyses of a cohort of 720 families affected by isolated or syndromic orofacial clefts, we unexpectedly identified 5 distinct rare germline HER2 variants in 5 unrelated families with growth deficits, orofacial clefts, and other craniofacial, skeletal, and auditory anomalies. In Xenopus embryos, these variants failed to recapitulate the developmental effects of WT HER2. In cultured cells, they disrupted HER2 protein stability, membrane localization, or site-specific phosphorylation, resulting in diminished ERK signaling. Strikingly, knock-in mice expressing a patient-derived HER2 variant and mice maternally exposed to Tucatinib, a recently approved anti-HER2 drug, both replicated patient phenotypes: delayed growth and diverse craniofacial abnormalities, including ocular dysgenesis, short jaws, and cleft palate. Collectively, our findings define a developmental disorder that we designate GRACE syndrome (Growth Retardation and Craniofacial Malformations Caused by HER2 Deficiency), establish HER2’s essential role in human growth and craniofacial morphogenesis, and reveal that HER2-targeted therapies during pregnancy can induce craniofacial defects and lifelong growth impairment in fetuses.

Authors

Huaxiang Zhao, Pan Wang, Yuhua Jiao, Huimei Huang, Min Yu, Qing He, Chengkai Pan, Shuang Guo, Wenbin Huang, Yunfei Jia, Qianying Kong, Huifang Peng, Yandong Han, Yuxia Hou, Zhanping Ren, Yongwei Tao, Fei Huang, Hongwei Jiang, Shan Sun, Yanying Dong, Jiuxiang Lin, Chunyan Yin, Xuechen Zhu, Feng Chen, Yi Ding

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Figure 3

HER2 is expressed in growth plate proliferating chondrocytes and craniofacial tissues in mice.

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HER2 is expressed in growth plate proliferating chondrocytes and craniof...
(A) Schematic diagram of mouse growth plate. RZ, resting zone; PZ, proliferating zone; HZ, hypertrophic zone. (B and C) Immunostaining of HER2 (red) in the P21 mouse proximal tibial growth plate shows its predominant expression in proliferating chondrocytes. The boxed region in panel B is shown at higher magnification in panel C. (D–F) Schematic diagrams of coronal sections of mouse craniofacial region at indicated stages (36, 37). (G–I) Overview of HER2 immunostaining (red) in coronal sections of mouse heads at E13.5, E15.0, and E15.5. Aside from epidermis and oral epithelium, HER2 is also expressed in the eyes and cranial neural crest–derived (CNC-derived) mesenchyme. (J–L) Magnified views of the maxillary region from panels G–I. HER2 shows strong expression in the differentiated osteoblasts and osteogenic front (green dashed circles in panels K and L) and the tooth germs (white dashed lines in panels J–L). In addition, HER2 expression is detected in midline epithelial seam formed by the fusing palatal shelves at E15.0 and diminishes as the seam underwent degradation at E15.5 (white arrowheads in panels K and L). (M–O) Magnified views of the mandibular region from panels G–I. Strong HER2 expression is detected in differentiated osteoblasts and osteogenic front (green dashed circles in panels M–O), but not in Meckel’s cartilage and perichondrium (yellow dashed circles in panels M–O). HER2 expression is also observed in the mandibular tooth germs (white dashed lines in panels M–O) and in the tongue muscle (white arrows in panels N and O). T, tongue; PS, palatal shelf; SP, secondary palate; MES, midline epithelial seam; CNC, cranial neural crest. Scale bar: 200 μm in all panels.

Copyright © 2026 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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